VICP Registry Case Source Bundle
Canonical URL: https://vicp-registry.org/case/USCOURTS-cofc-1_18-vv-01782
Package ID: USCOURTS-cofc-1_18-vv-01782
Petitioner: Lisa L. Arredondo
Filed: 2018-11-19
Decided: 2026-03-26
Vaccine: influenza
Vaccination date: 2017-09-21
Condition: Bell's palsy
Outcome: compensated
Award amount USD: 180000

AI-assisted case summary:
On November 19, 2018, Lisa L. Arredondo filed a petition alleging that an influenza vaccination administered in her left deltoid on September 21, 2017 caused Bell's palsy. Ms. Arredondo was a 51-year-old registered nurse at the time of vaccination, and the flu shot was required for her work. Respondent contested causation.

The medical record placed onset on October 1, 2017, ten days after vaccination. Within days, Ms. Arredondo sought care for right-sided facial symptoms: difficulty closing her eye, drooping of the eyelid and mouth, ear and facial pain, numbness or paresthesia, difficulty eating, drinking, speaking, and drooling. Her primary care physician diagnosed Bell's palsy, prescribed acyclovir and steroids, and ordered a brain MRI, which did not show a significant intracranial abnormality. Her employer also filed a VAERS report noting facial paralysis and neck pain after the flu shot.

The illness did not resolve quickly. Ms. Arredondo later treated with neurology, plastic surgery, ophthalmology, physical therapy, acupuncture, and repeated Botox injections. The damages record described persistent right-sided facial weakness and asymmetry, lagophthalmos and dry eye, synkinesis, ptosis, hyperacusis, ear pain or hearing changes, facial spasms, difficulty chewing and speaking, and emotional distress from disfigurement and loss of normal facial expression. She described the injury as affecting her work, marriage, social life, eating in public, photographs with family and friends, and the ordinary ability to smile.

For entitlement, Ms. Arredondo relied principally on Dr. Lawrence Steinman, a Stanford neurologist, who described Bell's palsy as an inflammatory peripheral-nerve disorder and proposed molecular mimicry and immune cross-reactivity between influenza-vaccine antigens and facial-nerve targets. Respondent relied on neurology and immunology experts, including Dr. Brian Callaghan and Dr. J. Lindsay Whitton, who disputed whether the proposed ganglioside and peripheral-nerve antigen theories were reliable and whether the record showed vaccine causation.

Special Master Nora Beth Dorsey found Ms. Arredondo entitled to compensation on October 31, 2023. She accepted the molecular mimicry theory as legally reliable for this case, found a logical sequence of cause and effect, found the ten-day onset medically acceptable, and found no persuasive alternative cause.

The parties could not resolve damages. Ms. Arredondo sought the $250,000 statutory cap for pain and suffering, while respondent argued for $140,000. On March 26, 2026, Special Master Dorsey awarded $180,000.00 for actual pain and suffering and also awarded funding for disputed life-care-plan items, including ongoing eye and mouth care supplies and a humidifier, with the parties directed to finalize the complete life care plan and confirm previously agreed amounts for lost wages and out-of-pocket expenses.

Theory of causation field:
Influenza vaccine September 21, 2017, at age 51, causing right-sided Bell's palsy with onset October 1, 2017 (10 days). COMPENSATED. Theory: immune-mediated peripheral facial nerve injury through molecular mimicry/cross-reactivity after flu vaccination. Petitioner expert Dr. Lawrence Steinman; respondent experts included Dr. Brian Callaghan and Dr. J. Lindsay Whitton. MRI showed no intracranial cause; records documented persistent facial weakness/asymmetry, dry eye, synkinesis, hyperacusis, ear/facial pain, Botox, PT, ophthalmology and plastic-surgery care. SM Nora Beth Dorsey granted entitlement October 31, 2023, then awarded $180,000 pain/suffering plus life-care-plan items on March 26, 2026. Attorney: Lisa Roquemore.

Public staged source text:

================================================================================
DOCUMENT 1: USCOURTS-cofc-1_18-vv-01782-0
Date issued/filed: 2023-11-27
Pages: 42
Docket text: PUBLIC RULING (Originally filed: 10/31/2023) regarding 92 Ruling on Entitlement. Signed by Special Master Nora Beth Dorsey. (kis) Service on parties made.
--------------------------------------------------------------------------------
Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 1 of 42
In the United States Court of Federal Claims
OFFICE OF SPECIAL MASTERS
Filed: October 31, 2023
* * * * * * * * * * * * * * * * * * * * * * * * *
LISA L. ARREDONDO, * PUBLISHED
*
Petitioner, * No. 18-1782V
*
v. * Special Master Nora Beth Dorsey
*
SECRETARY OF HEALTH * Entitlement; Influenza (“Flu”) Vaccine;
AND HUMAN SERVICES, * Bell’s Palsy.
*
Respondent. *
*
* * * * * * * * * * * * * * * * * * * * * * * * *
Lisa Roquemore, Law Office of Lisa A. Roquemore, Rancho Santa Margarita, CA, for
Petitioner.
Bridget Corridon, U.S. Department of Justice, Washington, DC, for Respondent.
RULING ON ENTITLEMENT1
I. INTRODUCTION
On November 19, 2018, Lisa L. Arredondo (“Petitioner”) filed a petition for
compensation under the National Vaccine Injury Compensation Program (“Vaccine Act” or “the
1 Because this Ruling contains a reasoned explanation for the action in this case, the undersigned
is required to post it on the United States Court of Federal Claims’ website and/or at
https://www.govinfo.gov/app/collection/uscourts/national/cofc in accordance with the E-
Government Act of 2002. 44 U.S.C. § 3501 note (2018) (Federal Management and Promotion of
Electronic Government Services). This means the Ruling will be available to anyone with
access to the Internet. In accordance with Vaccine Rule 18(b), Petitioner has 14 days to
identify and move to redact medical or other information, the disclosure of which would
constitute an unwarranted invasion of privacy. If, upon review, the undersigned agrees that the
identified material fits within this definition, the undersigned will redact such material from
public access.

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 2 of 42
Program”), 42 U.S.C. § 300aa-10 et seq. (2018).2 Petitioner alleges that she suffered Bell’s palsy
as the result of an influenza (“flu”) vaccination administered on September 21, 2017. Petition at
2 (ECF No. 1). Respondent argued against compensation, stating that “[P]etitioner is not entitled
to an award under the [Vaccine] Act.” Respondent’s Report (“Resp. Rept.”) at 4 (ECF No. 21).
After carefully analyzing and weighing the evidence presented in this case in accordance
with the applicable legal standards, the undersigned finds that Petitioner has provided
preponderant evidence that her flu vaccine caused her Bell’s palsy, satisfying Petitioner’s burden
of proof under Althen v. Secretary of Health & Human Services, 418 F.3d 1274, 1280 (Fed. Cir.
2005). Accordingly, Petitioner is entitled to compensation.
II. ISSUES TO BE DECIDED
Diagnosis is not at issue. Joint Prehearing Submission, filed Sept. 13, 2022 at 1 (ECF
No. 75). The parties stipulated that Petitioner received a flu vaccine on September 21, 2017, and
that onset of her symptoms, consistent with Bell’s palsy, was October 1, 2017. Id.
The central issue is whether Petitioner has provided preponderant evidence of causation
for all three Althen prongs. Joint Prehearing Submission at 2. Petitioner asserts that she has met
her burden under the Althen prongs. Petitioner’s Prehearing Brief (“Pet. Br.”), filed Sept. 6,
2022, at 25-32 (ECF No. 68). Respondent disagrees and argues that Petitioner failed to submit
preponderant evidence that her flu vaccine more likely than not caused her Bell’s palsy. Resp.
Prehearing Br. (“Resp. Br.”), filed Sept. 27, 2022, at 15-31 (ECF No. 78).
III. BACKGROUND
A. Medical Terminology
Bell’s palsy is defined as “unilateral facial paralysis of sudden onset, due to [a] lesion of
the facial nerve[,] [] resulting in characteristic distortion of the face.” Bell Palsy, Dorland’s
Med. Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=95779 (last
visited Oct. 23, 2023). Bell’s palsy is considered an “idiopathic peripheral nerve palsy involving
2 The National Vaccine Injury Compensation Program is set forth in Part 2 of the National
Childhood Vaccine Injury Act of 1986, Pub. L. No. 99-660, 100 Stat. 3755, codified as amended,
42 U.S.C. §§ 300aa-10 to -34 (2018) (“Vaccine Act” or “the Act”). All citations in this Ruling to
individual sections of the Vaccine Act are to 42 U.S.C.A. § 300aa.
2

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 3 of 42
the facial nerve.” Pet. Exhibit (“Ex.”) 19 at 1.3 The facial nerve (seventh cranial nerve)4 “travels
through a narrow, bony canal . . . in the skull, beneath the ear, to the muscles on each side of the
face.” Pet. Ex. 17 at 1.5 It innervates muscles on the face that “control eye blinking and closing,
and facial expressions like smiling and frowning.” Id. The facial nerve also “carries nerve
impulses to the . . . the tear glands, the saliva glands, and the muscles of a small bone in the
middle ear” as well as the tongue. Id. When the “function of the facial nerve is disrupted,”
facial paralysis or weakness occurs. Id.
3 A. Greco et al., Bell’s Palsy and Autoimmunity, 12 Autoimmunity Rev. 323 (2012).
4 The facial nerve, or seventh cranial nerve, “consist[s] of two roots: a large motor root, which
supplies the muscles of facial expression, and a smaller root, the nervus intermedius.” Nervus
Facialis, Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/dorland/
definition?id=92293 (last visited Oct. 19, 2023). The nervus intermedius, or intermediate nerve,
“joins the main root at, or merges with, the geniculate ganglion at the geniculum of the facial
nerve; it contributes parasympathetic and special sensory fibers to the facial nerve.” Nervus
Intermedius, Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/dorland/
definition?id=92313 (last visited Oct. 19, 2023).
5 Bell’s Palsy Fact Sheet, NINDS, https://www.ninds.nih.gov/bells-palsy-fact-sheet (last
modified June 6, 2018).
3

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 4 of 42
Pet. Ex. 19 at 2.
Although Bell’s palsy is a well-known and common disease, its etiology remains unclear.
Pet. Ex. 73 at 1;6 Pet. Ex. 68 at 1.7 However, autoimmune, inflammatory, and infectious
etiologies have been postulated. Pet. Ex. 19 at 1. Bell’s palsy has “been associated with [flu] or
a flu-like illness.” Pet. Ex. 17 at 1.
B. Procedural History
Petitioner filed her petition on November 19, 2018 and filed medical records8 and an
expert report from Dr. Lawrence Steinman the following day. Petition; Pet. Exs. 1-36. On
August 19, 2019, Respondent filed a Rule 4(a) Report providing the abbreviated facts of the case
but indicated that medical personnel at the Division of Injury Compensation Programs (“DICP”)
had not yet been able to review the claim and offer an opinion as to Respondent’s position.
Resp. Rept. at 3. Respondent stated that “[P]etitioner is not entitled to an award under the
[Vaccine] Act” but was awaiting “DICP’s input prior to making a determination whether an
informal resolution is warranted in this case.” Id. at 4. Thereafter, Respondent filed a status
report indicating his intent to defend the claim. Resp. Status Rept., filed Oct. 31, 2019 (ECF No.
24) (“[R]espondent is not interested in engaging in settlement discussions and intends to file a
responsive expert report.”).
The matter was reassigned to the undersigned on October 1, 2019. Notice of
Reassignment dated Oct. 1, 2019 (ECF No. 23). On March 23, 2020, Respondent filed expert
reports from Dr. Brian Callaghan and Dr. J. Lindsay Whitton. Resp. Exs. A, C. Petitioner filed a
responsive declaration on May 25, 2020. Pet. Ex. 46. On July 15, 2020, Petitioner filed a
supplemental expert report from Dr. Steinman. Pet. Ex. 47. And Respondent filed a
supplemental expert report from Dr. Whitton on September 20, 2020. Resp. Ex. E.
Pursuant to the parties’ request, the undersigned held a Rule 5 status conference on
December 2, 2020. Rule 5 Order dated Dec. 2, 2020 (ECF No. 45); see Pet. Joint Status Rept.,
filed Oct. 21, 2020 (ECF No. 43). The undersigned preliminarily found Petitioner’s proper
6 Weigong Zhou et al., A Potential Signal of Bell’s Palsy After Parenteral Inactivated Influenza
Vaccines: Reports to the Vaccine Adverse Event Reporting System (VAERS) United States,
1991-2001, 13 Pharmacoepidemiology & Drug Safety 505 (2004).
7 Cheng-Hsiu Chou et al., Bell’s Palsy Associated with Influenza Vaccination: Two Case
Reports, 25 Vaccine 2839 (2007).
8 Petitioner filed additional medical records throughout the course of litigation.
4

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 5 of 42
diagnosis was Bell’s palsy, not Ramsay Hunt syndrome.9 Rule 5 Order at 2. The undersigned
made a preliminary finding that Petitioner had provided preponderant evidence of causation
based on the Althen prongs and posited “that if this case went to a hearing, she would probably
find in favor of [P]etitioner.” Id. at 3. However, given the risk of litigation, she recommended
that “this case should be resolved by settlement.” Id.
The parties entertained settlement until March 2021. See ECF Nos. 49-50, 52. However,
after consideration, Respondent did not wish to engage in further settlement discussions. Resp.
Status Rept., filed Mar. 9, 2021 (ECF No. 52). At a status conference on April 15, 2021,
Petitioner conveyed her preference to resolve the case through an entitlement hearing. Order
dated Apr. 15, 2021 (ECF No. 54); see also Pet. Joint Status Rept., filed May 4, 2021 (ECF No.
55).
Petitioner filed a supplemental expert report from Dr. Steinman on August 24, 2022. Pet.
Ex. 75. An entitlement hearing was held October 18-19, 2022. Order dated Oct. 19, 2022 (ECF
No. 80). Petitioner, Dr. Steinman, Dr. Callaghan, and Dr. Whitton testified at the hearing.
Transcript (“Tr.”) 3, 145. On October 24, 2022, Petitioner filed a supplemental expert report
from Dr. Steinman and supporting medical literature. Pet. Exs. 83-86.
At a status conference on December 20, 2022, it was agreed that post-hearing briefs were
not necessary. Order dated Dec. 20, 2022 (ECF No. 86). However, given that Dr. Steinman
provided a post-hearing explanation on an issue, Respondent requested the opportunity to file a
responsive opinion and Petitioner further requested the opportunity to offer a rebuttal opinion.
Id. Respondent filed a supplemental expert report by Dr. Callaghan on January 31, 2023, and
Petitioner filed an opinion letter from Dr. Robert P. Lisak on February 8, 2023. Resp. Ex. G;
Pet. Ex. 91. On March 31, 2023, Respondent filed a status report in response to Dr. Lisak’s letter
and indicated the record was complete for a ruling. Resp. Status Rept., filed Mar. 1, 2023, at 3
n.3, 6 (ECF No. 90). The same day, Petitioner also filed a status report confirming the record
was complete for a ruling. Pet. Status Rept., filed Mar. 1, 2023 (ECF No. 91).
This matter is now ripe for adjudication.
C. Medical History
Petitioner is a registered nurse who received her flu vaccination due to work
requirements; she received the quadrivalent Flucelvax flu vaccine in her left deltoid on
September 21, 2017. Pet. Ex. 1 at 1; Tr. 7.
9 Ramsay Hunt syndrome is “herpes zoster involving the facial and vestibulocochlear nerves,
often associated with transitory ipsilateral facial paralysis and herpetic vesicles of the external
ear or tympanic membrane.” Ramsay Hunt Syndrome, Dorland’s Med. Dictionary Online,
https://www.dorlandsonline.com/dorland/definition?id=111266 (last visited Oct. 19, 2023).
Because the parties stipulated that Petitioner was properly diagnosed with Bell’s palsy, the
undersigned will not discuss the expert opinions pertaining to Ramsay Hunt in this Ruling. See
Joint Prehearing Submission at 1.
5

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 6 of 42
Thirteen days later, on October 4, 2017, Petitioner presented to her primary care
physician (“PCP”) at South Alamo Medical Group with paresthesia, “drooping right eye,” and
pain in her ear that started three days prior. Pet. Ex. 3 at 27. Associated symptoms included
“difficulty closing eye, drooping lower eyelid, facial muscle weakness[,] and pain near the ear.”
Id. Prior history of chickenpox was “unknown.” Id. Physical examination did not reveal any
rash or vesicles on her face or around her right ear. Id. at 29. Neurological examination revealed
the fifth (V)10 and seventh (VII) cranial nerves were abnormal on the right side. Id. Petitioner
was diagnosed with paresthesia and Bell’s palsy, prescribed acyclovir11 and steroids, and
magnetic resonance imaging (“MRI”) was ordered. Id. at 29-30. A brain MRI performed
without contrast on October 9 showed “[n]o significant intracranial abnormality.” Id. at 32.
On October 10, 2017, Petitioner’s employer submitted a report to the Vaccine Adverse
Event Reporting System (“VAERS”)12 on her behalf. Pet. Ex. 2. The adverse event was
described as facial paralysis and neck pain following the flu vaccine. Id. at 3. It reported that
Petitioner “woke up the night of [October 1, 2017] with pain in neck and left sided drooping[13]
which ha[d] not yet resolved.” Id. For the report, Petitioner reported to her employer that she
was diagnosed with Bell’s palsy. Id.
Petitioner returned to her PCP on October 11, 2017 “for evaluation of Bell’s palsy with
inability to smile and pain in right ear.” Pet. Ex. 3 at 33. Associated symptoms included
difficulty drinking, eating, and speaking, facial muscle weakness, “and pain near the ear, but no
blisters in or near the ear,[14] difficulty closing eye, drooping lower eyelid, drooling, hearing loss,
10 The fifth cranial nerve, or trigeminal nerve, “is sensory in supplying the face, teeth, mouth,
and nasal cavity, and motor in supplying the muscles of mastication.” Nervus Trigeminus,
Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/
dorland/definition?id=92428 (last visited Oct. 19, 2023)
11 Acyclovir is “a synthetic acyclic purine nucleoside with selective antiviral activity; it is active
against most known species of human herpesviruses, particularly against types 1 and 2, which
cause herpes simplex. It is used in the treatment of genital and mucocutaneous herpesvirus
infections; administered orally or topically.” Acyclovir, Dorland’s Med. Dictionary Online,
https://www.dorlandsonline.com/dorland/definition?id=833 (last visited Oct. 19, 2023)
12 VAERS is a “national early warning system to detect possible safety problems in [] vaccines”
co-managed by the Centers for Disease Control and Prevention (“CDC”) and the U.S. Food and
Drug Administration (“FDA”). About VAERS, https://vaers.hhs.gov/about.html (last visited
Oct. 19, 2023). “VAERS accepts and analyzes reports of adverse events (possible side effects)
after a person has received a vaccination. Anyone can report an adverse event to VAERS.
Healthcare professionals are required to report certain adverse events.” Id.
13 Reference to left side drooping appears to be an error, since all other records document
drooping of the right eye and right-sided symptoms.
14 Blisters or vesicles can be seen in Ramsay Hunt syndrome, and acute facial paralysis caused
by the herpes zoster virus. See Pet. Ex. 19 at 3.
6

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 7 of 42
lack of tears or sensitivity to light.” Id. Symptoms started 10 days prior. Id. Petitioner reported
“her [Bell’s] palsy [was] somewhat improving but she continue[d] to have pain above her right
ear [and] right side of face.” Id. It was noted that “[p]ossible contributing factors might include
[that she] received [f]lu shot at work [two] weeks ago.” Id. Neurologic examination showed
abnormal fifth and seventh cranial nerve function. Id. at 35. Diagnosis was Bell’s palsy. Id.
She was prescribed prednisone and tramadol for pain and was instructed to follow-up if there
were no improvements of symptoms in two weeks. Id.
At an optometry appointment in December 2017, Petitioner reported a “noticeable
decline or change in vision.” Pet. Ex. 5 at 4. Notes indicated Petitioner was “[r]eferred to Patti
Wieissler for acupuncture for [r]ight side [B]ell’s palsy [with] October 2017 onset.” Id. at 5.
On March 28, 2018, Petitioner followed up with her PCP. Pet. Ex. 3 at 40. Petitioner
reported she was “still having issues from her Bell’s palsy which was diagnosed on [October 4,
2017].” Id. Her ongoing symptoms included right eye twitching when she smiled, soreness on
the right side of her face, some hearing loss in her right ear, and occasional right eye blurry
vision. Id. Petitioner requested a neurology referral for further evaluation. Id. Petitioner also
requested a letter for her employer to be exempt from the annual flu vaccine. Id. She stated that
“her employer [would] be reporting her adverse reaction to the CDC.” Id. at 40, 44. Sonia
Villarreal, certified physician’s assistant (“PA-C”), wrote,
[Petitioner] received the [flu] vaccine at her place of employment on [September
21, 2017] then developed symptoms of Bell’s [p]alsy on [October 1, 2017]. She
was diagnosed with Bell’s [p]alsy on [October 4, 2017] when she saw one of our
other providers. Please exempt [Petitioner] from any future [flu] vaccines for her
employment since she is still dealing with complications since [October 2017].
Id. at 44.
Petitioner presented “with an eight month history of Bell’s palsy” to neurologist Dr. Peter
Tarbox for a neurological consultation on June 18, 2018. Pet. Ex. 7 at 1. History indicated that
“last year she received the flu vaccination and about a week after she developed right ear pain
and then numbness to the right tongue and then facial paralysis of the right side.” Id. She had
“numbness and tingling to the face and some dryness of her vision. She ha[d] decreased field
loss to the right.” Id. Petitioner reported she had “some recovery with some kinesis noted.” Id.
It was also noted she had “no significant lower [seventh] nerve recovery resulting with flattening
of the smile.” Id. Neurological examination showed “right peripheral VII [cranial nerve]
weakness on the right.” Id. at 3. “She [was] able to close her eyes but [did] have orbicularis
oculi eye weakness. She [was] [] able to elevate the right eyebrow. Her orbicularis oris
appear[ed] to be weak. She ha[d] some decreased sensitivity to touch subjectively in the right
VII [and eight cranial nerve regions].” Id. The remaining cranial nerves were intact. Id. Dr.
Tarbox’s impression was Bell’s palsy and polyneuropathy. Id. at 3-4.15 He recommended
15 On neurological examination, Dr. Tarbox also noted decreased sensitivity in the distribution of
the eighth cranial nerve. Pet. Ex. 7 at 3.
7

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 8 of 42
electrical stimulation, massages, and acupuncture. Id. at 4. Dr. Tarbox advised Petitioner that
given she was “eight to nine months [into] recovery there may be minimal significant recovery
from [her current] state,” but that nerve recovery was still possible for up to 18-months. Id.
On August 13, 2018, Petitioner followed up with Dr. Tarbox. Pet. Ex. 7 at 18. She
reported “no Bell’s palsy flare ups” since her last visit but continued to have “numbness and
tingling on [her] right side with a mild facial droop.” Id. Dr. Tarbox recommended Bell’s palsy
specific physical therapy. Id. at 20. Petitioner completed three sessions of physical therapy from
August 28 to September 11, 2018 with Amapola Mallari, physical therapist (“PT”). See Pet. Ex.
8 at 1-8.
Petitioner returned to her PCP on September 27, 2018. Pet. Ex. 3 at 45. She was still
experiencing a “drooping right eye, inability to smile, and pain in [her] right ear. Id. A
neurological examination showed abnormal fifth and seventh cranial nerve function. Id. at 46.
Petitioner requested a referral to an ear, nose, and throat (“ENT”) specialist. Id. at 47.
On September 28, 2018, Petitioner presented to ENT Dr. Walter Bain. Pet. Ex. 6 at 1.
History indicated she had hearing loss, taste decrease, and vertigo due to Bell’s palsy on October
3, 2017. Id. Examination showed a 50% reduction in strength on the right side of her face,
cerumen impaction, and mild bilateral sensorineural hearing loss with audiology measurements
in the normal range. Id. at 2-4.16
Petitioner had a speech evaluation on January 29, 2019. Pet. Ex. 40 at 1. She described
difficulty eating and drinking as well as pain when she moved the right side of her face. Id.
After reviewing her history and prior testing, the speech therapist ultimately determined that “no
speech therapy [was] recommended at [that] time” due to “very poor rehabilitative potential.”
Id. at 3.
On March 5, 2019, Petitioner presented Dr. Jackson, another ENT, for complaints of
dizziness, hearing loss and ear pain, pain swallowing, difficulty with speech, and facial
weakness. Pet. Ex. 38 at 1-3. History indicated Petitioner “developed weakness in the right side
of her face” in October 2017. Id. at 1. “She denied having evidence of shingles or other
symptoms when the facial weakness occurred, although she had undergone a flu shot [two]
weeks earlier.” Id. “She reported that her facial function improved about 50% over the ensuing
[three] months, but she was left with residual facial weakness.” Id. Dr. Jackson summarized
Petitioner’s onset of symptoms:
With the onset of facial weakness, she also noticed symptoms including right
eye/mouth dryness, right aural fullness, right tinnitus, and imbalance. She
reported right sided constant aural fullness. At onset of facial weakness, she
noticed temporary right sided hearing loss. She also [] noted that her right sided
hearing [] decreased when the aural fullness [was] severe. She reported
16 The audiogram showed mild relative elevation thresholds but were largely within normal
limits. Pet. Ex. 38 at 1.
8

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 9 of 42
intermittent dizziness described as imbalance. She reported that her dizziness []
occurred more in the morning and late afternoon. She reported her imbalance to
be mild severity, although it [] fluctuated in severity and [] worsen[ed] when her
right aural fullness [was] most pronounced. She reported right sided intermittent
tinnitus described as humming. She reported that the tinnitus [] occurred 1-2
times daily and [] lasted for seconds at a time. She reported right sided pain
below her right ear which radiate[d] to her jaw.
Id. He also noted Petitioner “reported allergy symptoms described as nasal congestion, nasal
discharge, postnasal drip, and eye dryness.” Id.
Petitioner’s examination by Dr. Jackson, including audiogram and tympanograms, was
normal. Pet. Ex. 38 at 2-5. House-Brackman17 grade was noted to be “II-III/VI” on the right
side. Id. at 4. Petitioner had another MRI which was normal. Id. at 8. The treatment plan
included further testing to find the cause of the dizziness and hearing symptoms. Id. at 5-6.
Facial physical therapy was also recommended. Id. at 5.
On October 2, 2019, Petitioner had an initial physical therapy examination with Diana
Schonoff, doctor of PT (“DPT”), at Garden Ridge Physical Therapy & Wellness Center. Pet. Ex.
45 at 1. It was noted that Petitioner got the flu vaccine on September 21, 2017, then two weeks
later, on October 1, 2017, developed “pain posterior [right] ear to jaw . . . then facial paralysis
[right] side.” Id. at 2. Petitioner reported she “did not go to [physical therapy] [] as
recommended but [she was] ready now.” Id. Petitioner’s chief complaints included pain,
swelling, and numbness in her right facial, ear, and neck region as well as issues with eating and
swallowing. Id. She reported feeling “self conscious eating or talking in front of people due to
synkinesis eye closure with mouth movements.” Id. House-Brackman was a grade III. Id. Dr.
Schonoff recommended physical therapy two to three times per week for a total of 18 sessions.
Id. at 3-4.
On October 23, 2020, Petitioner had a telehealth visit with Dr. Maria Alvarez of
Neurology Associates. Pet. Ex. 56 at 1. Petitioner reported she had Bell’s palsy since 2017. Id.
She reported an involuntary right face twitch that was “worse when she [was] tired” and a
“heaviness of [her] right face.” Id. Petitioner reported the involuntary twitch affected her speech
but did not cause any slurring or choking. Id. Dr. Alvarez noted “normal visual fields . . . mild
side face weakness, tongue motion normal, no slurring, no focal weakness, [and] no ataxia”18
17 The House-Brackmann facial nerve grading system is the most widely applied scoring system
“available to clinically assess the severity of peripheral facial nerve palsy.” Pet. Ex. 19 at 2. The
House-Brackman grading scale goes from Grade 1 (normal) to Grade 6 (total paralysis). Id. at 3
tbl.b.
18 Ataxia is “failure of muscular coordination; irregularity of muscular action.” Ataxia,
Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=4630
(last visited Oct. 19, 2023).
9

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 10 of 42
during Petitioner’s neurological examination. Id. at 2. The use of Botox injections and possible
gamma knife surgery was discussed. Id.19
Petitioner began Botox treatment in December 2020 and continued through March 2022.
Pet. Ex. 59 at 1, 3; Pet. Ex. 61 at 1, 3-4; Pet. Ex. 62 at 1-2, 5; Pet. Ex. 64 at 2. Petitioner reported
her facial spams were “stable” and getting “better with therapy.” Pet. Ex. 62 at 1; see also Pet.
Ex. 61 at 1.
On April 21, 2022, Petitioner had a yearly physical with Diana Lopez, advanced practice
registered nurse (“APRN”). Pet. Ex. 65 at 1. Nurse Lopez noted “cranial nerve [V] deficit”
during her neurological examination. Id.
No other relevant medical records were submitted.
D. Petitioner’s Declaration and Hearing Testimony
On May 25, 2020, Petitioner executed a declaration in response to comments in
Respondent’s expert’s reports questioning whether she had Ramsay Hunt syndrome. Pet. Ex. 46.
Throughout, she maintained her diagnosis was Bell’s palsy. Id. at 1-2.20
At the hearing, Petitioner testified she had been a nurse at Baptist Medical Center for 15
years prior to the flu vaccination at issue. Tr. 7-11. She recalled that prior to September 2017,
she was in good health. Tr. 12. She did not have any face, eye, or lip issues prior to the flu
vaccine besides needing reading glasses. Tr. 16.
Petitioner discussed the VAERS report submitted on her behalf by her employer. Tr. 12-
14. She testified the report stated that she had facial drooping on the left side, which was
inaccurate; instead, she had right-side facial drooping. Id. Additionally, Petitioner testified that
the employee health nurse advised her that she “should not get the flu vaccine since [she] got
Bell’s palsy after receiving the flu vaccine” and recommended she obtain an exemption letter
from her doctor. Tr. 24; see Pet. Ex. 3 at 44.
About two weeks after receiving her vaccination, Petitioner developed “a really sharp
pain behind [her] [right] ear” which was unusual. Tr. 14. She testified it was “really painful,”
and “something new to [her]” as it had never happened before. Tr. 15. She “had never been
seen by a physician for ear problems.” Id. On October 2, 2017, Petitioner went to work, because
she took some pain medicine and “the pain had subsided.” Id. When she got to work, she felt “a
little weird, tingling, [and] numbness . . . to the right side of [her] tongue.” Id. On October 3,
19 Botox was also recommended by plastic surgeon, Dr. Agustin Cornejo, in a March 2019
consultation to treat the asymmetry. Pet. Ex. 39 at 3.
20 Because the parties stipulated that Petitioner was properly diagnosed with Bell’s palsy, the
undersigned will not discuss this declaration further as it only pertains to the Ramsay Hunt
versus Bell’s palsy issue. See Joint Prehearing Submission at 1; Pet. Ex. 46.
10

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 11 of 42
Petitioner was off from work and when she woke up that morning, she noticed a drooping of her
face. Id. She was unable to brush her teeth without difficulty. Id. Her eye was also affected.
Id. Her face was paralyzed, “like frozen,” and she was unable to close her eye. Id.
Because Petitioner had seen Bell’s palsy before in the scope of her work as a nurse, she
thought she was having either Bell’s palsy or a stroke. Tr. 20. Accordingly, Petitioner recalled
that when she started experiencing these symptoms, she sought treatment from her PCP. Id. She
went to her PCP “the day after getting Bell’s palsy, so it was October 4, 2017.” Id. Petitioner
testified that the doctor asked her if she had blisters or herpes or any sores anywhere on her body
or facial area which Petitioner responded “no.”21 Tr. 22. Petitioner was given medication and
steroids. Id.
Petitioner recalled that she returned to her PCP on October 11, 2017 because her
condition was worsening. Tr. 22. She was having “a lot of dryness to [her] eye, dryness to [her]
mouth, . . . a lot of pain, [and] a lot of spasms, like charley horses [in] back of [her] ear to the jaw
area, pulling of [her] neck.” Id. She had problems eating and drinking, drooling, and sensitivity
of her ear and right side. Tr. 22-23. Because she was not able to close her eye, it was dry and
irritated. Tr. 23. She developed blurred vision and used lubricating ointment and eyedrops. Id.
Petitioner wore an eye mask at night to sleep and when she showered, she put a towel band over
her eye to prevent soap from getting into her eye. Tr. 24.
In her testimony, Petitioner stated that her final diagnosis was Bell’s palsy. Tr. 23. She
testified that her treating physicians “did not see any blisters, any sores” and so they believed the
cause was “possibl[y] [the] flu vaccine.” Id. She saw a neurologist in June 2018 due to
continued symptoms. Tr. 25. Recommended treatment included physical therapy, Botox, and
acupuncture. Tr. 25-26. Petitioner underwent all of the recommended treatment. Id. Petitioner
also described the photographs filed showing the effect of Bell’s palsy on her facial appearance.
Tr. 17-19.
As of the date of the hearing, October 18, 2022, Petitioner was still experiencing
“synkinesis, [] blurriness, and vision problems.” Tr. 26. She was still unable to completely close
her eye and had continued dryness of her eye and mouth. Id. She also had difficulty chewing
food and had spasms of the right side of her face. Id.
E. Expert Reports
1. Petitioner’s Expert, Dr. Lawrence Steinman22
21 Petitioner testified that despite the records indicating such, she was not asked about a prior
history of chickenpox. Tr. 21; see Pet. Ex. 3 at 27. If she had been asked, Petitioner would have
answered that she did have chicken pox when she was between the age of seven and eight years
old. Tr. 21.
22 Dr. Steinman submitted four expert reports in this matter and testified at the entitlement
hearing. Pet. Exs. 10, 47, 75, 83; Tr. 3, 145.
11

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 12 of 42
a. Background and Qualifications
Dr. Steinman is board certified in neurology and has practiced neurology at Stanford
University for over 40 years. Pet. Ex. 10 at 1; Pet. Ex. 11 at 2. He received his B.A. from
Dartmouth College in 1968 and his M.D. from Harvard University in 1973. Pet. Ex. 11 at 1.
Thereafter, he completed an internship in surgery, a residency in pediatrics, and a residency in
pediatric and adult neurology from Stanford University Hospital, as well as three fellowships.
Id. He currently works as a Professor at Stanford University. Id. Dr. Steinman is also “actively
involved in patient care” and has cared for hundreds of adults and children with various
neuroinflammatory diseases, including Bell’s palsy, transverse myelitis, Guillain-Barré
syndrome (“GBS”),23 acute disseminated encephalomyelitis, neuromyelitis optica, and multiple
sclerosis. Pet. Ex. 10 at 1; see also Tr. 59. He has authored or co-authored over 500
publications. Pet. Ex. 11 at 5-47.
b. Opinion
Dr. Steinman opined “to a high degree of medical certainty and by a preponderance of
evidence,” the contents of the flu vaccine Petitioner received on September 21, 2017, through the
mechanism of molecular mimicry, triggered Petitioner’s Bell’s palsy ten days post-vaccination.
Pet. Ex. 10 at 1; see also Tr. 61. He offered several mimics to explain how the flu vaccine can
trigger an immune cross-reaction and cause Bell’s palsy. Pet. Ex. 10 at 17.
i. Althen Prong One
The mechanistic theory proposed by Dr. Steinman for how the flu vaccine can cause
Bell’s palsy was molecular mimicry. Pet. Ex. 10 at 6. He explained, molecular mimicry is the
concept whereby “shared structures on a virus or bacteria or in a vaccine can trigger a cross-
reactive response to self[-antigens].” Id. (citing Pet. Ex. 24 at 3).24 “In some people, . . . a
foreign antigen may resemble antigen produced by the body. Such molecular mimicry provokes
the T cells to attack the body tissues that contain the self-antigens.” Pet. Ex. 24 at 3.
In support of his theory generally, Dr. Steinman first described Bell’s palsy and
compared it with GBS. Tr. 63-64. Dr. Steinman described Bell’s palsy as “an inflammatory
disease of the facial nerve” and like GBS, is an “acute demyelinating disease of the peripheral
nervous system.” Tr. 61; Pet. Ex. 19 at 4. “In most cases, Bell’s palsy is a mononeuritic variant
23 GBS is a “rapidly progressive ascending motor neuron paralysis of unknown etiology,
frequently seen after an enteric or respiratory infection. An autoimmune mechanism following
viral infection has been postulated.” Guillain-Barré Syndrome, Dorland’s Med. Dictionary
Online, https://www.dorlandsonline.com/dorland/definition?id=110689 (last visited Oct. 19,
2023); see also Pet. Ex. 19 at 1 (describing GBS as a neurologic disorder with a recognized “cell-
mediated immunity against peripheral nerve myelin antigens”).
24 Lawrence Steinman, Autoimmune Disease, 269 Sci. Am. 107 (1993).
12

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 13 of 42
of [GBS].” Pet. Ex. 19 at 4; see also Tr. 63-64 (testifying there is strong evidence suggesting
Bell’s palsy is a manifestation of a peripheral neuropathy). While Dr. Steinman acknowledged
the cause of Bell’s palsy remains unknown, viral infections or an autoimmune process have been
postulated. Pet. Ex. 10 at 5 (citing Pet. Ex. 19 at 1). Greco et al. explained that Bell’s palsy and
GBS may share a similar etiology and pathogenesis, which includes an “autoimmunity cell-
mediated reaction against a protein of the peripheral nerve myelin.” Pet. Ex. 19 at 1, 5; see also
Pet. Ex. 53 at 1 (providing a general overview of three potential mechanisms for viral induced
autoimmune diseases: molecular mimicry, bystander activation and persistent virus infection).25
Accordingly, Dr. Steinman intermittently referred to GBS literature in support of molecular
mimicry.
Dr. Steinman proposed two separate and independent “pillars” or theories to illustrate
how molecular mimicry could trigger Bell’s palsy following flu vaccination. Pet. Ex. 10 at 7; Tr.
64-65. He described how the contents of the flu vaccine “share structural similarities with the
proteins glycolipids in the facial nerve including gangliosides and the P2 protein.” Pet. Ex. 10 at
6, 16.26 Thus, his two theories are based on homology between components of the flu vaccine
with (1) gangliosides in the peripheral nerve myelin and (2) with P2 protein of the peripheral
myelin.
1. Ganglioside Theory
Dr. Steinman’s first proposed theory is that the Flucelvax[27] vaccine “likely triggered an
anti-ganglioside immune response leading to Bell’s [p]alsy, due to the presence of an H1N1
component.” Pet. Ex. 10 at 7 (emphasis omitted).
At the hearing, Dr. Steinman opined that gangliosides are recognized as a component in
the flu vaccine that could trigger GBS. Tr. 67. In support of this opinion, he cited the Institute
of Medicine’s (“IOM”)28 acknowledgment that “the ganglioside molecular mimicry theory” is
“the premier example of how something in a vaccine could cause . . . [GBS].” Id. (citing Pet. Ex.
25 Robert S. Fujinami et al., Molecular Mimicry, Bystander Activation, or Viral Persistence:
Infections and Autoimmune Disease, 19 Clinical Microbiology Revs. 80 (2006).
26 According to Dr. Steinman, the peripheral nerve protein, P1L, is now known as P2 peripheral
myelin protein. Pet. Ex. 10 at 6; Tr. 231-33.
27 The flu vaccine Petitioner received was the 2017-2018 Flucelvax. Pet. Ex. 1 at 1; see Pet. Ex.
84 (package insert).
28 Inst. of Med., Evaluating Biological Mechanisms of Adverse Events, in Adverse Effects of
Vaccines: Evidence and Causality 57 (Kathleen Stratton et al. eds., 2012). The IOM is now the
National Academy of Medicine.
13

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 14 of 42
18 at 99-101). He noted Ang et al.29 published one of the first papers asserting that molecular
mimicry plays a role in inflammatory neuropathy. Pet. Ex. 10 at 7 (citing Pet. Ex. 25). They
showed that a ganglioside antibody from the bacteria Campylobacter jejuni (“C. jejuni”)30 was
detected in GBS. Id. (citing Pet. Ex. 25 at 1). The ganglioside antibody was also found in
patients with Miller Fisher syndrome31 “where the facial nerve is often targeted.” Id. (citing Pet.
Ex. 25 at 1).
Dr. Steinman explained that while gangliosides are not proteins (they consists of sugar
and lipid components), “they bind to proteins and they glycosylate[32] proteins in the nervous
system.” Tr. 208. As such, gangliosides are myelin carbohydrates. Pet. Ex. 10 at 7. Ang et al.
concluded that “molecular mimicry between C. jejuni [lipopolysaccharides] and gangliosides
plays a key role in the induction of antiganglioside antibodies and neurological symptoms in
patients with GBS and [Miller Fisher syndrome].” Pet. Ex. 25 at 6; see also Pet. Ex. 27 at 1
29 C.W. Ang et al., Structure of Campylobacter jejuni Lipopolysaccharides Determines
Antiganglioside Specificity and Clinical Features of Guillain-Barré and Miller Fisher Patients, 70
Infection & Immunity 1202 (2002).
30 Dr. Steinman testified that C. jejuni is a “gastrointestinal bacteria known to be associated with
[GBS], and like many bacteria, it has ganglioside, and we have in our nervous system
ganglioside.” Tr. 66.
31 Miller Fisher syndrome is “a variant of [GBS] characterized by areflexia, ataxia, and
ophthalmoplegia.” Fisher Syndrome, Dorland’s Med. Dictionary Online,
https://www.dorlandsonline.com/dorland/definition?id=110608 (last visited Oct. 19, 2023).
Areflexia is the “absence of reflexes.” Areflexia, Dorland’s Med. Dictionary Online,
https://www.dorlandsonline.com/dorland/definition?id=4035 (last visited Oct. 19, 2023).
Ophthalmoplegia is the “paralysis of the eye muscles.” Ophthalmoplegia, Dorland’s Med.
Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=35269 (last visited
Oct. 19, 2023).
32 Glycosylation is “the formation of linkages with glycosyl groups.” Glycosylation, Dorland’s
Med. Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=20670 (last
visited Oct. 23, 2023); see also Tr. 173 (Respondent’s expert, Dr. Whitton, testifying that
glycosylation “just means adding sugars to”).
14

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 15 of 42
(indicating that the anti-GQ1b antibodies33 found in patients with Miller Fisher syndrome and
other related conditions may be “due to the different expression of gangliosides in different parts
of the nervous system”);34 Pet. Ex. 28 at 2-3 (noting ganglion involvement in isolated cranial
neuropathies like Bell’s palsy).35
Dr. Steinman cited medical articles that examined whether flu vaccines could elicit anti-
ganglioside responses in the absence of C. jejuni. Nachamkin et al.36 found that vaccines
containing H1N1 induced anti-GM1 antibodies37 in mice. Pet. Ex. 26 at 1, 5. They also found
antibody responses to hemagglutinin; a viral surface glycoprotein found in H1N1. Id. They
determined hemagglutinin could bind to cellular gangliosides and mimic an anti-ganglioside
antibody using the 1976 swine flu vaccine, which contained H1N1. Id.; see also Tr. 66. While
Dr. Steinman acknowledged that Nachamkin et al. did not test the 2017-2018 flu vaccine, he
explained that the 2017-2018 flu vaccine contained H1N1 component like the vaccine studied by
Nachamkin et al. Pet. Ex. 10 at 7; see Pet. Ex. 23 at 2.38 Dr. Steinman also cited An et al.,39
which provided that the manner in which hemagglutinin is glycosylated may impact immune
processing leading to molecular mimicry. Pet. Ex. 50 at 1.
33 Anti-GQ1b IgG antibodies are immune markers for Miller Fisher syndrome and GBS. See
Pet. Ex. 28 at 1. “A common role of serum GQ1b antibodies in the pathogenic mechanism of
these conditions have been supported by a study of the ganglioside composition of human cranial
nerves that reveal a high concentration of GQ1b epitopes in the paranodal region and Ranvier
nodes of the extramedually parts, particularly of the III, IV, and V [cranial] nerves.” Id. at 2.
Nodes of Ranvier are “constrictions occurring on myelinated nerve fibers at regular intervals of
about 1 mm; at these sites the myelin sheath is absent and the axon is enclosed only by Schwann
cell processes.” Nodes of Ranvier, Dorland’s Med. Dictionary Online,
https://www.dorlandsonline.com/dorland/definition?id=93095 (last visited Oct. 19, 2023).
34 Y. Fukami et al., Anti-GQ1b Antibody Syndrome: Anti-Ganglioside Complex Reactivity
Determines Clinical Spectrum, 23 Eur. J. Neurology 320 (2016).
35 Filippo Greco et al., Recurrent Facial Nerve Palsy Associated with Anti-GQ1b IgG
Antibodies, 30 Brain & Development 606 (2008).
36 Irving Nachamkin et al., Anti-Ganglioside Antibody Induction by Swine (A/NJ/1976/H1N1)
and Other Influenza Vaccines: Insights into Vaccine-Associated Guillain-Barré Syndrome, 198 J.
Infectious Diseases 226 (2008).
37 Ganglioside GM-1 is “one of several gangliosides considered a target antigen in the
pathogenesis of GBS.” Pet. Ex. 26 at 5.
38 U.S. Food & Drug Admin., Influenza Virus Vaccine for the 2017-2018 Season, (last updated
Nov. 30, 2017).
39 Yanming An et al., N-Glycosylation of Seasonal Influenza Vaccine Hemagglutinins:
Implication for Potency Testing and Immune Processing, 93 J. Virology e01693 (2019).
15

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 16 of 42
The vaccines studied by Nachamkin et al. were egg-based. Tr. 66; Pet. Ex. 26 at 2. Dr.
Steinman testified that the research showed “in the rich environment of an egg growing [flu]
virus, that the [flu] proteins, like the hemagglutinin and neuraminidase, get glycosylated.” Tr.
88. Dr. Steinman explained that the 2017-2018 Flucelvax vaccine was not egg-based but instead
grown from canine kidney cells. Tr. 66-67; Pet. Ex. 84 at 10. Dr. Steinman testified that “canine
kidney cells are very good at glycosylating. Tr. 67. Thus, Dr. Steinman opined that an egg-
based vaccine was not required for molecular mimicry. Id. Likewise, he opined that C. jejuni
was not needed. Id. In fact, he believed that canine kidney cells are “even better than the egg
cultures at glycosylating the [flu] proteins.” Tr. 86-87.40 Dr. Steinman concluded that “[a]
ganglioside is a ganglioside whether the chemistry is in a chicken egg or a canine kidney cell or a
human cell.” Pet. Ex. 47 at 4; see also Tr. 89 (“A ganglioside from a dog is the same as a
ganglioside from a chicken.”).
Accordingly, Dr. Steinman opined that a human getting a flu vaccine can “mount a
response to ganglioside” and that “anti-ganglioside antibodies are associated with facial nerve
palsy.” Tr. 210-11; Pet. Ex. 10 at 7 (citing Pet. Exs. 19, 27);41 see also Pet. Ex. 18 at 101.
2. P2 Protein Theory
The second theory proposed by Dr. Steinman is that there is molecular mimicry between
components of the flu vaccine and the P2 protein in myelin. Pet. Ex. 10 at 7. Dr. Steinman
opined that “P2 is attacked in Bell’s palsy.” Tr. 56.
Dr. Steinman cited Abramsky et al.42 to show that “[i]mmune responses to P2 have been
associated with Bell’s [p]alsy [] and inflammatory neuropathy” thus supporting a cell-mediated
autoimmune mechanism in Bell’s palsy. Pet. Ex. 10 at 6-7 (citing Pet. Ex. 20 at 1, 4 fig.1).
Abramsky et al. “demonstrated a defined in vitro response to a human basic protein [] of
peripheral nerve myelin in patients with Bell’s palsy” resulting in immunologic lymphocyte
alterations. Pet. Ex. 20 at 5. This response suggests that the sensitization of lymphocytes to the
self-protein “may be an important factor in the pathogenesis of the paralysis.” Id. at 7.
The human basic protein in peripheral nerve protein discussed in Abramsky et al. was
referred to as the P1L protein. See Pet. Ex. 20 at 5. According to Dr. Steinman, the P1L protein
described in Abramsky et al. is now known as the P2 peripheral myelin protein. Pet. Ex. 10 at 6;
Tr. 231-33. To explain this change, Dr. Steinman cited a paper he co-authored that was
40 For more discussion on the foundation for this opinion, see Tr. 87-88; Pet. Ex. 47 at 4; Pet. Ex.
50 at 10, 12 tbl.3; Pet. Ex. 49 at 1.
41 Y. Fukami et al., Anti-GQ1b Antibody Syndrome: Anti-Ganglioside Complex Reactivity
Determines Clinical Spectrum, 23 Eur. J. Neurology 320 (2016).
42 O. Abramsky et al., Cellular Immune Response to Peripheral Nerve Basic Protein in Idiopathic
Facial Paralysis (Bell’s Palsy), 26 J. Neurological Sci. 13 (1975).
16

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 17 of 42
published in 1981. Tr. 57-58; Pet. Ex. 22 at 1.43 In the study, Dr. Steinman and colleagues
immunized rats of different genetic backgrounds with the P2 protein to show that the P2 protein
can cross paths with the flu vaccine to cause cranial nerve damages. Tr. 58; Pet. Ex. 22 at 1.
Their findings can be summarized as follows:
Experimental allergic neuritis (EAN) is an inflammatory demyelinating peripheral
neuropathy induced by immunization against components of peripheral nervous
system [] myelin. EAN appears after immunization of the Lewis rat with purified
[peripheral nervous system] myelin from many other species. Myelin of the
[peripheral nervous system] contains two major basic proteins: P1 protein
(molecular weight, 18,000) is similar or identical to central nervous system (CNS)
myelin basic protein, the encephalitogen responsible for experimental allergic
encephalomyelitis (EAE). A smaller basic protein, P2 (molecular weight,
12,000), has an amino acid composition unrelated to P1. The critical antigen
responsible for the induction of EAN is P2.
Pet. Ex. 22 at 1.
Accordingly, Dr. Steinman explained that the change of nomenclature from P1 to P2 is
based on molecular weights of the proteins and one of the proteins, P1L, is not in the peripheral
nervous system. Tr. 236. Further, the authors of the 1981 paper found that the critical antigen
responsible for induction of EAN was the P2 protein. Id.; Pet. Ex. 22 at 1; see also Pet. Ex. 86 at
1 (suggesting the P2 protein is the antigen responsible for EAN).44
Following the hearing, Dr. Steinman submitted a supplemental report and literature to
further clarify the nomenclature issue of P1L protein and P2 protein. See Pet. Exs. 83-88. He
explained the “species of the P2 is [] important in assigning what molecular weight the P2
protein has, since the P2 proteins are of varying lengths and amino acid composition from
species to species.” Pet. Ex. 83 at 3. Citing Kadlubowski and Hughes,45 Dr. Steinman wrote that
P1 refers to myelin basic protein with a molecular weight of 18,000, and P2 refers to myelin
basic protein with molecular weights of 12,000-14,000, “depending on the species.” Id. (citing
Pet. Ex. 88 at 1).
According to Dr. Steinman, Kadlubowski and Hughes “report[ed] the ‘issues’
surrounding P1L[] that led to its renaming of P2.” Pet. Ex. 83 at 3. They wrote, “[o]f the two
43 Lawrence Steinman et al., Genetic Control of Susceptibility to Experimental Allergic Neuritis
and the Immune Response to P2 Protein, 31 Neurology 950 (1981).
44 S.W. Brostoff & E.H. Eylar, The Proposed Amino Acid Sequence of the P1 Protein of Rabbit
Sciatic Nerve Myelin, 153 Archives Biochemistry & Biophysics 590 (1972).
45 M. Kadlubowski & R.A.C. Hughes, Identification of the Neuritogen for Experimental Allergic
Neuritis, 277 Nature 140 (1979).
17

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 18 of 42
basic proteins in peripheral myelin, P1 has been shown to be the same as the encephalitogenic[46]
basic protein in the rabbit sciatic nerve, and this is likely to be the same for other species.” Pet.
Ex. 88 at 2; see also Pet. Ex. 86 at 1. “Thus, attention has focused on the other basic protein, P2,
which may be specific to peripheral nerve myelin.” Pet. Ex. 88 at 2. All were ultimately
unsuccessful, suggesting that “isolation might lead to an alteration in the considerable secondary
structure of P2.” Id. Additional papers explored the P2 protein,47 and ultimately were “able to
isolate P2 in a form which is neuritogenic.” Id. Brostoff et al.48 also studied P2 as the myelin
basic proteins in the peripheral nervous system. Pet. Ex. 87 at 1. “Another, smaller basic protein
([molecular weight] 12,000) is almost always present as well in [peripheral nervous system]
myelin. This smaller protein, referred to as the P2 protein, seems to be a unique [peripheral
nervous system] protein with no relationship to the larger basic protein.” Id. (internal citations
omitted).49 After a review of the relevant studies and findings, Dr. Steinman concluded that
“P1L, the neuritogenic protein that triggered Bell’s palsy” in Abramsky et al. was renamed to P2.
Pet. Ex. 83 at 4.
After verifying “that P2 is targeted in Bell’s palsy,” Dr. Steinman used a three-step
process to identify protein sequences that could implicate molecular mimicry between the flu
vaccine and the P2 antigen. Tr. 69; see Tr. 212, 215; Pet. Ex. 47 at 7-8. First, Dr. Steinman
conducted a BLAST50 search to determine whether there was any similarity, or sequence
homology, between the components of the 2017-2018 Flucelvax vaccine and the myelin protein
P2. Tr. 69; see also Pet. Ex. 10 at 7, 10.51 Dr. Steinman started by looking at one of the proteins
46 Dr. Steinman opined encephalitogenic means “it is in the brain.” Pet. Ex. 83 at 4.
47 S.W. Brostoff et al., Induction of Experimental Allergic Neuritis with a Peptide from Myelin
P2 Basic Protein, 268 Nature 752 (1977). This article was not filed.
48 S.W. Brostoff et al., The P2 Protein of Bovine Root Myelin: Partial Chemical
Characterization, 24 J. Neurochemistry 289 (1975).
49 For additional discussion of the P1L and P2L issue, see Pet. Ex. 83 at 3-4; Tr. 237; Pet. Ex. 20
at 3.
50 A BLAST (Basic Local Alignment Search Tool) search “finds regions of similarity between
biological sequences. The program compares nucleotide or protein sequences to sequence
databases and calculates the statistical significance.” BLAST, https://blast.ncbi.nlm.nih.gov/Blast
.cgi (last visited Sept. 8, 2023). Dr. Steinman testified that this cannot be done with regard to his
ganglioside theory because a “BLAST search is suitable for seeing the similarity between one
protein and another,” not for a sugar. Tr. 68.
51 For a complete explanation of Dr. Steinman’s investigation, including his discussion on the
number of amino acids required for homology relevant to molecular mimicry as well as the
procedure he followed in conducting his BLAST searches, see Pet. Ex. 10 at 7-15; Pet. Ex. 47 at
7-12; Pet. Ex. 75 at 1-4; Tr. 73, 217-18
18

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 19 of 42
in the flu vaccine, hemagglutinin. Tr. 73-74; see also Pet. Ex. 23 at 2.52 He found “a 5 of 11
exact homology[53] in amino acids for the P2 protein and a component of hemagglutinin of the
[flu] A virus (A/Michigan/45/2015(H1N1)) found in the 2017-2018 [flu] vaccine.” Pet. Ex. 10 at
10; see also Tr. 69-70, 73. He also found another component of the vaccine had sequence
homology with the P2 protein,54 and noted that not all components of the 2017-2018 flu vaccine
do. Pet. Ex. 10 at 11-12; Tr. 73-74.
Next, Dr. Steinman filtered the areas of alignment between the vaccine and the myelin
protein P2 from the BLAST search and “eliminate[d] sequence homologies that [were] below a
threshold that ha[d] been shown to induce neuroinflammation with clinical symptoms like
paralysis in the [experimental encephalomyelitis (“EAE”)] model.” Pet. Ex. 47 at 7. Relying on
medical literature, Dr. Steinman opined the sequence he found was significant due to the
presence of five identical amino acids in a longer sequence. Pet. Ex. 10 at 11; Pet. Ex. 75 at 1-3;
Tr. 70. For support, he cited Lanz et al.,55 which found five out of 12 identical amino acids for
molecular mimicry between Epstein-Barr virus and multiple sclerosis. Pet. Ex. 76 at 1; Tr. 216,
218-19.
Additionally, studies by Gautam et al. found “[five] of 12 amino acids, not even
consecutive amino acids, was sufficient to trigger [EAE].” Pet. Ex. 10 at 7 (citing Pet. Ex. 29 at
52 Dr. Steinman testified that hemagglutinin and neuraminidase are the H and N of H1N1. Tr.
74.
53 The five identical amino acids Dr. Steinman identified were YKLAT, with YVKSTKLRLAT
as the sequence for the hemagglutinin component of the vaccine and YMKALGVGLAT as the
sequence for the peripheral myelin protein 2. Pet. Ex. 10 at 11.
54 “Another homology of similar significance is found in the B Brisbane component and the P2
protein, where the sequence LSTQNVIDAEKA has five of 12 identical amino acids.” Pet. Ex.
10 at 11-12.
55 Tobias V. Lanz et al., Clonally Expanded B Cells in Multiple Sclerosis Bind EBV EBNNA1
and GlialCAM, 603 Nature 321 (2022). Dr. Steinman is a named author in this paper.
19

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 20 of 42
1;56 Pet. Ex. 30 at 1;57 Pet. Ex. 31 at 1);58 see also Tr. 46-47. Therefore, Dr. Steinman
determined the “[five] of 11 identical amino acids between a component of the vaccine and P2
protein . . . [was] very likely sufficient to trigger clinically relevant inflammation in peripheral
nerve.” Pet. Ex. 10 at 11 (emphasis omitted); see also Pet. Ex. 47 at 6; Tr. 70.
Dr. Steinman disagreed with Respondent’s expert, Dr. Whitton, who asserted that much
longer sequences (of 80 amino acids) were required for homology based on the paper by
Silvanovich et al.59 Tr. 214-18 (citing Resp. Ex. C, Tab 10); see also Tr. 176. Instead, Dr.
Steinman opined that the immune system interacts with shorter sequences of amino acids. See
Tr. 214-18. Further, Dr. Steinman explained that Silvanovich et al. pertained to allergic
responses not immune system responses, and thus, it was not relevant. Tr. 93-94; Pet. Ex. 10 at
13. Additionally, Dr. Steinman noted that Silvanovich et al. endorsed the use of BLAST
searches. Tr. 94.60
The third step of his process “retains those peptide sequences identified in the first two
steps, only if they have been identified by other investigators using one and/or two other US
government databases.” Pet. Ex. 47 at 7. Dr. Steinman searched the sequence,
YVKSTKLRLAT, which had 5 of 11 identical amino acids between a component of the vaccine
and P2 protein in the Immune Epitope DataBase (“IEDB”).61 Pet. Ex. 47 at 9; Tr. 75, 213-15.
56 Anand M. Gautam et al., A Viral Peptide with Limited Homology to a Self Peptide Can Induce
Clinical Signs of Experimental Autoimmune Encephalomyelitis, 161 J. Immunology 60 (1998).
Dr. Steinman is a named author in this paper.
57 Anand M. Gautam et al., Minimum Structural Requirements for Peptide Presentation by Major
Histocompatibility Complex Class II Molecules: Implications in Induction of Autoimmunity, 91
Immunology 767 (1994). Dr. Steinman is a named author in this paper.
58 Anand M. Gautam et al., A Polyalanine Peptide with Only Five Native Myelin Basic Protein
Residues Induces Autoimmune Encephalomyelitis, 176 J. Experimental Med. 605 (1992). Dr.
Steinman is a named author in this paper.
59 Andre Silvanovich et al., The Value of Short Amino Acid Sequence Matches for Prediction of
Protein Allergenicity, 90 Toxicological Scis. 252 (2006).
60 Silvanovich et al. stated that BLAST searches “rank the similarity of a query protein to its
corresponding matches and provide a measure of the reliability of the alignment.” Resp. Ex. C,
Tab 10 at 7.
61 The IEDB “catalogs experimental data on antibody and T cell epitopes studied in humans,
non-human primates, and other animal species in the context of infectious disease, allergy,
autoimmunity and transplantation. The IEDB also hosts tools to assist in the prediction and
analysis of epitopes.” Immune Epitope Database and Analysis Resource, https://www.iedb.org/
(last updated Sept. 3, 2023). The IEDB is a freely available resource funded by the National
Institute of Allergy and Infectious Diseases. Id.
20

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 21 of 42
The sequence appeared in the IEDB, which Dr. Steinman asserted was evidence that it was an
epitope that had been reported in humans. Pet. Ex. 47 at 8-9; see also Tr. 215. The epitope also
appeared in Influenza Research Database (“IRD”).62 Pet. Ex. 47 at 7, 9-10. Dr. Steinman
testified that because it was reported in the IEDB and IRD, this indicated that “others have
looked at that sequence that was identified and . . . studied it.” Tr. 75; see also Tr. 214-15.
“Other immunologists show that this is actually recognized by the immune system when they’re
looking at hemagglutinin, [and the] similarity between P2 and the hemagglutinin.” Tr. 75; see
also Pet. Ex. 47 at 9.
After explaining his two theories, Dr. Steinman acknowledged the limitations to this
process of illustrating molecular mimicry and sequence homology. See, e.g., Pet. Ex. 75 at 2, 5-
6.63 However, because he was unable to perform research on the Petitioner, and because there is
“no animal model for Bell’s palsy,” he asserted that his “three steps of filtration using peer
reviewed journals . . . three different US government-financed search tools (BLAST, IEDB, and
IRD) make a compelling theory that molecular mimics in the [flu] vaccine received by
[P]etitioner could trigger immunity to P2 myelin protein.” Pet. Ex. 47 at 12 (emphasis omitted);
see also Tr. 48. He emphasized that his opinions that there are “homologies with antigens that
are homologous mimics of the vaccine and that are targeted in Bell’s palsy” are based on
Abramsky et al., Winer et al.,64 Steinman et al., and the criteria from Gautam et al. Pet. Ex. 47 at
12 (citing Pet. Exs. 20-22, 29-31).
Dr. Steinman also opined that “it takes more than a molecular mimic to trigger a disease.
[Steinman et al.] says you have to have the right genes.” Tr. 58 (citing Pet. Ex. 22 at 5). “Other
genetic and environmental factors are necessary before these self-reactive immune responses to
myelin might trigger conditions like Bell’s palsy.” Pet. Ex. 10 at 15-16. Still, he opined
molecular mimicry is important in “trying to understand how something can be triggered by a
vaccine or by a virus.” Tr. 58.
3. Medical Literature and Case Reports
In further support of his opinions, Dr. Steinman cited studies and case reports on the
association between the flu vaccine and Bell’s palsy. See Pet. Ex. 75 at 6-7. Several of the
studies cited by Dr. Steinman acknowledge finding a signal or increased risk of Bell’s palsy after
administration of the flu vaccination. Id.
62 The IRD “is a US NIH/NIAID-funded, freely-available online bioinformatics resource for
influenza virus data search, analysis and visualization.” Richard H. Scheuermann, Influenza
Research Database (IRD), J. Craig Venter Institute, https://www.jcvi.org/research/influenza-
research-database-ird (last visited Oct. 23, 2023); see also Bacterial and Viral Bioinformatics
Resource Center, https://www.bv-brc.org/ (last visited Oct. 23, 2023).
63 For the limitations acknowledged by Dr. Steinman, see Tr. 51-52, 74-77.
64 J.B. Winer et al., A Prospective Study of Acute Idiopathic Neuropathy. I. Clinical Features
and Their Prognostic Value, 51 J. Neurology Neurosurgery & Psychiatry 605 (1988).
21

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 22 of 42
Zhou et al. reviewed and analyzed VAERS reports between 1991 and 2001 to determine
whether there was an association between Bell’s palsy and the flu vaccine. Pet. Ex. 73 at 1-2.65
The authors identified 197 possible cases of Bell’s palsy after receipt of a flu vaccine. Id. Of the
197 reports, Bell’s palsy diagnosis was verified in 154, and among those, 145 cases received the
flu vaccine alone. Id. The authors concluded there “may be a signal of possible association
between [flu] vaccines and an increased risk of Bell’s palsy.” Id. at 5. They noted the etiology
and pathogenesis of Bell’s palsy is not clear, but that there is “concern that latent [HSV-1]
infections of the geniculate ganglia of facial nerves may be one of the causes of Bell’s palsy” and
that “[i]mmune response mechanisms have also been considered.” Id.
Bardage et al.66 was a population-based study in Sweden with H1N1 vaccine (Pandemrix)
from October 2009 and March 2010 which reported an increased risk of Bell’s palsy. Pet. Ex. 67
at 2, 4. The authors found “a significantly increased risk for Bell’s palsy” in “those vaccinated in
the early phase of the vaccination campaign (≤ 45 days), when high risk groups predominated.”
Id. at 4. “In contrast, among people vaccinated after the first 45 days of the campaign,
representing more closely the general population, [they] found no statistically significant
associations between vaccination and autoimmune or neurological diseases.” Id. The authors
concluded that they “[could not] explain the small increase in risk for Bell’s palsy seen in this
study.” Id. at 5.
Next, Dr. Steinman cited a recent 2020 study authored by Kamath et al.67 who “analyzed
[VAERS] data to determine whether the facial paralysis reporting rate is higher in those who
received the [flu] vaccination compared with those who received other vaccines.” Pet. Ex. 70 at
1. The authors evaluated VAERS reports from January 2015 to October 2019 and identified 250
reports of facial paralysis in patients who received flu vaccines and 346 reports of facial
paralysis for all other vaccines. Id. at 3. “[Their] study show[ed] that the likelihood of reporting
facial paralysis following [flu] vaccination [was] higher compared with other vaccines.” Id. at 4.
The authors found an onset median of three (range of 1-10) days but noted “the number of
65 Zhou et al. also acknowledged the issues and limitations with VAERS, stating, in relevant part,
“[d]ata from VAERS should be interpreted with caution because they represent adverse events
that occurred after vaccination, not all of which may have been caused by vaccination. Temporal
association alone does not mean that the vaccine caused the illness or symptoms.” Pet. Ex. 73 at
5.
66 Carola Bardage et al., Neurological and Autoimmune Disorders After Vaccination Against
Pandemic Influenza A (H1N1) with a Monovalent Adjuvanted Vaccine: Population Based
Cohort Study in Stockholm, Sweden, 343 BMJ 1 (2011).
67 Ashwin Kamath et al., Facial Paralysis Following Influenza Vaccination: A Disproportionality
Analysis Using the Vaccine Adverse Event Reporting System Database, 20 Clinical Drug
Investigation 883 (2020). Like the authors in Zhou et al., the authors acknowledged the
limitations in their findings, including the “inherent limitations of the VAERS database analysis
and the fact that disproportionality measures only indicate the presence of a signal.” Pet. Ex. 70
at 4-6.
22

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 23 of 42
patients for whom the time of onset data were recorded was limited.” Id. at 5. Most of the cases
of facial paralysis occurred within the first two weeks following vaccination with the seasonal
trivalent or quadrivalent intramuscular flu vaccine. Id. at 6. They noted “[t]he appearance of
Bell’s palsy after the vaccination supports the immunological hypothesis.” Id. at 4.
Lastly,68 Dr. Steinman cited Huang et al.,69 who used a “capture-recapture method to (1)
assess the reporting completeness of Taiwan’s passive safety surveillance system for selected
adverse events after 2009 H1N1 vaccines; and (2) evaluate the risks of these events for the
biologically plausible postvaccination risk intervals.” Pet. Ex. 69 at 2. The authors identified
1,475 cases of Bell’s palsy, with 298 patients developing Bell’s palsy 0-42 days after flu
vaccination. Id. at 3 tbl.2. The authors also determined the estimated number of Bell’s palsy
cases that occured 0-42 days after flu vaccination was 525, while the expected number of cases
was 354. Id. at 3, 3 tbls.3-4. Huang et al. concluded “[t]here was an increased risk for Bell’s
palsy in the interval 0-42 days after vaccination.” Id. at 3.
In addition to the above studies, Dr. Steinman also cited Chou et al., an article that
discussed two case reports of Bell’s palsy following flu vaccination. Pet. Ex. 75 at 7 (citing Pet.
Ex. 68 at 1). The first was of a 30-year-old male who developed symptoms 10 days after
administration of a flu vaccine. Pet. Ex. 68 at 1. He had received a flu vaccine in the past and
had no history of any adverse drug reactions, no personal or family history of neurological
disorders, and no history of recent infections. Id. The authors found “no other explanation for
the Bell’s palsy except for the [flu] vaccine. Furthermore, because the peripheral facial palsy
presented within [one] month between the vaccination and the onset of neurological symptoms, a
causal relationship was suspected . . . when there was no evidence of infection.” Id. at 2. The
second case report was of an 80-year-old man who developed symptoms three days after flu
vaccination. Id. He had a history of type II diabetes and hypertension. Id. He had also received
a flu vaccine previously and gave no history of an adverse drug reaction, had no personal or
family history of neurological disorders, and no history of recent infections. Id. Because of his
history of diabetes and hypertension, the authors were unable to “definitively implicate the [flu]
vaccine as etiologic for Bell’s palsy.” Id.
In response to Respondent’s experts’ reliance on different epidemiological studies, Dr.
Steinman made several observations. He noted that some of the studies do not account for
differences in the seasonal flu vaccine from year to year, and therefore, they may not be relevant
to the 2017-2018 flu vaccine. Tr. 85, 101. He testified that the cases cited above by Bardage et
68 Dr. Steinman also cited an article by Rath et al., regarding the “need to define Bell’s palsy as
an adverse event following immunization,” noting the need to achieve consensus on the
definition of the illness and the need to have complete diagnostic testing to assess it as an
adverse event. Pet. Ex. 72 at 3 (Barbara Rath et al., “All That Palsies is Not Bell’s [1]”—–The
Need to Define Bell’s Palsy As an Adverse Event Following Immunization, 26 Vaccine 1
(2007)).
69 Wan-Ting Huang et al., The Reporting Completeness of a Passive Safety Surveillance System
for Pandemic (H1N1) 2009 Vaccines: A Capture-Recapture Analysis, 30 Vaccine 2168 (2012).
23

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 24 of 42
al., Chou et al., and Huang et al. are relevant to the 2017-2018 flu vaccine at issue here because
they all contain an H1N1 strain. Tr. 101. Further, he testified that “epidemiology does not rule
out the rare case.” Tr. 85-86.
ii. Althen Prongs Two and Three
Dr. Steinman opined “the [flu] vaccination that [P]etitioner received on Sept[ember] 21,
2017 contained components that ha[d] chemical structures that [were] cross-reactive with myelin
antigens, both the P2 protein and gangliosides. These cross-reactive immune responses triggered
Bell’s [p]alsy” “ten days later on Oct[ober] 4, 2017.” Pet. Ex. 10 at 16-17.
Petitioner received the Flucelvax vaccine on September 21, 2017. Pet. Ex. 10 at 4 (citing
Pet. Ex. 1 at 1; Pet. Ex. 2 at 3). Ten days later, on October 4, 2017, Petitioner presented to the
South Alamo Medical Group “for evaluation of possible Bell’s palsy with drooping right eye and
pain in ear. Associated symptoms include[d] difficulty closing eye, drooping lower eyelid, facial
muscle weakness[,] and pain near the ear. Symptoms started approximately [three] days before
this visit.” Id. at 4, 16 (quoting Pet. Ex. 3 at 27). In review of the medical history, Dr. Steinman
noted that when Petitioner presented on October 11, 2017, there were “no blisters in or near the
ear.” Id. at 4 (quoting Pet. Ex. 3 at 33).
The correct diagnosis, in Dr. Steinman’s opinion, is Bell’s palsy, “the diagnosis made by
treating physicians.” Pet. Ex. 10 at 4. While he initially noted that alternative causes such as
infectious diseases “were ruled out by the treating physicians” because “[n]o anti-viral therapy
was given, indicating to [Dr. Steinman] that the treating doctors did not think this was a viral
mediated seventh nerve palsy like Ramsay Hunt syndrome,” Dr. Steinman later corrected this
position. Id.; see also Pet. Ex. 47 at 1; Tr. 99. He acknowledged that antiviral medication was
given to Petitioner but that it did not change his opinion or theories that the flu vaccine triggered
her Bell’s palsy through an immune response. Pet. Ex. 47 at 1; Tr. 99-100.
Moreover, Dr. Steinman noted that the medical records “made the link between the
vaccine and [Petitioner’s] Bell’s [p]alsy as well.” Pet. Ex. 10 at 16; see also Pet. Ex. 47 at 13;
Pet. Ex. 75 at 8. “It was noted that the possible contributing factor might include the receipt of
the flu vaccine two weeks ago.” Pet. Ex. 10 at 16 (citing Pet. Ex. 3 at 33). He also pointed out
that “a letter was written to exempt [Petitioner] from future [flu] vaccines since she was still
dealing with complications since October 2017.” Id. (citing Pet. Ex. 3 at 44).
Relying on Schonberger et al.70 “as a surrogate for how soon a[] [flu] vaccine could
trigger clinically relevant inflammation in the peripheral nervous system,” Dr. Steinman opined
“the timing in this case fits well with the findings from the CDC.” Pet. Ex. 10 at 16 (citing Pet.
Ex. 36); see also Tr. 83. Schonberger et al. reviewed case reports from the CDC of GBS after
the flu vaccine administration and found, on average, an onset between two and three weeks.
70 Lawrence B. Schonberger et al., Guillain Barré Syndrome Following Vaccination in the
National Influenza Immunization Program, United States, 1976-1977, 110 Am J. Epidemiology
105 (1979).
24

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 25 of 42
Pet. Ex. 36 at 2. Accordingly, Dr. Steinman opined that 10 days “is absolutely consistent with
what could occur between a [flu] vaccine and the onset of an inflammatory neuropathy.” Tr. 83.
Further, Zhou et al. found around 77% of the Bell’s palsy reports had an onset between
one and 30 days after flu vaccination. Pet. Ex. 73 at 4.71 Kamath et al. similarly found a median
range onset of one to 10 days. Pet. Ex. 70 at 5. Huang et al. identified 298 patients who
developed Bell’s palsy 0-42 days after flu vaccination. Pet. Ex. 69 at 3 tbl.2. And Chou et al.
discussed two case reports of Bell’s palsy after flu vaccination and reported onset intervals of
three days and 10 days. Pet. Ex. 68 at 1-2.
2. Respondent’s Expert, Dr. Brian C. Callaghan72
a. Background and Qualifications
Dr. Callaghan is an Associate Professor of Neurology at the University of Michigan and
“a neuromuscular specialist with a primary interest in patients with neuropathy such as Bell’s
palsy.” Resp. Ex. A at 1. Dr. Callaghan is also a staff physician in the Department of Neurology
for the Veterans Affairs Ann Arbor Health System. Resp. Ex. B at 2. He earned his M.D. from
the University of Pennsylvania Medical Center and his M.S. in Clinical Research Design and
Statistical Analysis at the University of Michigan. Id. at 1. He completed his residency in
neurology and completed a neuromuscular fellowship. Id. He serves as co-section editor for a
neurology journal, peer reviews for several neurology journals, and has over 120 publications
with a focus on neuropathy, including the appropriate diagnostic evaluation and treatment. Id. at
4, 10-17; Tr. 111. Dr. Callaghan testified he has seen approximately 30 patients in his career that
have presented with clinical presentations of Bell’s palsy. Tr. 108.73
b. Opinion
Dr. Callaghan opined that Petitioner’s flu vaccination “was not the cause of her facial
weakness.” Resp. Ex. A at 2. He reasoned “the current literature does not support an association
between [flu] vaccination and Bell’s palsy.” Id.; see also Tr. 126.
i. Althen Prong One
71 The authors stated that “reporting bias may explain the short onset intervals observed in [their]
study. Therefore, the short onset interval should be interpreted with caution. It may not
represent the true onset time due to the differential reporting bias in a passive surveillance
system.” Pet. Ex. 73 at 5.
72 Dr. Callaghan submitted two expert reports in this matter and testified at the entitlement
hearing. Resp. Exs. A, G; Tr. 3, 145.
73 Dr. Callaghan testified that Bell’s palsy is “a relatively benign condition in that most patients .
. . don’t always come to neurologists, and they often don’t need neuromuscular specialists. But
when they’re complicated, they do.” Tr. 108.
25

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 26 of 42
In his first expert report, Dr. Callaghan focused on his opinion that “the current literature
does not support an association between [flu] vaccination and Bell’s palsy.” Resp. Ex. A at 2;
see also Tr. 126. Dr. Callaghan opined that “the mechanism of Bell’s palsy is not well known
and the papers that Dr. Steinman provide[d] [were] based on GBS and MS.” Resp. Ex. A at 2.
In support of his opinion, Dr. Callaghan cited several works of medical literature that he claimed,
“do[] not support an association between [flu] vaccination and Bell’s palsy.” Id.; see also Tr.
118-19.
First, Dr. Callaghan cited Mutsch et al.,74 which “investigated the association between the
intranasal [flu] vaccination in Switzerland with Bell’s palsy and found a strong relationship.”
Resp. Ex. A at 2 (citing Resp. Ex. A, Tab 1 at 1).75 However, according to Dr. Callaghan, they
“did not find an association with the parenteral [flu] vaccination.” Id. (citing Resp. Ex. A, Tab 1
at 6). The authors found that “[i]n contrast to the parenteral vaccines, the intranasal vaccine
significantly increased the risk of Bell’s palsy” and that “there was essentially no risk of Bell’s
palsy after receipt of the traditional, parenteral [flu] vaccine.” Resp. Ex. A, Tab 1 at 1, 4.
Stowe et al.76 “investigated the association between the parenteral [flu] vaccination and
the pneumococcal vaccination with Bell’s palsy.” Resp. Ex. A at 2 (citing Resp. Ex. A, Tab 2 at
1).77 The population-based study of 2,128 individuals who developed Bell’s palsy from 1992 to
2005 found “no evidence of an increased risk [of Bell’s palsy] in the three months following
parenteral inactivated [flu] vaccine.” Resp. Ex. A, Tab 2 at 1-2. They also found no increased
risk of Bell’s palsy following the pneumococcal vaccination. Id. The authors wrote, “[t]his
study suggests that the association seen with the inactivated intranasal [flu] vaccine may be
specific to the administration of the intranasal vaccine and the association observed cannot be
extrapolated to the parenteral inactivated vaccine.” Id. at 3.
Rowhani-Rahbar et al.78 examined the association between Bell’s palsy and vaccines in
children within the patient data base of Kaiser Permanente Northern California from 2001 to
74 Margot Mutsch et al., Use of the Inactivated Intranasal Influenza Vaccine and the Risk of
Bell’s Palsy in Switzerland, 350 New Eng. J. Med. 896 (2004).
75 The Mutsch et al. study examined data in Switzerland from 2000 to 2001, and the article does
not reference the H1N1 as part of the flu vaccine administered during that time frame. See Resp.
Ex. A, Tab 1.
76 Julia Stowe et al., Bell’s Palsy and Parenteral Inactivated Influenza Vaccine, 2 Hum. Vaccines
110 (2006).
77 The Stowe et al. study used data from 1992 to 2005, and the articles does not reference H1N1
as included in the flu vaccines given those years in the UK. See Resp. Ex. A, Tab 2.
78 Ali Rowhani-Rahbar et al., Immunization and Bell’s Palsy in Children: A Case-Centered
Analysis, 175 Am. J. Epidemiology 878 (2012).
26

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 27 of 42
2006. Resp. Ex. A, Tab 3 at 1-2.79 Of the 822 children in the study, 233 received at least one
vaccine in the 12 months prior to onset. Id. at 4. The authors found no association between
vaccination (flu (trivalent), hepatitis B, or any vaccine) and Bell’s palsy during their risk
intervals of 1-14 days, 1-28 days, and 29-56 days. Id.
Wijnans et al.80 did study a vaccine containing H1N1. Resp. Ex. A, Tab 4 at 1. The
study population was comprised of all Bell’s palsy cases using a primary health care database in
the United Kingdom from 2009 to 2013. Id. at 1-2. They found a relative incidence rate of
Bell’s palsy between one and 42 days post-flu vaccination to be 0.88. Id. at 5. When adjusted
for confounders, the relative incidence rate decreased to 0.85. Id. There was an increased risk of
Bell’s palsy on the day of [flu] vaccination,” which the authors found to be “a likely
opportunistic recording of cases.” Id. at 6. However, the authors did not find evidence
supporting an increased risk of Bell’s palsy. Id. at 8.
Finally, Dr. Callaghan noted that the IOM81 published a report in 2012 concluding that
“[t]he evidence favors rejection of a causal relationship between inactivated [flu] vaccine and
Bell’s palsy.” Resp. Ex. A, Tab 5 at 2; see also Tr. 128-29.82 He added that all of Dr.
Steinman’s points to support the flu vaccination and Bell’s palsy “ignore the robust
epidemiologic evidence that there is no association between [flu] vaccination or any vaccination
and Bell’s palsy, [as] supported by the [IOM] 2012 report.” Resp. Ex. A at 2; see also Tr. 126-
27 (testifying that while the cause of Bell’s palsy is unknown, vaccination is not part of the
literature thought to be a causal mechanism and the epidemiologic studies above do not show an
association between flu vaccine and Bell’s palsy).
At the hearing and in his second report, Dr. Callaghan weighed in on Dr. Steinman’s
proposed theory, which he understood to be that there is “some homology between the [flu]
vaccine and P2 and/or that the [flu] vaccine is capable of producing antibodies against
gangliosides, and that therefore, [] led to Bell’s palsy.” Tr. 123; see also Resp. Ex. G at 1-3.
79 The H1N1 vaccine was first administered in the United States in 2009. H1N1, Vaccine
Against 2009 H1N1 Influenza Virus, Ctrs. for Disease Control & Prevention,
https://www.cdc.gov/h1n1flu/vaccination/public/vaccination_qa_pub.htm (last visited Oct. 20,
2023). There is no indication that it was administered to the patients in this study, conducted
from 2001 to 2006.
80 Leonoor Wijnans et al., Bell’s Palsy and Influenza (H1N1)pdm09 Containing Vaccines: A
Self-Controlled Case Series, 12 PLoS e0175539 (2017).
81 Inst. of Med., Influenza Vaccine, in Adverse Effects of Vaccines: Evidence and Causality 293
(Kathleen Stratton et al. eds., 2012). This is also cited as Resp. Ex. C, Tab 5.
82 The IOM study referenced two articles, Stowe et al. and Greene et al., and based on the
information provided, it does not appear that these studies included vaccines containing the
H1N1 virus, as it was not administered in the United States until 2009, outside of the years
referenced in these studies. See Resp. Ex. A, Tab 5; Resp. Ex. A, Tab2.
27

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 28 of 42
Dr. Callaghan first took issue with Dr. Steinman’s comparison of Bell’s palsy and GBS.
Tr. 123-24. He testified “GBS is a disease of . . . all the nerves in your body . . . whereas Bell’s
palsy is injury to one cranial nerve, so they’re very different.” Tr. 124. Additionally, he noted
that “GBS can only be treated with IVIG and plasmapheresis which are not used for Bell’s
palsy.” Tr. 127.
Dr. Callaghan testified that while Bell’s palsy is a common mononeuropathy, the cause is
currently unknown. Resp. Ex. G at 1; Tr. 117-18. Importantly, he pointed out that neither
gangliosides nor P2 are known or thought to be part of the pathogenesis of Bell’s palsy. Tr. 124.
Regarding gangliosides, Dr. Callaghan testified that “there’s not just one ganglioside. There are
specific gangliosides, so [Dr. Steinman was] talking about a whole family of molecules,” which,
to Dr. Callaghan, did not make sense. Tr. 124-25. He testified that there is not a “strong link”
between the flu vaccine and ganglioside antibodies. Tr. 125.
Regarding P2, Dr. Callaghan testified that the medical community does not know why
people get Bell’s palsy; they do not think that “there’s antibodies or [the] immune system is
triggered to attack P2 as part of the known pathogenies of Bell’s palsy.” Tr. 135. While Dr.
Steinman relied on Abramsky et al. for the position that P2 is involved in Bell’s palsy, Dr.
Callaghan explained that in Abramsky et al., “P2 did not cause lymphocyte transformation in
Bell’s palsy patients in vitro whereas P1L did cause lymphocyte transformation.” Resp. Ex. G at
2. Dr. Callaghan opined that in Abramsky et al., “there was no evidence to support Dr.
Steinman’s theory that P2 plays any role in the pathogenesis of Bell’s palsy.” Id. at 1; see also
Tr. 229-30. Moreover, while Dr. Steinman alleged P1L was later renamed P2, Dr. Callaghan
opined that “doesn’t make sense” because both P1L and P2 were discussed and examined in
Abramsky et al. and “P2 was negative in [Abramsky et al.] There was no response when trying
to stimulate the lymphocytes from patients with Bell’s palsy, whereas P1L [there] was.” Resp.
Ex. G at 2; Tr. 229. And according to Dr. Callaghan, the medical literature filed after the hearing
to support Dr. Steinman’s position “provide[d] no evidence or ‘actual scientific facts’ to support
[Dr. Steinman’s] claim that P1L was renamed P2.” Resp. Ex. G at 2 (quoting Tr. 238).
Nonetheless, at the hearing, Dr. Callaghan agreed that there are “very small amounts of
homology between the [flu] vaccine and P2.” Tr. 125. But he opined that “showing homology
at a few amino acids” does not link “molecular mimicry all the way from the [flu] vaccine to
Bell’s palsy.” Tr. 125-26. Even if homology exists, Dr. Callaghan opined that would only be the
first step. Tr. 126. The next step would be to “see that the patients have antibodies to both . . .
the epitope that’s supposed to be triggering this, in this case P2, [] against . . . the [flu] vaccine,”
and then have animal models which show “that this actually is the mechanism by which someone
can get a disease such as Bell’s palsy.” Id. Dr. Callaghan opined “we have none of that here.”
Id.
ii. Althen Prongs Two and Three
Dr. Callaghan agreed, more likely than not, that Petitioner had Bell’s palsy. Resp. Ex. G
at 1; Tr. 114-15. However, he believed “there was a significant chance that Ramsay Hunt may
be an alternative explanation due to [P]etitioner having symptoms that were not typical of a
28

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 29 of 42
seventh cranial nerve injury.” Resp. Ex. G at 1; see also Tr. 114-15.83 On cross-examination,
however, Dr. Callaghan acknowledged that there was no indication Petitioner had a virus or
infection. Tr. 134. Additionally, he opined that there is no relevancy to the fact that she was
prescribed acyclovir. Tr. 137.
Regarding timing, Dr. Callaghan agreed with Dr. Steinman that Petitioner’s Bell’s palsy
symptoms developed approximately 10 days after vaccination. Tr. 133-34. He conceded that
“the timing is appropriate” based on the GBS literature. Id.
3. Respondent’s Expert, J. Lindsay Whitton84
a. Background and Qualifications
Dr. Whitton received his B.Sc. in molecular biology, his M.B., Ch.B. in medicine, and his
Ph.D. in herpesvirus transcription from the University of Glasgow in Scotland. Resp. Ex. D at 1.
He also completed internships in medicine and surgery and has held various professor positions
since 1986. Id.; Resp. Ex. C at 1. Dr. Whitton was involved as a researcher and professor at the
Scripps Research Institute in California for approximately 38 years; but as of the date of the
hearing, he was only serving as the Chair of the Appointments Promotions Committee. Tr. 149-
51; Resp. Ex. D at 1. Dr. Whitton is a member of various professional societies and editorial
boards and has authored or co-authored almost 200 publications. Resp. Ex. D at 1-15. Dr.
Whitton does not provide patient care or diagnose or treat patients with Bell’s palsy. Tr. 148,
158 (testifying that he is not licensed as a medical doctor); Resp. Ex. C at 2-3 (acknowledging
that he cannot opine on the clinical aspects of the case).
b. Opinion
Dr. Whitton’s opinions were focused on the association between the flu vaccine and
Bell’s palsy. He did not believe “the vaccine played any part at all” in Petitioner’s development
of Bell’s palsy. Tr. 155, 194.
i. Althen Prong One
Dr. Whitton first noted that the etiology of Bell’s palsy is often unclear, however, he
acknowledged that potential causal mechanisms include inflammation and autoimmunity. Resp.
Ex. C at 3; Tr. 197. He also testified that “facial paralysis can be triggered by virus infection, by
varicella zoster virus.” Tr. 157. And he opined the presentation of the disease “is strongly
suggestive of a standard virus-mediated disease and not of an autoimmune reaction to the virus.”
Tr. 161.
83 The parties stipulated that Petitioner’s diagnosis was Bell’s palsy, not Ramsay Hunt syndrome.
Joint Prehearing Submission at 1.
84 Dr. Whitton submitted two expert reports in this matter and testified at the entitlement hearing.
Resp. Exs. C, E; Tr. 145.
29

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 30 of 42
For molecular mimicry to occur, Dr. Whitton stated that at least two things must happen.
Tr. 166. First, “the foreign antigen must induce an immune response.” Id. He noted that it
cannot be assumed “that the sequence in a protein or a ganglioside is always going to trigger an
immune response.” Id. Second, “the immune response, if it’s induced, must be able to cross-
react with or recognize a host component.” Id. He emphasized that not every part of the host
component, here as a protein or ganglioside, can trigger an immune response. Tr. 167. Dr.
Whitton opined that “[t]he causation of disease by molecular mimicry is a third and entirely
separate step.” Id. He testified it is “fairly difficult” to cause disease via molecular mimicry and
that molecular mimicry is not known to be a frequent cause of human disease. Tr. 169-70, 202;
see also Resp. Ex. E at 9-10.
Dr. Whitton responded to both molecular mimicry theories presented by Dr. Steinman.
Regarding the ganglioside theory, Dr. Whitton testified that there is “no evidence that
gangliosides are involved in Bell’s palsy.” Tr. 173. While he admitted gangliosides are thought
to be targets of autoimmunity in some cases of GBS, he agreed with Dr. Callaghan, that GBS and
Bell’s palsy are “very different,” and he is not aware of “any evidence that says that immune
response to gangliosides are involved in Bell’s palsy.” Tr. 170.
For support, he noted that the vaccines in Nachamkin et al., relied upon by Dr. Steinman,
were grown from eggs, unlike the Flucelvax vaccine. Tr. 174. Moreover, Nachamkin et al.
discussed GBS, not Bell’s palsy. Tr. 172-74. He testified that Nachamkin et al. “suggested
several ways in which the contents of [] flu vaccines grown in eggs might be able to trigger anti-
ganglioside antibodies.” Tr. 172. His understanding of how this might be done is “by
transferring alien gangliosides, in other words, gangliosides from birds or gangliosides from the
eggs.” Id. Dr. Callaghan disagreed with Dr. Steinman’s reliance on Nachamkin et al. because
there is “no way that Flucelvax could have included avian gangliosides” because Flucelvax is
grown in canine cells. Id.; see also Resp. Ex. C at 8 (opining there is “no possibility that
Flucelvax . . . contains any avian gangliosides” (emphasis omitted)). Thus, he also disagreed
with Dr. Steinman’s opinion that “gangliosides are gangliosides.” Tr. 172. Instead, Dr. Whitton
referenced An et al. and opined that “[g]angliosides are glycosylated lipids. They’re not
glycosylated proteins.” Tr. 173-74.
Additionally, Dr. Whitton cited Lei et al.85 to support his position that there is no
correlation with flu vaccination and the induction of antiganglioside antibodies. Resp. Ex. C at 7
(citing Resp. Ex. C, Tab 7). However, Lei et al. stated they “could not exclude the possibility
that anti-GM1 antibodies might be generated rarely in [flu] vaccinees.” Resp. Ex. C, Tab 7 at 5.
Regarding Dr. Steinman’s P2 theory, Dr. Whitton first opined that, to his knowledge,
“there’s no association between P2 protein and Bell’s palsy pathogenesis.” Tr. 174, 192. Dr.
Whitton rejected Dr. Steinman’s three-step process supporting his molecular mimicry theory.
85 Ting Lei et al., Anti-ganglioside Antibodies Were Not Detected in Human Subjects Infected
with or Vaccinated Against 2009 Pandemic Influenza A (H1N1) Virus, 30 Vaccine 2605 (2012).
30

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 31 of 42
Resp. Ex. E at 5-7; Tr. 186; see also Tr. 168 (testifying one cannot reliably predict cross-
reactivity).
First, he stated that BLAST searches were designed “to evaluate evolutionary
relationships between proteins” not “to identify and predict immunological reactions.” Tr. 175;
see also Resp. Ex. C at 9. Thus, Dr. Whitton opined Dr. Steinman’s BLAST searches are “very
far” from being relevant; he deemed them “unsatisfactory” or “not useful.” Resp. Ex. C at 8, 18;
Tr. 200; see also Resp. Ex. E at 1.86 Dr. Whitton opined that “none of Dr. Steinman’s BLAST-
identified homologies [met] or exceed[ed] the three Silvanovich [et al.] criteria, and the BLAST
algorithm . . . itself tells us that the homologies [presented] [were] the result of chance.” Resp.
Ex. C at 11 (citing Resp. Ex. C, Tab 10; Resp. Ex. C, Tab 11);87 see also Tr. 179.
According to Dr. Whitton, three criteria were recommended by Silvanovich et al. when
using bioinformatic methods to evaluate protein sequence similarity and homology
determinations for allergens. Tr. 179; see Resp. Ex. C at 10-11. Dr. Whitton opined that the first
Silvanovich et al. criterion is that “the homology identified by BLAST must be at least 80 amino
acids in length.” Tr. 176. The second criterion is that “within those 80 amino acids, there must
be a match, an identity of at least 28 amino acids, [or] 35 percent identity.” Tr. 176-77. The
third criterion is that the E-value88 of the BLAST homology should be “about one in 10 million,
around [] 10 to the minus seven [10-7].” Tr. 177; see also Resp. Ex. C, Tab 11.89 Dr. Whitton
testified that Dr. Steinman’s BLAST searches did not meet any of these criteria, and the E-values
of Dr. Steinman’s BLAST searches were “all one to 10 million-fold higher than that.” Tr. 177.
Therefore, Dr. Whitton concluded that the homologies were “undoubtedly the results of chance.”
Id.
In contrast, Dr. Steinman opined that the immune system interacts with shorter sequences
of amino acids than outlined in Silvanovich et al.90 See Tr. 214-18. Additionally, Silvanovich et
al. applies in the contexts of allergens to determine the potential for allergy reactions (to assess
86 For a full and detailed explanation of Dr. Whitton’s opinions about Dr. Steinman’s use of
BLAST searches, see Resp. Ex. C at 8-16; Resp. Ex. E at 1-7; Tr. 175-86, 224-27.
87 Andre Silvanovich et al., The Use of E-Scores to Determine the Quality of Protein
Alignments, 54 Regulatory Toxicology & Pharmacology S26 (2009).
88 The E-value, or expect value, “is parameter that describes the number of hits one can ‘expect’
to see by chance when searching a database of a particular size. It decreases exponentially as the
Score (S) of the match increases.” Frequently Asked Questions, BLAST, Nat’l Libr. Med.,
https://blast.ncbi.nlm.nih.gov/doc/blast-help/FAQ.html (last visited Oct. 23, 2023).
89 For a full and detailed explanation of Dr. Whitton’s opinions of BLAST E-values, see Tr. 177-
78, 224-27; Resp. Ex. C at 11.
90 Dr. Steinman also testified that Silvanovich et al. is one reason why he starts with a BLAST
search but that it is only the first step of his process. Tr. 94.
31

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 32 of 42
the safety of genetically modified crops). See Resp. Ex. C, Tab 11 at 1. In response, Dr.
Whitton testified that the World Health Organization (“WHO”) “approve[d] this approach for
identification of allergens,” and allergens trigger an immune response.” Tr. 179. Thus, Dr.
Whitton concluded that “the Silvanovich et al. criteria do apply to the immune response.” Id.;
see also Tr. 93-94.
Rather than applying the Silvanovich et al. criteria, Dr. Steinman used Lanz et al. and
other literature to show the homology was significant. See Pet. Ex. 10 at 11. Lanz et al.,
published in 2022 with Dr. Steinman as a named author, “demonstrate[d] high-affinity molecular
mimicry” between Epstein-Barr virus nuclear antigen1 and a central nervous system protein
(GlialCAM). Pet. Ex. 76 at 1. The study also showed the functional relevance of their findings
as it relates to multiple sclerosis. Id. Dr. Whitton criticized Dr. Steinman’s reliance on Lanz et
al. because they did not use a BLAST search to identify homology. Tr. 192. Moreover, he
added that Lanz et al. is about Epstein-Barr virus and multiple sclerosis and therefore he argued
that “both the alleged cause and the alleged outcome are different” than the case here. Tr. 188.
Relating back to Dr. Whitton’s opinion that two things must happen for molecular
mimicry to occur, Dr. Whitton conceded that step one, “the induction of immune response by
that sequence of flu [hemagglutinin] . . . may be fulfilled” by the homology proposed by Dr.
Steinman. Tr. 187; see also Tr. 166. Regarding step two, “which is the cross-recognition of the
proposed target sequence in P2,” Dr. Whitton opined “there is zero evidence presented for that.”
Tr. 187; see also Tr. 166.
Moreover, Dr. Whitton opined just because there is homology found in a BLAST search,
does not mean there is molecular mimicry. Resp. Ex. C at 14; Tr. 182, 187.91 He testified that
“[y]ou will always find multiple homologies when you properly compare two proteins” and that
most homologies do not trigger a biologic meaningful cross-reactive immune response. Tr. 182-
85; see also Resp. Ex. C at 13-15 (opining that “the mere existence of homology is
immunologically meaningless”). He explained that “[w]hen a foreign protein is injected into an
animal, immune responses are made only to certain parts of the protein[,] not to each and every
run of amino acids in the protein.” Resp. Ex. C at 14 (emphasis omitted). Therefore, when a
BLAST search “shows a homology between a foreign protein and a host protein, one cannot
assume that the foreign part of the homology triggers any immune response whatsoever.” Id.
And even if an “imaginary immune response is induced by the foreign amino-acid sequence, one
must not assume that that immune response can cross-react with the host part of the homology.”
Id. (emphasis omitted).
Finally, Dr. Whitton opined that “[t]he high incidence of Bell’s palsy, together with the
large number of flu vaccines administered annually, means that the temporal relationship
between vaccination and disease is far more likely to be coincidental than causal.” Resp. Ex. C
91 For additional discussion by Dr. Whitton about why he disagreed with Dr. Steinman, see Resp.
Ex. C at 15, Tr. 190-91, 201.
32

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 33 of 42
at 18; see also Tr. 193-94. Dr. Whitton cited Black et al.,92 which “evaluated the likelihood of
coincidental occurrence between flu vaccination and several neurological diseases including
GBS.” Resp. Ex. C at 17 (citing Resp. Ex. C, Tab 12). Relying on Black et al., he opined that
given the incidence of GBS cases and the number of flu vaccines administered per year, the
number of GBS cases within six weeks of vaccination is “purely by chance” and “coincidental.”
Id. Like Dr. Callaghan, Dr. Whitton also cited the 2012 IOM publication finding no evidence of
increased risk of Bell’s palsy after inactivated flu vaccination. Id. at 4 (citing Resp. Ex. A, Tab
5).
Ultimately, Dr. Whitton concluded that “neither gangliosides nor P2 protein are known to
be potential targets in Bell’s palsy.” Tr. 203.
ii. Althen Prongs Two and Three
Dr. Whitton did not agree that there was a causational relationship between Petitioner’s
flu vaccination and the development of her Bell’s palsy. Tr. 194. Specifically, he opined “the
evidence . . . presented to support the contention that the flu vaccine administered on [September
21, 2017] was responsible for the signs/symptoms experienced by [Petitioner] is extremely
weak.” Resp. Ex. C at 17.
He noted Petitioner’s treating physician initially ordered an antiviral, acyclovir, as a
treatment for her Bell’s palsy. Resp. Ex. C at 17 (citing Pet. Ex. 3 at 29). This is one reason that
Dr. Whitton’s believed that “medical personnel clearly considered viral infection as a likely
cause” of her Bell’s palsy. Id. However, Dr. Whitton did not opine, more likely than not, that
Petitioner’s Bell’s palsy was caused by a viral infection. See id. at 1, 4-5.
Dr. Whitton agreed that Petitioner’s onset of Bell’s palsy was approximately 10 days
after administration of the flu vaccine. Resp. Ex. C at 1; Tr. 194. He did not refute Dr.
Steinman’s opinion that the temporal association between vaccination and onset of Petitioner’s
Bell’s palsy was appropriate given the theory of molecular mimicry.
4. Letter from Dr. Robert P. Lisak93
Dr. Lisak is a Professor of Neurology and Professor of Biochemistry, Microbiology and
Immunology at Wayne State University School of Medicine. Pet. Ex. 92 at 2. He is also a
Neurologist at Harper University Hospital and Detroit Receiving Hospital. Id. at 3. He has been
involved in neuroimmunologic research, including the study of myelin basic proteins, since
1966. Pet. Ex. 91 at 1.
92 Steven Black et al., Importance of Background Rates of Disease in Assessment of Vaccine
Safety During Mass Immunisation with Pandemic H1N1 Influenza Vaccines, 374 Pub. Health
2115 (2009).
93 Dr. Lisak did not testify at the hearing.
33

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 34 of 42
Petitioner submitted a letter by Dr. Lisak after the hearing to comment on the P1 and P2
myelin protein nomenclature issue. Pet. Ex. 91 at 1. He supported Dr. Steinman’s position
regarding the “evolution of the terminology of the [peripheral nervous system] myelin basic
protein” and that the P1L protein referenced in Abramsky et al. is now called P2. Id. Dr. Lisak
explained that
[t]he original terminology of P1L and P2(L) in the Abramsky [et al.] papers is
known to be incorrect. It is known and widely accepted since the late 1970s that
P1L is the P2 protein used in all the other papers Dr. Steinman cited, as well as in
[his own] studies[94] . . . and that of others, induces [EAN] and is specific to the
[peripheral nervous system]. What Abramsky [et al.] termed P2 (L) is actually P1
. . . that is identical to [myelin basic protein] the constituent of CNS that induces
[EAE]. The use of the name P2 myelin protein is the correct term for the
[peripheral nervous system] myelin specific protein being studied in EAN and
studies of human serum and lymphocyte reactivity in diseases.
Id.
IV. DISCUSSION
A. Standards for Adjudication
The Vaccine Act was established to compensate vaccine-related injuries and deaths. §
10(a). “Congress designed the Vaccine Program to supplement the state law civil tort system as
a simple, fair and expeditious means for compensating vaccine-related injured persons. The
Program was established to award ‘vaccine-injured persons quickly, easily, and with certainty
and generosity.’” Rooks v. Sec’y of Health & Hum. Servs., 35 Fed. Cl. 1, 7 (1996) (quoting
H.R. Rep. No. 908 at 3, reprinted in 1986 U.S.C.C.A.N. at 6287, 6344).
Petitioner’s burden of proof is by a preponderance of the evidence. § 13(a)(1). The
preponderance standard requires a petitioner to demonstrate that it is more likely than not that the
vaccine at issue caused the injury. Moberly v. Sec’y of Health & Hum. Servs., 592 F.3d 1315,
1322 n.2 (Fed. Cir. 2010). Proof of medical certainty is not required. Bunting v. Sec’y of Health
& Hum. Servs., 931 F.2d 867, 873 (Fed. Cir. 1991). Petitioner need not make a specific type of
evidentiary showing, i.e., “epidemiologic studies, rechallenge, the presence of pathological
markers or genetic predisposition, or general acceptance in the scientific or medical communities
to establish a logical sequence of cause and effect.” Capizzano v. Sec’y of Health & Hum.
Servs., 440 F.3d 1317, 1325 (Fed. Cir. 2006). Instead, Petitioner may satisfy her burden by
presenting circumstantial evidence and reliable medical opinions. Id. at 1325-26.
In particular, Petitioner must prove that the vaccine was “not only [the] but-for cause of
the injury but also a substantial factor in bringing about the injury.” Moberly, 592 F.3d at 1321
(quoting Shyface v. Sec’y of Health & Hum. Servs., 165 F.3d 1344, 1352-53 (Fed. Cir. 1999));
94 Dr. Lisak referenced papers numbered 90, 92, 115, and 120 from his CV, however those were
not filed. Pet. Ex. 91 at 1; see Pet. Ex. 92 at 23-24.
34

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 35 of 42
see also Pafford v. Sec’y of Health & Hum. Servs., 451 F.3d 1352, 1355 (Fed. Cir. 2006). The
received vaccine, however, need not be the predominant cause of the injury. Shyface, 165 F.3d
at 1351. A petitioner who satisfies this burden is entitled to compensation unless Respondent
can prove, by a preponderance of the evidence, that the vaccinee’s injury is “due to factors
unrelated to the administration of the vaccine.” § 13(a)(1)(B). However, if a petitioner fails to
establish a prima facie case, the burden does not shift. Bradley v. Sec’y of Health & Hum.
Servs., 991 F.2d 1570, 1575 (Fed. Cir. 1993).
“Regardless of whether the burden ever shifts to the [R]espondent, the special master
may consider the evidence presented by the respondent in determining whether the [P]etitioner
has established a prima facie case.” Flores v. Sec’y of Health & Hum. Servs., 115 Fed. Cl. 157,
162-63 (2014); see also Stone v. Sec’y of Health & Hum. Servs., 676 F.3d 1373, 1379 (Fed. Cir.
2012) (“[E]vidence of other possible sources of injury can be relevant not only to the ‘factors
unrelated’ defense, but also to whether a prima facie showing has been made that the vaccine
was a substantial factor in causing the injury in question.”); de Bazan v. Sec’y of Health & Hum.
Servs., 539 F.3d 1347, 1353 (Fed. Cir. 2008) (“The government, like any defendant, is permitted
to offer evidence to demonstrate the inadequacy of the [P]etitioner’s evidence on a requisite
element of the [P]etitioner’s case-in-chief.”); Pafford, 451 F.3d at 1358-59 (“[T]he presence of
multiple potential causative agents makes it difficult to attribute ‘but for’ causation to the
vaccination. . . . [T]he Special Master properly introduced the presence of the other unrelated
contemporaneous events as just as likely to have been the triggering event as the vaccinations.”).
B. Causation
To receive compensation through the Program, Petitioner must prove either (1) that she
suffered a “Table Injury”—i.e., an injury listed on the Vaccine Injury Table—corresponding to a
vaccine that she received, or (2) that she suffered an injury that was actually caused by a
vaccination. See §§ 11(c)(1), 13(a)(1)(A); Capizzano, 440 F.3d at 1319-20. Because Petitioner
does not allege she suffered a Table Injury, she must prove a vaccine she received caused her
injury. To do so, Petitioner must establish, by preponderant evidence: “(1) a medical theory
causally connecting the vaccination and the injury; (2) a logical sequence of cause and effect
showing that the vaccination was the reason for the injury; and (3) a showing of a proximate
temporal relationship between vaccination and injury.” Althen, 418 F.3d at 1278.
The causation theory must relate to the injury alleged. Petitioner must provide a sound
and reliable medical or scientific explanation that pertains specifically to this case, although the
explanation need only be “legally probable, not medically or scientifically certain.” Knudsen v.
Sec’y of Health & Hum. Servs., 35 F.3d 543, 548-49 (Fed. Cir. 1994). Petitioner cannot
establish entitlement to compensation based solely on her assertions; rather, a vaccine claim must
be supported either by medical records or by the opinion of a medical doctor. § 13(a)(1). In
determining whether Petitioner is entitled to compensation, the special master shall consider all
material in the record, including “any . . . conclusion, [or] medical judgment . . . which is
contained in the record regarding . . . causation.” § 13(b)(1)(A). The undersigned must weigh
the submitted evidence and the testimony of the parties’ proffered experts and rule in Petitioner’s
favor when the evidence weighs in her favor. See Moberly, 592 F.3d at 1325-26 (“Finders of
fact are entitled—indeed, expected—to make determinations as to the reliability of the evidence
35

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 36 of 42
presented to them and, if appropriate, as to the credibility of the persons presenting that
evidence.”); Althen, 418 F.3d at 1280 (noting that “close calls” are resolved in Petitioner’s
favor).
Testimony that merely expresses the possibility—not the probability—is insufficient, by
itself, to substantiate a claim that such an injury occurred. See Waterman v. Sec’y of Health &
Hum. Servs., 123 Fed. Cl. 564, 573-74 (2015) (denying Petitioner’s motion for review and
noting that a possible causal link was not sufficient to meet the preponderance standard). The
Federal Circuit has made clear that the mere possibility of a link between a vaccination and a
petitioner’s injury is not sufficient to satisfy the preponderance standard. Moberly, 592 F.3d at
1322 (emphasizing that “proof of a ‘plausible’ or ‘possible’ causal link between the vaccine and
the injury” does not equate to proof of causation by a preponderance of the evidence); Boatmon
v. Sec’y of Health & Hum. Servs., 941 F.3d 1351, 1359-60 (Fed. Cir. 2019). While certainty is
by no means required, a possible mechanism does not rise to the level of preponderance.
Moberly, 592 F.3d at 1322; see also de Bazan, 539 F.3d at 1351.
V. ANALYSIS
A. Althen Prong One
Under Althen prong one, Petitioner must set forth a medical theory explaining how the
received vaccine could have caused the sustained injury. Andreu v. Sec’y of Health & Hum.
Servs., 569 F.3d 1367, 1375 (Fed. Cir. 2009); Pafford, 451 F.3d at 1355-56. Petitioner’s theory
of causation need not be medically or scientifically certain, but it must be informed by a “sound
and reliable” medical or scientific explanation. Boatmon, 941 F.3d at 1359; see also Knudsen,
35 F.3d at 548; Veryzer v. Sec’y of Health & Hum. Servs., 98 Fed. Cl. 214, 223 (2011) (noting
that special masters are bound by both § 13(b)(1) and Vaccine Rule 8(b)(1) to consider only
evidence that is both “relevant” and “reliable”). If Petitioner relies upon a medical opinion to
support her theory, the basis for the opinion and the reliability of that basis must be considered in
the determination of how much weight to afford the offered opinion. See Broekelschen v. Sec’y
of Health & Hum. Servs., 618 F.3d 1339, 1347 (Fed. Cir. 2010) (“The special master’s decision
often times is based on the credibility of the experts and the relative persuasiveness of their
competing theories.”); Perreira v. Sec’y of Health & Hum. Servs., 33 F.3d 1375, 1377 n.6 (Fed.
Cir. 1994) (stating that an “expert opinion is no better than the soundness of the reasons
supporting it” (citing Fehrs v. United States, 620 F.2d 255, 265 (Ct. Cl. 1980))).
The undersigned finds Petitioner has set forth a sound and reliable medical theory,
molecular mimicry, to explain how the flu vaccine can cause Bell’s palsy.
Moreover, the medical literature and the testimony and opinions of Dr. Steinman show
that there is persuasive evidence of the similarity between GBS and Bell’s palsy, that Bell’s
palsy is a variant of GBS, and that molecular mimicry is an appropriate causal mechanism of
GBS and Bell’s palsy. Further, the literature provides support for Dr. Steinman’s opinion that
Bell’s palsy is caused by molecular mimicry.
36

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 37 of 42
Greco et al. provides a comprehensive analysis of the relevant immunological theories of
causation in Bell’s palsy, specifically molecular mimicry. The authors state, “[s]ome evidence
implicates the involvement of immune mechanisms in Bell’s palsy. Many reports have indicated
the association between facial paralysis and [GBS], a condition that was recently shown to be a
cell mediated, autoimmune neuritis.” Pet. Ex. 19 at 4. The authors also discuss Abramsky et al.,
which Dr. Steinman relies upon to show homology between the flu vaccine and human basic
protein (P1L, now P2L) of peripheral nerve myelin in patients with Bell’s palsy. Abramsky et al.
also suggests that “cell-mediated autoimmune mechanisms may be of importance in the
pathogenesis of Bell’s palsy.” Id.; see also Pet. Ex. 20 at 1. Bell’s palsy, like GBS, is an acute
demyelinating disease of the peripheral nervous system. There is a body of evidence showing
there is an immune-mediated causal theory that is sound and reliable, and the most likely of the
relevant immune-mediated mechanisms is molecular mimicry. Thus, the undersigned finds that
Petitioner has provided sound and reliable evidence for the application of molecular mimicry in
the context of Bell’s palsy.
Molecular mimicry has been accepted as a sound and reliable theory in many
demyelinating conditions, including GBS, in the Vaccine Program, forming the basis for
petitioners to be entitled to compensation. See, e.g., Conte v. Sec’y of Health & Hum. Servs.,
No. 17-403V, 2020 WL 5743696, at *57 (Fed. Cl. Spec. Mstr. July 27, 2020) (noting the theory
of molecular mimicry in a GBS case is “well-established and well-settled in the Vaccine
Program”); Barone v. Sec’y of Health & Hum. Servs., No. 11-707V, 2014 WL 6834557, at *8-9
(Fed. Cl. Spec. Mstr. Nov. 12, 2014) (noting molecular mimicry “has been accepted in other
Program cases as a reliable medical explanation for how various autoimmune conditions could
develop after the receipt of different kinds of vaccinations”); Larson v. Sec’y of Health & Hum.
Servs., No. 16-633V, 2023 WL 3765631 (Fed. Cl. Spec. Mstr. June 1, 2023), mot. for review
denied, 2023 WL 6387783 (Fed. Cl. Oct. 2, 2023); Maloney v. Sec’y of Health & Hum. Servs.,
No. 19-1713V, 2022 WL 1074087 (Fed. Cl. Spec. Mstr. Mar. 17, 2022).95
Petitioner also provided preponderant evidence, by expert opinion and medical literature,
of an association between the flu vaccine and Bell’s palsy. Zhou et al. concluded there “may be
a signal of possible association between [flu] vaccines and an increased risk of Bell’s palsy.”
Pet. Ex. 47 at 5. Bardage et al. reported “a significantly increased risk for Bell’s palsy” in “those
vaccinated in the early phase of the vaccination campaign (≤ 45 days), when high risk groups
predominated.” Pet. Ex. 41 at 4. Kamath et al. noted that reports of Bell’s palsy were higher
after receipt of the flu vaccination as compared to other vaccines. Pet. Ex. 70 at 4-6. Lastly,
Huang et al. concluded there was an increased risk of Bell’s palsy after the H1N1 vaccination.
Pet. Ex. 69 at 2.
The lack of epidemiological evidence is not dispositive. It is difficult to use
epidemiology to determine whether a vaccine is implicated in causation. Because while adverse
reactions like this do not appear in the epidemiological evidence cited by Respondent’s experts,
it may be that events are too rare to be captured. Moreover, “[r]equiring epidemiologic studies . .
95 The undersigned acknowledges that the last case in this string cite involves a different vaccine,
although the same illness and general theory.
37

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 38 of 42
. or general acceptance in the scientific or medical communities . . . impermissibly raises a
claimant’s burden under the Vaccine Act and hinders the system created by Congress, in which
close calls regarding causation are resolved in favor of injured claimants.” Andreu, 569 F.3d at
1378 (quoting Capizzano, 440 F.3d at 132-26); see also Althen, 418 F.3d at 1280 (noting that
“close calls” are resolved in Petitioner’s favor). The undersigned does not find the
epidemiological literature to be definitive or determinative in this regard.
The undersigned also finds that there is scientific support for Dr. Steinman’s two theories
that illustrate how molecular mimicry could cause Bell’s palsy. Dr. Steinman has identified
components of the flu vaccine that could initiate the development of antibodies that could cross-
react with peripheral nerve myelin and trigger an autoimmune response.
His first theory is based on ganglioside mimicry. Greco et al. provides foundational
support by showing that human cranial nerves are composed of gangliosides. Nachamkin et al.
shows that ganglioside antibodies (from C. jejuni infection) are found in patients with GBS.
Nachamkin et al. also provides evidence that flu vaccines, including those containing H1N1,
induce antibody responses to anti-gangliosides (anti-GM1) and to hemagglutinin (found in the
2017-2018 vaccine, Flucelvax). An et al. shows that the flu vaccine grown in canine kidney cells
(used in Flucelvax) could glycosylate flu vaccine proteins, like the egg-based vaccines studied by
Nachamkin et al.
Thus, Dr. Steinman produced literature to show that Bell’s palsy involves the cranial
nerves, and that gangliosides are found in these nerves. He has shown that patients with GBS,
and Miller Fisher (a variant of GBS which involves cranial nerves) have anti-ganglioside
antibodies. Next, he has shown that flu vaccines (H1N1) induce antibody responses. And he
establishes the flu vaccine at issue here, although grown in canine kidney cells, glycosylates flu
vaccine protein like its egg-based counterpart. For each aspect of his theory, Petitioner has
provided scientific support through medical literature.
There is also evidence to support Dr. Steinman’s second theory based on the P2 protein in
myelin in the peripheral nerves. Abramsky et al. found a “defined in vitro response to a human
basic protein” (P1L) of peripheral nerve myelin in patients with Bell’s palsy and suggested that
molecular mimicry may play a causal role. Pet. Ex. 20 at 4. Dr. Steinman provides preponderant
evidence that the nomenclature has changed, and that that P1L is now referenced as P2.96 The
P2 protein may be specific to the peripheral nerve myelin, targeted in Bell’s palsy. Dr. Steinman
then uses a three-step process to identify protein sequences that could implicate molecular
mimicry between the flu vaccine and P2.
Petitioner need not make a specific type of evidentiary showing or require identification
of homology to prove that molecular mimicry is a sound and reliable theory by preponderant
evidence. Given the state of current scientific knowledge, there is no way that a petitioner could
96 Assuming the undersigned’s ruling on this point is in error, it does not change the ruling in
favor of entitlement, as this issue is not determinative of the outcome, in that Dr. Steinman
provides an alternative mechanistic theory (gangliosides) which is sound and reliable.
38

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 39 of 42
satisfy such a requirement. Further, requiring proof of specific homology or proof of identical
protein sequences between the flu vaccine and the peripheral nervous system to prove causation
would require scientific certainty, which is a bar too high. See Knudsen, 35 F.3d at 549
(explaining that “to require identification and proof of specific biological mechanisms would be
inconsistent with the purpose and nature of the vaccine compensation program”).
Regarding Dr. Steinman’s testimony about homologous sequences, the undersigned finds
that he was illustrating how molecular mimicry can cause Bell’s palsy using readily available
resources. Dr. Steinman explained that he could not perform research on Petitioner. He also
explained the limitations of the process that he used. The undersigned will not reject the
mechanistic theory of molecular mimicry because Dr. Steinman was unable to prove his theory
in a laboratory. The undersigned is not willing to disregard applicable medical literature, or
ignore her knowledge and experience about the application of molecular mimicry in the context
of demyelinating peripheral neuropathies, when molecular mimicry has been repeatedly shown
by preponderant evidence to be a sound and reliable theory in the context of vaccine causation.
Lastly, the undersigned’s finding is consistent with her prior ruling involving the flu
vaccine and Bell’s palsy. See E. A. v. Sec’y of Health & Hum. Servs., No. 18-1587V, 2023 WL
2640710 (Fed. Cl. Spec. Mstr. Jan. 24, 2023). In E.A., the Petitioner received a flu vaccination
on October 19, 2015. Id. at *4, *29. Approximately forty days post-vaccination, she awoke with
left facial numbness and weakness. Id. Examination revealed weakness of the seventh cranial
nerve. Id. She was diagnosed with Bell’s palsy. Id. Petitioner’s expert opined that molecular
mimicry was the most likely mechanism, and he explained that components of the vaccine can
lead to autoimmune responses directed against the facial nerve triggering demyelination and
resulting in neuropathy. Id. at *19, *27-28. The experts cited many of the same articles and
advanced many of the same arguments for and against causation that were discussed herein. Id.
at *14-25, *27-28. The undersigned found that the Petitioner in E.A. had provided preponderant
evidence of a sound and reliable causal theory, satisfying Althen prong one. Id. at *28. The
undersigned again evaluates the same evidence here, and comes to the same conclusion.
For the reasons discussed above, the undersigned finds that Petitioner has provided
preponderant evidence of a sound and reliable causal theory, satisfying Althen prong one.
B. Althen Prong Two
Under Althen prong two, Petitioner must prove by a preponderance of the evidence that
there is a “logical sequence of cause and effect showing that the vaccination was the reason for
the injury.” Capizzano, 440 F.3d at 1324 (quoting Althen, 418 F.3d at 1278). “Petitioner must
show that the vaccine was the ‘but for’ cause of the harm . . . or in other words, that the vaccine
was the ‘reason for the injury.’” Pafford, 451 F.3d at 1356 (internal citations omitted).
In evaluating whether this prong is satisfied, the opinions and views of the vaccinee’s
treating physicians are entitled to some weight. Andreu, 569 F.3d at 1367; Capizzano, 440 F.3d
at 1326 (“[M]edical records and medical opinion testimony are favored in vaccine cases, as
treating physicians are likely to be in the best position to determine whether a ‘logical sequence
of cause and effect show[s] that the vaccination was the reason for the injury.’” (quoting Althen,
39

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 40 of 42
418 F.3d at 1280)). Medical records are generally viewed as trustworthy evidence, since they are
created contemporaneously with the treatment of the vaccinee. Cucuras v. Sec’y of Health &
Hum. Servs., 993 F.2d 1525, 1528 (Fed. Cir. 1993). The Petitioner need not make a specific
type of evidentiary showing, i.e., “epidemiologic studies, rechallenge, the presence of
pathological markers or genetic predisposition, or general acceptance in the scientific or medical
communities to establish a logical sequence of cause and effect.” Capizzano, 440 F.3d at 1325.
Instead, Petitioner may satisfy her burden by presenting circumstantial evidence and reliable
medical opinions. Id. at 1325-26.
Regarding Althen prong two, the undersigned finds there is no issue regarding diagnosis,
as the parties agree that Petitioner had Bell’s palsy. This diagnosis is well supported by the
medical records and the opinions of the treating physicians.
Further, the undersigned finds that Petitioner provided preponderant evidence of a logical
sequence of cause and effect showing that her vaccination was the cause of her Bell’s palsy.
First, Petitioner’s clinical course is consistent with the medical literature and case reports of
Bell’s palsy following vaccination.
Petitioner received the flu vaccine on September 21, 2017, and 13 days later, on October
4, presented to her physician with difficulty closing her eye, drooping eye, facial muscle
weakness, and ear pain. Physical examination revealed palsy of the facial nerve (seventh cranial
nerve). An MRI was done without contrast and did not reveal abnormalities. Although
Petitioner did not have MRI findings that specifically showed enhancement of the cranial nerve
or a specific demyelinating process, she did have abnormal findings of the seventh cranial nerve
on neurological examination.
Further, the undersigned finds no evidence of any alternative cause. There is no evidence
in the record to suggest that Petitioner had varicella zoster. Physical examination did not reveal
any vesicles, rash, or lesions consistent with varicella zoster. She also did not test positive for
Lyme disease. Dr. Callaghan acknowledges that there was no indication of a virus or infection.
While Dr. Whitton opines Petitioner’s “medical personnel clearly considered viral infection as a
likely cause” because they prescribed acyclovir, there were no signs of infection on examination.
Resp. Ex. C at 17. And Dr. Callaghan opines that the prescription of acyclovir had no relevance.
It is important to note that Dr. Whitton is not licensed as a medical doctor, and he
testified that he does not diagnose or treat patients who have neurological illnesses, like Bell’s
palsy. Thus, he has not determined whether a patient’s Bell’s palsy was caused by infection or
vaccination. While Dr. Whitton is eminently qualified to opine in the area of his expertise—
immunology and microbial science—the undersigned finds that his opinions as to diagnosis
and/or alternate cause carry less weight, especially given his testimony acknowledging that he
could not opine on the clinical aspects of the case. Tr. 158; Resp. Ex. C at 2-3.
Dr. Callaghan, who is a medical doctor (neurologist), did not offer an opinion that
infection caused Petitioner’s Bell’s palsy. Because Dr. Callaghan is well qualified to opine on
diagnosis and the etiology of that diagnosis by virtue of his training, experience, and
qualifications, the undersigned finds his opinions more persuasive. In weighing the
40

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 41 of 42
persuasiveness of opinion testimony, special masters may consider the relative expertise,
backgrounds, and specialties of the experts. Locane v. Sec’y of Health & Hum. Servs., 685 F.3d
1375, 1380 (Fed. Cir. 2012); Stone, 676 F.3d at 1382 (noting the special master correctly found
one experts testimony on an issue to be more reliable than the others due to “more extensive and
more recent experience”); Pafford, 451 F.3d at 1359 (affirming the special master’s rejection of
expert’s testimony because he lacked proper qualifications in the specialty areas in which he
testified); see also Dwyer v. Sec’y of Health & Hum. Servs., No. 03-1202V, 2010 WL 892250,
at *64 (Fed. Cl. Spec. Mstr. Mar. 12, 2010) (giving greater weight to M.D. epidemiologists’
opinions on medical issues than to Ph.D. epidemiologist’s opinion). The undersigned
acknowledges the Circuit Court’s directive, and here, Dr. Whitton agrees that the clinical issues,
which include the question of alternative causes, is outside of his expertise. The question of
whether Petitioner’s Bell’s palsy was caused by an alternative cause like infection involves the
practice of medicine, which requires specific training, experience, and qualifications, and in
general, experience in caring for patients.
Moreover, Dr. Whitton fails to state his opinion as to alternate cause to a reasonable
degree of probability. He opines that because Petitioner’s treating physicians ordered an
antiviral medication, acyclovir, that they considered “viral infection as a likely cause.” Resp. Ex.
C at 17. However, he does not express the opinion, more likely than not, that a viral infection
was the cause of Petitioner’s Bell’s palsy. Accordingly, the undersigned finds that Dr. Whitton’s
opinion does not carry sufficient weight to support alternative causation.
Thus, the undersigned finds that Petitioner provided preponderant evidence of a logical
sequence of cause and effect, satisfying Althen prong two.
C. Althen Prong Three
Althen prong three requires Petitioner to establish a “proximate temporal relationship”
between the vaccination and the injury alleged. Althen, 418 F.3d at 1281. That term has been
defined as a “medically acceptable temporal relationship.” Id. The Petitioner must offer
“preponderant proof that the onset of symptoms occurred within a timeframe which, given the
medical understanding of the disease’s etiology, it is medically acceptable to infer causation-in-
fact.” de Bazan, 539 F.3d at 1352. The explanation for what is a medically acceptable time
frame must also coincide with the theory of how the relevant vaccine can cause the injury alleged
(under Althen Prong One). Id.; Koehn, 773 F.3d at 1243; Shapiro v. Sec’y of Health & Hum.
Servs., 101 Fed. Cl. 532, 542 (2011), recons. den’d after remand, 105 Fed. Cl. 353 (2012), aff’d
mem., 503 F. App’x 952 (Fed. Cir. 2013).
The parties stipulate, and the experts agree, that Petitioner received the flu vaccine on
September 21, 2017, and approximately 10 days later, on October 1, 2017, she developed Bell’s
palsy. Dr. Steinman opines that 10 days is appropriate given the purported autoimmune
mechanism of molecular mimicry. He also provides medical literature which shows onset ranges
from one to 30 days (Zhou et al.), three to 10 days (Chou et al.), and zero to 42 days (Huang et
al.). Moreover, Respondent’s experts do not provide evidence refuting Dr. Steinman’s opinion
that there was an appropriate temporal association between vaccination and the onset of
Petitioner’s Bell’s palsy.
41

Case 1:18-vv-01782-UNJ Document 98 Filed 11/27/23 Page 42 of 42
Therefore, Petitioner has provided preponderant evidence satisfying Althen prong three.
D. Alternative Causation
Because the undersigned concludes that Petitioner established a prima facie case,
Petitioner is entitled to compensation unless Respondent can put forth preponderant evidence
“that Petitioner’s injury was in fact caused by factors unrelated to the vaccine.” Whitecotton v.
Sec’y of Health & Hum. Servs., 17 F.3d 374, 376 (Fed. Cir. 1994), rev’d on other grounds sub
nom., Shalala v. Whitecotton, 514 U.S. 268 (1995); see also Walther v. Sec’y of Health & Hum.
Servs., 485 F.3d 1146, 1151 (Fed. Cir. 2007). As discussed above in the Althen prong two
analysis, the undersigned found Respondent failed to establish evidence to show that Petitioner’s
Bell’s palsy was caused by a source other than vaccination. Thus, Respondent did not prove by a
preponderance of evidence that Petitioner’s injury is “due to factors unrelated to the
administration of the vaccine.” § 13(a)(1)(B).
VI. CONCLUSION
For the reasons discussed above, the undersigned finds that Petitioner has established by
preponderant evidence that her flu vaccine caused her Bell’s palsy. Therefore, Petitioner is
entitled to compensation. A separate damages order will issue.
IT IS SO ORDERED.
s/Nora Beth Dorsey
Nora Beth Dorsey
Special Master
42

================================================================================
DOCUMENT 2: USCOURTS-cofc-1_18-vv-01782-1
Date issued/filed: 2026-04-28
Pages: 21
Docket text: PUBLIC ORDER/RULING (Originally filed: 3/26/2026) regarding 163 Findings of Fact & Conclusions of Law. Signed by Special Master Nora Beth Dorsey. (aevw) Service on parties made.
--------------------------------------------------------------------------------
Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 1 of 21
In the United States Court of Federal Claims
OFFICE OF SPECIAL MASTERS
Filed: March 26, 2026
* * * * * * * * * * * * * * * * * * * * * * * * *
LISA L. ARREDONDO, * PUBLISHED
*
Petitioner, * No. 18-1782V
*
v. * Special Master Nora Beth Dorsey
*
SECRETARY OF HEALTH * Ruling Awarding Damages; Influenza
AND HUMAN SERVICES, * (“Flu”) Vaccine; Bell’s Palsy; Pain and
* Suffering; Life Care Plan.
Respondent. *
*
* * * * * * * * * * * * * * * * * * * * * * * * *
Lisa Roquemore, Law Office of Lisa A. Roquemore, Rancho Santa Margarita, CA, for Petitioner.
Kimberly Shubert Davey, U.S. Department of Justice, Washington, DC, for Respondent.
RULING ON DAMAGES1
On November 19, 2018, Lisa L. Arredondo (“Petitioner”) filed a petition for
compensation under the National Vaccine Injury Compensation Program (“Vaccine Act” or “the
Program”), 42 U.S.C. § 300aa-10 et seq. (2018)2 alleging that she suffered Bell’s palsy as the
result of an influenza (“flu”) vaccination administered on September 21, 2017. Petition at 2
(ECF No. 1). On October 31, 2023, the undersigned issued a Ruling on Entitlement, finding
Petitioner entitled to compensation. Ruling on Entitlement dated Oct. 31, 2023 (ECF No. 92).
1 Because this Ruling contains a reasoned explanation for the action in this case, the undersigned
is required to post it on the United States Court of Federal Claims’ website and/or at
https://www.govinfo.gov/app/collection/uscourts/national/cofc in accordance with the E-
Government Act of 2002. 44 U.S.C. § 3501 note (2018) (Federal Management and Promotion of
Electronic Government Services). This means the Ruling will be available to anyone with
access to the Internet. In accordance with Vaccine Rule 18(b), Petitioner has 14 days to
identify and move to redact medical or other information, the disclosure of which would
constitute an unwarranted invasion of privacy. If, upon review, the undersigned agrees that the
identified material fits within this definition, the undersigned will redact such material from
public access.
2 The National Vaccine Injury Compensation Program is set forth in Part 2 of the National
Childhood Vaccine Injury Act of 1986, Pub. L. No. 99-660, 100 Stat. 3755, codified as amended,
42 U.S.C. §§ 300aa-10 to -34 (2018). All citations in this Ruling to individual sections of the
Vaccine Act are to 42 U.S.C. § 300aa.

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 2 of 21
The parties were unable to resolve damages and requested that the Court enter a schedule
for damages briefs. Since then, the parties’ briefs have been filed.
After consideration of all of the evidence, and for the reasons described below, the
undersigned finds that Petitioner is entitled to $180,000.00 for actual pain and suffering. This
Ruling also awards the costs for certain disputed items in the life care plan.
I. PROCEDURAL HISTORY
Petitioner filed her petition on November 19, 2018. Petition. The early procedural
history from November 2018 through March 2023 was set forth in the undersigned’s Ruling on
Entitlement and will not be repeated here. See Ruling on Entitlement at 4-5.
Following the undersigned’s Ruling on Entitlement, the parties engaged in settlement
discussions but were not able to resolve this matter informally. The parties indicated that certain
life care plan items as well as pain and suffering remained in dispute.3 See Joint Status Report
(“Rept.”), filed Oct. 16, 2025 (ECF No. 156); Joint Status Rept., filed Mar. 25, 2026 (ECF No.
162). The parties briefed the issue of pain and suffering and provided additional evidence in
support of the parties’ positions on the remaining items in dispute in the life care plan. See
Petitioner’s Exhibits (“Pet. Exs.”) 114-22; Respondent’s (“Resp.”) Exs. J-K; Pet. Damages Brief
in Support of Her Pain Suffering and Emotional Distress (“Pet. Br.”), filed June 19, 2025 (ECF
No. 146); Resp. Response to Pet. Br. (“Resp. Br.”), filed Sept. 17, 2025 (ECF No. 152); Pet.
Reply Damages Br. in Support of Her Pain Suffering and Emotional Distress (“Pet. Reply Br.”),
filed Oct. 16, 2025 (ECF No. 155).
This matter is now ripe for adjudication.
II. FACTUAL HISTORY4
A. Medical Record History
Petitioner was a 51-year-old registered nurse at the time of her flu vaccination on
September 21, 2017. Pet. Ex. 1 at 1; Transcript (“Tr.”) 7. Petitioner’s medical history prior to
3 The parties were able to resolve lost wages ($1,552.88), out-of-pocket expenses ($10,312.87),
and most items in the life care plan. See Joint Status Report (“Rept.”), filed June 6, 2025, at 1
(ECF No. 140); Joint Status Rept., filed Mar. 2, 2026 (ECF No. 159). The parties confirmed that
the only items in dispute are past and future pain and suffering and certain life care items. Joint
Status Rept., filed Mar. 25, 2026 (ECF No. 162).
4 This factual history was largely taken from the undersigned’s Ruling on Entitlement as well as
the parties’ damages briefs, with edits from the undersigned, as the undersigned finds the parties
accurately depicted the facts and circumstances here. See Ruling on Entitlement at 5-11; Pet. Br.
at 2-11; Resp. Br. at 2-9.
2

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 3 of 21
vaccination did not suggest facial weakness or a neurological condition. Resp. Br. at 2-3 (citing
Pet. Ex. 3 at 20-26).
Thirteen days later, on October 4, 2017, Petitioner presented to her primary care
physician (“PCP”) for paresthesia, “drooping right eye,” and pain in her ear that started three
days prior. Pet. Ex. 3 at 27. Associated symptoms included “difficulty closing eye, drooping
lower eyelid, facial muscle weakness[,] and pain near the ear.” Id. Petitioner was diagnosed
with paresthesia and Bell’s palsy, prescribed acyclovir and steroids, and magnetic resonance
imaging (“MRI”) was ordered. Id. at 29-30. A brain MRI performed without contrast on
October 9 showed “[n]o significant intracranial abnormality.” Id. at 32.
On October 10, 2017, Petitioner’s employer submitted a Vaccine Adverse Event
Reporting System (“VAERS”) report on her behalf. Pet. Ex. 2. The adverse event was described
as facial paralysis and neck pain following the flu vaccine. Id. at 3. It reported that Petitioner
“woke up the night of [October 1, 2017] with pain in neck and left sided drooping[5] which ha[d]
not yet resolved;” diagnosis was Bell’s palsy. Id.
Petitioner returned to her PCP on October 11, 2017 “for evaluation of Bell’s palsy with
inability to smile and pain in right ear.” Pet. Ex. 3 at 33. Associated symptoms included
difficulty drinking, eating, and speaking, facial muscle weakness, pain near the ear, difficulty
closing eye, drooping lower eyelid, drooling, hearing loss, and lack of tears or sensitivity to light.
Id. Petitioner reported “her [Bell’s] palsy [was] somewhat improving but she continue[d] to
have pain above her right ear [and] right side of face.” Id. Diagnosis was Bell’s palsy. Id. She
was prescribed prednisone and tramadol for pain and was instructed to follow up if there were no
improvements in symptoms in two weeks. Id.
At an optometry appointment in December 2017, Petitioner reported a “noticeable
decline or change in vision.” Pet. Ex. 5 at 4. Notes indicated Petitioner was “[r]eferred to Patti
Wieissler for acupuncture for [r]ight side [B]ell’s palsy [with] October 2017 onset.”6 Id. at 5.
On March 28, 2018, Petitioner followed up with her PCP. Pet. Ex. 3 at 40. Petitioner
reported she was “still having issues from her Bell’s palsy,” including right eye twitching when
she smiled, soreness on the right side of her face, some hearing loss in her right ear, and
occasional blurry vision in her right eye. Id.
Petitioner presented to neurologist Dr. Peter Tarbox for a neurological consultation for
her eight-month history of Bell’s palsy on June 18, 2018. Pet. Ex. 7 at 1. Petitioner had
“numbness and tingling to the face and some dryness of her vision. She ha[d] decreased field
loss to the right.” Id. Petitioner reported she had “some recovery with some kinesis noted.” Id.
5 Reference to left-sided drooping appears to be an error, since all other records document
drooping of the right eye and right-sided symptoms. At the entitlement hearing, Petitioner
discussed this note and testified that the report inaccurately noted her facial drooping to be on the
left side instead of the right. Tr. 12-14.
6 It is not clear whether Petitioner underwent acupuncture as no records were filed.
3

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 4 of 21
It was also noted she had “no significant lower [seventh] nerve recovery resulting with flattening
of the smile.” Id. Neurological examination showed “right peripheral VII [cranial nerve]
weakness on the right.” Id. at 3. “She [was] able to close her eyes but [did] have orbicularis
oculi eye weakness. She [was] [] able to elevate the right eyebrow. Her orbicularis oris
appear[ed] to be weak. She ha[d] some decreased sensitivity to touch subjectively in the right
VII [and eight cranial nerve regions].”7 Id. The remaining cranial nerves were intact. Id. Dr.
Tarbox’s impression was Bell’s palsy and polyneuropathy. Id. at 3-4. He recommended
electrical stimulation, massages, and acupuncture. Id. at 4. Dr. Tarbox advised Petitioner that
given she was “eight to nine months [into] recovery there may be minimal significant recovery
from [her current] state,” but that nerve recovery was still possible for up to 18 months. Id.
On August 13, 2018, Petitioner followed up with Dr. Tarbox. Pet. Ex. 7 at 18. She
reported “no Bell’s palsy flare ups” since her last visit but continued to have “numbness and
tingling on [her] right side with a mild facial droop.” Id. Dr. Tarbox recommended Bell’s palsy
specific physical therapy (“PT”). Id. at 20.
Petitioner completed three sessions of PT from August 28 to September 11, 2018 with
physical therapist Amapola Mallari. Pet. Ex. 8 at 1-8. At the initial PT consultation, an
examination documented decreased right-sided brow elevation, brow depression, and a right-
sided decrease in smiling, puckering, nostril flaring, and platysma. Id. at 2. By her third and last
PT session, Petitioner demonstrated improvements with whistling, laughing, and smiling. Id. at
7.
Petitioner returned to her PCP on September 27, 2018. Pet. Ex. 3 at 45. She was still
experiencing a “drooping right eye, inability to smile, and pain in [her] right ear.” Id. Petitioner
requested a referral to an ear, nose, and throat (“ENT”) specialist. Id. at 47.
On September 28, 2018, Petitioner presented to ENT Dr. Walter Bain. Pet. Ex. 6 at 1.
History indicated she had hearing loss, taste decrease, and vertigo due to her Bell’s palsy. Id.
She also reported a “wind type sound” in her right ear with smiling, eating, or talking. Id.
Examination showed a 50% reduction in strength on the right side of her face, cerumen
impaction, and mild bilateral sensorineural hearing loss with audiology measurements in the
normal range.8 Id. at 2-4. Dr. Bain removed Petitioner’s cerumen impaction and prescribed a
nasal spray to treat her eustachian tube dysfunction. Id. at 4-5.
Petitioner had a speech evaluation on January 29, 2019. Pet. Ex. 40 at 1. Petitioner
described difficulty eating and drinking as well as pain when she moved the right side of her
face. Id. Petitioner also reported “sharp pain” during facial exercises and “pressure in her ear
when she smiles.” Id. Examination revealed Petitioner had a moderate right-sided facial droop
when smiling; she could not contain air pressure in her mouth due to right cheek weakness; and
7 On neurological examination, Dr. Tarbox also noted decreased sensitivity in the distribution of
the eighth cranial nerve. Pet. Ex. 7 at 3.
8 The audiogram showed mild relative elevation thresholds but were largely within normal limits.
Pet. Ex. 38 at 1.
4

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 5 of 21
she could not raise her right eyebrow. Id. at 2. Petitioner had no issues chewing but her swallow
test revealed mild difficulty securing a bolus and mild right-sided anterior leakage. Id.
Assessment noted Petitioner had mild oral dysphagia secondary to her facial weakness due to
Bell’s palsy. Id. at 3. After reviewing her history and prior testing, the speech therapist did not
recommend speech therapy due to Petitioner’s “very poor rehabilitative potential.” Id. It was
also noted that Petitioner was “not expected to make progress via skilled speech therapy
services.” Id.
On March 1, 2019, Petitioner saw her dentist9 and asked if Bell’s palsy could impact her
oral health. Pet. Ex. 41 at 3. She was told that if her condition causes dry mouth, it could result
in increased caries and higher risk for “burning mouth syndrome, oral mucositis[,] and . . . fungal
infections.” Id. The dentist recommended oral lubricants, like NeutraSal, to alleviate dry mouth
and provide protective benefits. Id. Petitioner was also advised to seek dental care more than
twice a year to monitor her oral health. Id. On examination, Petitioner had good oral hygiene,
with only light plaque, and she was encouraged to continue brushing and flossing. Pet. Ex. 43 at
1.
On March 5, 2019, Petitioner presented Dr. Lance Jackson, another ENT, for complaints
of dizziness, hearing loss, ear pain, pain swallowing, difficulty with speech, and facial weakness.
Pet. Ex. 38 at 1-3. Petitioner’s Bell’s palsy symptoms included facial weakness, right eye/mouth
dryness, right aural fullness, right tinnitus, dizziness/imbalance, right-sided constant aural
fullness, and temporary right-sided hearing loss. Id. “She also [] noted that her right sided
hearing [] decreased when the aural fullness [was] severe.” Id. Petitioner’s dizziness/imbalance
“occurred more in the morning and late afternoon” and was of “mild severity, although it []
fluctuated in severity and [] worsen[ed] when her right aural fullness [was] most pronounced.”
Id. Her tinnitus was described as “humming” that “occurred 1-2 times daily and [] lasted for
seconds at a time.” Id. Lastly, she reported “right sided pain below her right ear which
radiate[d] to her jaw.” Id. Over the first three months after her diagnosis, Petitioner reported a
50% improvement in facial function, however, she continued to have residual facial weakness.
Id. Petitioner also “reported allergy symptoms described as nasal congestion, nasal discharge,
postnasal drip, and eye dryness.” Id.
Petitioner’s examination by Dr. Jackson, including audiogram and tympanograms, was
normal. Pet. Ex. 38 at 2-5. House-Brackman10 grade was noted to be “II-III/VI” on the right
side. Id. at 4. Petitioner had another MRI which was normal. Id. at 8. The treatment plan
included further testing to find the cause of the dizziness and hearing symptoms. Id. at 5-6.
Facial physical therapy was also recommended. Id. at 5.
9 Despite evidence of significant prior dental work, including several missing teeth, cosmetic
Lumineers, and crowns and fillings, no dental records were filed for care between 2012 and
March 2019. See Pet. Exs. 41, 43, 100.
10 The House-Brackmann facial nerve grading system is the most widely applied scoring system
“available to clinically assess the severity of peripheral facial nerve palsy.” Pet. Ex. 19 at 2 (A.
Greco et al., Bell’s Palsy and Autoimmunity, 12 Autoimmun. Rev. 323 (2012)). The House-
Brackman grading scale goes from Grade 1 (normal) to Grade 6 (total paralysis). Id. at 3 tbl.b.
5

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 6 of 21
On March 19, 2019, Petitioner was examined by plastic surgeon, Dr. Agustin Cornejo,
for right-sided asymmetry of her forehead, brows, and mouth. Pet. Ex. 39 at 1-2. Dr. Cornejo
recommended Botox therapy. Id. at 3.
On May 30, 2019, Petitioner presented to Dr. Cristo Calle, internist, with complaints of
dry eyes and mouth and right-sided face pain rated 2-3/10. Pet. Ex. 42 at 1. Dr. Calle
recommended eye drops, saliva stimulants, acupuncture, and Botox as treatment. Id. at 3-4.
On June 24, 2019, Petitioner presented to ophthalmologist Dr. Sean Paul with a chief
complaint of ptosis for the past two years, which Dr. Paul labeled as moderate in severity. Pet.
Ex. 44 at 1. Dr. Paul diagnosed Petitioner with lagophthalmos in the right eye (the inability of
the upper and lower eyelids to meet upon closing) and informed her that the condition may
improve without treatment. Id. Dr. Paul discussed surgical options, but Petitioner chose to defer
a decision on surgery at that time. Id. at 2.
A few months later, on October 2, 2019, Petitioner had an initial PT examination with
Diana Schonoff, Doctor of PT, at Garden Ridge Physical Therapy & Wellness Center. Pet. Ex.
45 at 1. It was noted that Petitioner got the flu vaccine on September 21, 2017, then two weeks
later, on October 1, 2017, developed “pain posterior [right] ear to jaw . . . then facial paralysis
[right] side.” Id. at 2. Petitioner reported she did not go to PT as previously recommended “but
[she was] ready now.” Id. Petitioner’s chief complaints included pain, swelling, and numbness
in her right facial, ear, and neck region as well as issues with eating and swallowing. Id. She
reported feeling “self conscious eating or talking in front of people due to synkinesis eye closure
with mouth movements.” Id. House-Brackman was a grade III. Id. Dr. Schonoff recommended
PT two to three times per week. Id. at 3-4. Petitioner attended a total of 18 sessions through
November 18, 2019. Id. at 18. During PT, Petitioner was consistently noted to have facial
swelling due to lymphedema, which was treated with a pressure garment, and she demonstrated
some improvement with increased facial strength, decreased eye twitching, and significantly
decreased spasms and tightness. Id.
One year later, on October 23, 2020, Petitioner had a telehealth visit with Dr. Maria
Alvarez of Neurology Associates for her Bell’s palsy. Pet. Ex. 56 at 1. Petitioner reported an
involuntary right-sided facial twitch that was “worse when she [was] tired” and a “heaviness of
[her] right face.” Id. Petitioner reported that the involuntary twitch affected her speech but did
not cause any slurring or choking. Id. On examination, Dr. Alvarez noted mild right-sided
hemifacial spasm and mild right-sided facial weakness. Id. at 2. The use of Botox injections and
possible gamma knife surgery were discussed. Id.
Petitioner began Botox treatment in December 2020 and continued to receive Botox
through December 2024. Pet. Ex. 59 at 1, 3; Pet. Ex. 60 at 1; Pet. Ex. 61 at 1, 3-4; Pet. Ex. 62 at
1-2, 5; Pet. Ex. 64 at 2; Pet. Ex. 89 at 1-4; Pet. Ex. 93 at 1-12; Pet. Ex. 99 at 1-4; Pet. Ex. 114 at
1-4. Petitioner reported her facial spams were “stable” and getting “better with therapy.” Pet.
Ex. 62 at 1; see also Pet. Ex. 61 at 1.
6

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 7 of 21
On October 25, 2021, Petitioner saw her dentist for a bi-annual appointment. Pet. Ex.
100 at 3. Petitioner complained of sensitivity when biting. Id. Light tarter buildup was noted on
examination. Id.
Petitioner returned to the dentist six months later, on April 28, 2022, for sensitivity in a
tooth that had a ten-year-old filling, and she was found to have an abscess. Pet. Ex. 101 at 1.
She had a root canal and crown in May 2022. Id. at 1-3. In June 2022, she underwent additional
dental work due to fractures in two different teeth. Id. at 4-5. In August 2022, Petitioner began
treatment with Invisalign. Id. at 5-6.
On March 9, 2023, Petitioner saw her dentist for a routine periodontal examination, and
she was noted to have gingival inflammation due to a buildup of calculus at the gumline. Pet.
Ex. 101 at 7-8. There were no concerns noted regarding dry mouth, but Petitioner was
encouraged to brush three times a day with an electric toothbrush and to floss nightly. Id. at 8.
On September 12, 2023, at Petitioner’s next routine dental examination, she was noted to have
plaque-induced gingival inflammation. Id. at 9. Petitioner was again counseled to brush three
times a day and to floss nightly. Id. at 10. On September 18, 2023, Petitioner received a crown
on another tooth that had a filling that was over ten years old. Id. at 10-11.
On July 25, 2023, Petitioner saw an optometrist who noted excess tearing and mild
bilateral conjunctival injection consistent with allergies. Pet. Ex. 95 at 2. Petitioner also
reported significant itchiness in both eyes. Id. The optometrist also observed that Petitioner’s
right eyelid fell away from the normal position but considered that finding of “low clinical
significance.” Id. Assessment was lagophthalmos of both right eyelids, and she was prescribed
lubricating and allergy eye drops for both eyes. Id. Her eyeglass prescription was updated, and
her correctible vision was 20/20 in each eye. Id.
On September 18, 2024, Petitioner was evaluated for bilateral ptosis, and a plan was
made for a brow lift. Pet. Ex. 108 at 3-4. Her “droopy eyelids [were] “moderate in severity,
right upper eyelid and left upper eyelid [were] equal.” Id. at 1.
B. Declarations, Testimony, and Letters
1. Petitioner
At the hearing, Petitioner testified she had been a nurse at Baptist Medical Center for 15
years prior to the flu vaccination at issue. Tr. 7-11. She recalled that prior to September 2017,
she was in good health. Tr. 12. She did not have any face, eye, or lip issues prior to the flu
vaccine besides needing reading glasses. Tr. 16.
About two weeks after receiving her vaccination, Petitioner developed “a really sharp
pain behind [her] [right] ear” which was unusual. Tr. 14. She testified it was “really painful,”
and “something new to [her]” as it had never happened before. Tr. 15. She “had never been
seen by a physician for ear problems.” Id. On October 2, 2017, Petitioner went to work, because
she took some pain medicine and “the pain had subsided.” Id. When she got to work, she felt “a
little weird, tingling, [and] numbness . . . to the right side of [her] tongue.” Id. On October 3,
7

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 8 of 21
Petitioner was off from work and when she woke up that morning, she noticed a drooping of her
face. Id. She was unable to brush her teeth without difficulty. Id. Her eye was also affected.
Id. Her face was paralyzed, “like frozen,” and she was unable to close her eye. Id.
Because Petitioner had seen Bell’s palsy before in the scope of her work as a nurse, she
thought she was having either Bell’s palsy or a stroke. Tr. 20. Accordingly, Petitioner recalled
that she sought treatment from her PCP “the day after getting Bell’s palsy, so it was October 4,
2017.” Id. Petitioner was given medication and steroids. Tr. 22.
Petitioner recalled that she returned to her PCP on October 11, 2017 because her
condition was worsening. Tr. 22. She was having “a lot of dryness to [her] eye, dryness to [her]
mouth, . . . a lot of pain, [and] a lot of spasms, like charley horses [in] back of [her] ear to the jaw
area, pulling of [her] neck.” Id. She had problems eating and drinking, drooling, and sensitivity
of her ear and right side. Tr. 22-23. Because she could not close her eye, it was dry and irritated.
Tr. 23. She developed blurred vision and used lubricating ointment and eyedrops. Id. Petitioner
wore an eye mask at night to sleep and when she showered, she put a towel band over her eye to
prevent soap from getting into her eye. Tr. 24.
In her testimony, Petitioner stated that her final diagnosis was Bell’s palsy. Tr. 23. She
testified that her treating physicians believed the cause was “possibl[y] [the] flu vaccine.” Id.
She saw a neurologist in June 2018 due to continued symptoms. Tr. 25. Recommended
treatment included physical therapy, Botox, and acupuncture. Tr. 25-26. Petitioner underwent
all of the recommended treatment.11 Id. Petitioner also described the photographs filed showing
the effect of Bell’s palsy on her facial appearance. Tr. 17-19.
As of the date of the hearing, October 18, 2022, Petitioner was still experiencing
“synkinesis, [] blurriness, and vision problems.” Tr. 26. She was still unable to completely close
her eye and had continued dryness of her eye and mouth. Id. She also had difficulty chewing
food and had spasms of the right side of her face. Id.
Petitioner also filed two supplemental declarations in 2025. Pet. Exs. 119-20. In the first
declaration, signed June 17, 2025, Petitioner explained her Bell’s palsy symptoms have been
“traumatic and horrifying,” and she has continued to suffer “significant pain, depression,
anxiety[,] and overall loss of self esteem.” Pet. Ex. 119 at ¶ 4. She “felt helpless and
overwhelmed,” “lost [her] marriage,” “sought counseling from [her] trusted Pastor . . . to assist
with [her] psychological wounds, depression[,] and [] anxiety.” Id. Petitioner explains she
“ha[s] had a difficult time coping with [her] disfigurement and [] pain,” which was a 10/10 in the
beginning and is now a 3-4/10, constant, and dull. Id. She also “worr[ies] about [] upcoming
surgeries and recovery. It’s the fear of the unknown and potential complications . . . [as well as]
post surgery pain and bruising.” Id. at ¶ 5.
Petitioner asserts her Bell’s palsy “has had a very negative impact on [her] self image;”
she continues to avoid photographs, social interactions, and eye contact because she is self-
conscious about her face. Pet. Ex. 119 at ¶ 6. Her “decrease in social interaction has led to
11 Acupuncture records do not appear to be filed.
8

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 9 of 21
loneliness, isolation, and depression.” Id. And she finds it “challeng[ing] trying to mentally and
emotionally cope with all of these issues.” Id. She also explained that she continues to
experience loss of taste, dryness, and numbness and continues to drop food and liquids from her
mouth. Id. Petitioner maintains her Bell’s palsy has affected her “daily life, work life, social
life[,] and romantic life.” Id. at ¶ 7.
The second declaration, signed October 13, 2025, addresses the effect of her Bell’s palsy
on her marriage and family life. Pet. Ex. 120. Petitioner asserts the nature and quality of her
marriage was impacted because her husband immediately moved to Florida for contract work
and only returned intermittently a few times. Id. at ¶ 5. Petitioner is “certain” her Bell’s palsy
impacted her marriage. Id. She maintains they have been separated “since [he] left” and “[h]e
has lived in Florida since [her] injury.” Id. at ¶¶ 6-7. She explained she “ha[s] not had the
emotional strength to go through a dissolution,” and thus, they are technically still married. Id. at
¶ 7. Despite this, she maintains “that does not make [her] emotional issues attendant to [her]
Bells Palsy issues and [her] husband leaving any less devastating.” Id.
2. Petitioner’s Mother, Esther Arredondo
Petitioner’s mother, Esther Arredondo, signed a declaration on October 13, 2025, to
support Petitioner’s assertion that her husband left her due to her Bell’s palsy. Pet. Ex. 121. She
lived with Petitioner from 2018 to May 2025. Id. at ¶¶ 4-5. She explained that Petitioner’s
husband, Martin, did not live with Petitioner at this time. Id. at ¶ 6. For the first three years of
Petitioner’s Bell’s palsy injury, he had six-month work contracts out of state and would return
for a week or two until his next contract began. Id. Ms. Arredondo maintains that he would
return “only for his benefit” and that “[t]his was not a marriage.” Id. “He was not by any stretch
of the imagination a husband to [Petitioner],” according to Ms. Arredondo, and he has not
returned since 2020. Id. Ms. Arredondo “believe[s] [Petitioner’s] husband left because he could
not deal with [Petitioner’s] bell’s palsy and her marred beauty.” Id. at ¶ 7.
Ms. Arrendondo also explained what she has witnessed Petitioner go through, physically
and emotionally, since her Bell’s palsy diagnosis. Pet. Ex. 121 at ¶ 7. Petitioner continues to
have facial pain and tightness, she drools when eating, her right eye twitches and squints when
she speaks and blinks, and she has a lopsided smile, which has made her embarrassed to take
photographs and eat in front of others. Id. Ms. Arredondo noted Petitioner “believes her father
was overworked from maintaining [Petitioner’s] 5-acre home,” which led to his heart attack and
death. Id. Ms. Arredondo also explained Petitioner struggles financially due to the lack of
support from her husband, which required a change in her work schedule to compensate. Id.
3. Reverend Mike Barron
Reverend Mike Barron has known Petitioner for over 40 years. Pet. Ex. 116 at 1. He
stated that he “witnessed the pain and suffering she was experienc[ing] following Bell’s [p]alsy
and what effect it had on her life.” Id. Petitioner reported “considerable facial pain, sadness[,]
and discouragement.” Id. She “presented herself feeling distressed, frustrated, [and] anxious
because her face was significantly distorted” and she was embarrassed of her difficulty speaking
and eye and mouth spasms. Id. Petitioner also reported her Bell’s palsy affected her daily
9

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 10 of 21
routines, work, social life, and marriage; she no longer had the “desire” or “motivation” to eat
out at restaurants or attend church functions, and she was hesitant to take photographs with
family and friends. Id.
III. PAIN AND SUFFERING
A. Parties’ Pain and Suffering Contentions
1. Petitioner’s Contentions
Petitioner requests a pain and suffering award of $250,000.00. Pet. Br. at 15; Pet. Reply
Br. at 15. If Petitioner is not granted the statutory cap of $250,000.00 for past pain and suffering,
she requests future pain and suffering until she meets the cap. Pet. Reply Br. at 15.
Petitioner maintains that she has been cognizant of the pain and emotional distress she
has endured due to her Bell’s palsy since the onset. Pet. Br. at 11.
As to duration, Petitioner contends her injury “has been anything but brief;” she has
suffered since October 2017, over eight years, and continues to suffer. Pet. Br. at 11.
For severity of injury, Petitioner maintains “[h]er life has not been and never will be the
same.” Pet. Br. at 11-12. Petitioner summarizes her Bell’s palsy resulted in her “losing [] her
marriage and the ability to be kissed and be intimate;” has had an “impact on her psyche” due to
her “[n]ot being able to smile, kiss, [and] eat comfortably in front of people;” has led her to be
unable to socialize like she used to; and has resulted in pain. Id. at 12.; see also Pet. Reply Br. at
6. She hopes recommended surgeries will fix her face disfigurement so that her self-esteem can
improve; however, she believes “[i]t is unlikely her marriage will heal after this length of time.”
Pet. Br. at 12. And even after these surgeries, she will continue to suffer “due to eye issues and
sensitivity of hearing.” Id. Overall, she classifies her facial palsy as “at least[] moderate” as
evidenced by the need for Botox and surgery.” Pet. Reply Br. at 11.
Petitioner details all that she has endured due to her Bell’s palsy. Pet. Reply Br. at 3-4.
She has difficulty eating, drinking, and brushing her teeth; she is embarrassed to eat in front of
others; she has lost her sense of taste on the right side of her mouth, and the “decrease in her
ability to taste has [had] a significant impact on the pleasure and gratification she used to have in
terms of eating food;” she has dryness and sensitivity to temperature on the right side of her
mouth; she has difficulty speaking and saying certain words/letters as well as smiling; she has
synkinesis and involuntary muscular movements accompanying voluntary movement; she has
right eye dryness due to her inability to close it, requiring eye drops, ointments, and tape to close
her eye, which has also affected her vision; and she has hyperacusis (where soft sounds cannot
be heard and loud sounds are intolerable or distorted), ear pain, and hearing loss. Id. These
issues, Petitioner asserts, have had a negative impact on her work life, social life, and activities
of daily living. Id. at 4, 6.
Her Bell’s palsy has also greatly impacted her marriage and social life. Pet. Reply Br. at
6. “Her mood can change from irritable to very sensitive. . . . She is very sensitive to how she
10

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 11 of 21
looks as now she has a disfigured face and believes such has had an impact with her husband,
who took a three month agency contract position in Florida.” Id. Petitioner asserts her marriage
is still impacted by her injury; though they are not divorced, they continue to live separate lives
in different states. Id. at 8.
Petitioner maintains her case is unique in the Vaccine Program due to her injury of Bell’s
palsy and her pain and suffering and emotional distress. Pet. Br. at 14; Pet. Reply Br. at 13-14.
Petitioner cited to Fu et al.12 to support her contentions. Pet. Br. at 14-15 (citing Pet. Ex. 117).
Fu et al. studied the psychological distress in 103 patients with facial palsy. Pet. Ex. 117 at 1.
The authors found “[f]emales had significantly higher levels of anxiety compared to males,”
which they noted was “possibly owing to the great emphasis placed on their appearance by
society,” while “[f]emale and male participants were equally likely to experience high levels of
depression.” Id. at 1, 4. The number of female and male participants was not noted. See id. at
1-5. The study found “significant associations between participants’ illness perceptions and their
level of distress” as well as “strong evidence that unplanned alteration of the face will cause
psychosocial problems.” Id. at 1, 5. Petitioner asserts the “facial disfigurement and the
functional ramifications described in [Fu et al.]” is akin to what she went through—“[she] has
anxiety and depression, her quality of life has been diminished[,] and she has suffered from
impaired interpersonal relationships.” Pet. Br. at 15; see also Pet. Reply Br. at 6.
In her reply brief, Petitioner distinguishes her case from the petitioner in Sturdevant, who
also suffered Bell’s palsy with permanent residual effects. Pet. Reply Br. at 12 (citing
Sturdevant v. Sec’y of Health & Hum. Servs., No. 17-172V, 2024 WL 1045145 (Fed. Cl. Spec.
Mstr. Feb. 12, 2024)). Mr. Sturdevant had mild disfigurement, his records documented a
“pleasant face,” and he did not undergo invasive treatments or procedures, while Petitioner here
continues to have facial disfigurement, she received Botox treatments and will continue to do so,
and she will have a corrective surgery. Id.; see also Sturdevant, 2024 WL 1045145, at *7-8, *10.
Petitioner maintains she is entitled to an award of no less than $250,000.00 for her pain
and suffering and emotional distress that she has suffered over the last eight years and will
continue to suffer for at least a few more years. Pet. Reply Br. at 15.
2. Respondent’s Contentions
Respondent argues that based on the facts of this case, Petitioner should be awarded
$140,000.00 for pain and suffering. Resp. Br. at 1. Respondent contends that Petitioner is not
entitled to the pain and suffering statutory cap of $250,000.00 because she “is not among the
most severely injured petitioners in the Program, she has achieved some recovery with treatment,
and her case is distinguishable from other cases in which petitioners were awarded the statutory
cap for pain and suffering.” Id. at 12.
First, Respondent does not dispute awareness of injury. See Resp. Br. at 1-22.
12 L. Fu et al., Psychological Distress in People with Disfigurement from Facial Palsy, 25 Eye
1322 (2011).
11

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 12 of 21
Respondent compares this case with Sturdevant, arguing Sturdevant is instructive as it is
the only Bell’s palsy reasoned damages case with “roughly comparable facts.”13 Resp. Br. at 12-
15, 21. Petitioner here and the petitioner in Sturdevant “suffered similar symptoms with similar
sequela,” and both will likely never fully recover. Id. at 13-14. Respondent acknowledges there
are differences between Petitioner’s case and that of the petitioner in Sturdevant. Id.
Respondent notes Petitioner here received more treatment than Mr. Sturdevant, including two
rounds of PT and three Botox injections each year since December 2020, while Mr. Sturdevant’s
treatment was limited to steroids, physical therapy, and home exercises. Id. at 14. And
Respondent agrees “there is evidence [Petitioner] will require ongoing Botox injections and
possible surgery to correct her persistent facial asymmetry,” which was not present in Mr.
Sturdevant’s case. Id. at 15. Respondent maintains Sturdevant is instructive “as [P]etitioner’s
clinical course was similar to Mr. Sturdevant’s;” however, because “[P]etitioner pursued far
more treatment than Mr. Sturdevant, her award should be higher, but no more than $140,000.00.”
Id. at 18.
Respondent next notes that “[w]hile [P]etitioner states that she has suffered more
extensive pain and suffering, the record as a whole does not substantiate several of her
concerns.” Resp. Br. at 15. First, with regard to Petitioner’s assertion her marriage was
negatively impacted by her Bell’s palsy, Respondent notes the records do not support her claim.
Id. Respondent acknowledges Petitioner feels her husband left her due to her Bell’s palsy, but
notes he left to fulfill an out-of-state employment contract in Florida and would return home
when not on contract. Id. There is no objective evidence on the record to support her assertion
that her husband left due to her Bell’s palsy symptoms or that the symptoms caused any issues
within their marriage. Id. (citing Gentile v. Sec’y of Health & Hum. Servs., No. 16-980V, 2020
WL 3618909, at *7 (Fed. Cl. Spec. Mstr. June 5, 2020) (considering a letter, affidavit, and
testimony from the petitioner’s ex-husband stating the vaccine injury was a contributing factor to
their divorce)).
Second, Respondent notes there are no records showing Petitioner sought care for anxiety
or depression related to her Bell’s palsy. Resp. Br. at 16. On two occasions, she reported
psychological symptoms, including “mild intermittent” anxiety, depression, stress, sadness, and
insomnia on September 27, 2018, and feeling self-conscious due to her synkinesis on October 2,
2019. Id. (citing Pet. Ex. 3 at 45; Pet. Ex. 45 at 2). Respondent agrees Petitioner “likely
experienced distress outside of these two dates” but asserts these concerns were not raised with
medical providers. Id.
Third, Respondent points out that medical records do not support Petitioner’s contentions
that she suffered tongue paralysis or cannot entirely close her mouth and cites medical records in
support. Resp. Br. at 17 (citing Pet. Ex. 40 at 2 (a speech evaluation documenting normal tongue
13 Respondent also addresses the cases Petitioner relies upon as comparable, though they
“involv[ed] entirely different conditions, and numerous cases resolved via proffer, where the
underlying facts were not included in a published decision.” Resp. Br. at 18-20. Due these
issues raised by Respondent, as well as the fact there are two reasoned Bell’s palsy damages
decisions to compare to Petitioner’s case here, the undersigned does not discuss these cases.
12

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 13 of 21
strength, range of motion, and sensation; no issues with mastication or swallowing; and only
mild right-sided weakness involving labial closure related to consumption of thin liquids)).
Petitioner also reports a loss of taste; however, she only reported a decrease in taste at an
ENT appointment in September 2018 and not at any future appointments, including an ENT
appointment in May 2019. Resp. Br. at 17 (citing Pet. Ex. 6 at 1; Pet. Ex. 38 at 1).
As to her claims of vision loss, Respondent notes she had eyeglasses prior to her Bell’s
palsy, and there is no evidence of permanent vision changes. Resp. Br. at 17-18 (citing Pet. Ex.
5).
Next, Respondent contends Petitioner’s assertions of speech difficulties are not
substantiated by the record. Resp. Br. at 18. Respondent cited Petitioner’s speech evaluation,
which did not document these issues. Id. (citing Pet. Ex. 40 at 1).
Lastly, Respondent noted Petitioner has not shown her employment has been adversely
affected by her injury as she contends. Resp. Br. at 18.
Respondent maintains Petitioner has failed to show a pain and suffering award of
$250,000.00 is supported by the facts of her case or comparable cases, and instead Respondent
contends a pain and suffering award of $140,000.00 should be awarded to Petitioner given her
overall clinical course and extensive treatment. Resp. Br. at 12, 21.
B. Pain and Suffering Legal Framework
Compensation awarded pursuant to the Vaccine Act shall include “[f]or actual and
projected pain and suffering and emotional distress from the vaccine-related injury, an award not
to exceed $250,000.” § 15(a)(4). Petitioner bears the burden of proof with respect to each
element of compensation requested. Brewer v. Sec’y of Health & Hum. Servs., No. 93-0092V,
1996 WL 147722, at *22-23 (Fed. Cl. Spec. Mstr. Mar. 18, 1996).
There is no formula for assigning a monetary value to a person’s pain and suffering and
emotional distress. I.D. v. Sec’y of Health & Hum. Servs., No. 04-1593V, 2013 WL 2448125, at
*9 (Fed. Cl. Spec. Mstr. May 14, 2013) (“Awards for emotional distress are inherently subjective
and cannot be determined by using a mathematical formula.”); Stansfield v. Sec’y of Health &
Hum. Servs., No. 93-0172V, 1996 WL 300594, at *3 (Fed. Cl. Spec. Mstr. May 22, 1996)
(“[T]he assessment of pain and suffering is inherently a subjective evaluation.”). Factors to be
considered when determining an award for pain and suffering include: (i) awareness of the
injury; (ii) severity of the injury; and (iii) duration of the suffering. I.D., 2013 WL 2448125, at
*9 (quoting McAllister v. Sec’y of Health & Hum. Servs., No. 91-1037V, 1993 WL 777030, at
*3 (Fed. Cl. Spec. Mstr. Mar. 26, 1993), vacated & remanded on other grounds, 70 F.3d 1240
(Fed. Cir. 1995)).
The undersigned may look to prior pain and suffering awards to aid in the resolution of
the appropriate amount of compensation for pain and suffering in this case. See, e.g., Doe 34 v.
Sec’y of Health & Hum. Servs., 87 Fed. Cl. 758, 768 (2009) (finding that “there is nothing
13

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 14 of 21
improper in the chief special master’s decision to refer to damages for pain and suffering
awarded in other cases as an aid in determining the proper amount of damages in this case”).
The undersigned may also rely on her experience adjudicating similar claims. Hodges v. Sec’y
of Health & Hum. Servs., 9 F.3d 958, 961 (Fed. Cir. 1993) (noting that Congress contemplated
the special masters would use their accumulated expertise in the field of vaccine injuries to judge
the merits of individual claims). Importantly, however, it must also be stressed that pain and
suffering is not determined based on a continuum. See Graves v. Sec’y of Health & Hum.
Servs., 109 Fed. Cl. 579 (2013).
In Graves, Judge Merow rejected the special master’s approach of awarding
compensation for pain and suffering based on a spectrum from $0.00 to the statutory
$250,000.00 cap. Judge Merow noted that this constituted “the forcing of all suffering awards
into a global comparative scale in which the individual petitioner’s suffering is compared to the
most extreme cases and reduced accordingly.” Graves, 109 Fed. Cl. at 589-90. Instead, Judge
Merow assessed pain and suffering by looking to the record evidence, prior pain and suffering
awards within the Vaccine Program, and a survey of similar injury claims outside of the Vaccine
Program. Id. at 595.
C. Pain and Suffering Analysis
In determining an award in this case, the undersigned does not rely on a single decision
or case. Rather, the undersigned has reviewed the particular facts and circumstances in this case,
giving due consideration to the circumstances and damages in other cases cited by the parties and
other relevant cases, as well as her knowledge and experience adjudicating similar cases. The
undersigned has reviewed the entire record, including medical records, declarations, expert
reports, and all other evidence that has been filed, and finds an award of $180,000.00 in actual
pain and suffering is fair, reasonable, and appropriate here.
It is appropriate to consider the severity of the injury, awareness of the injury, and
duration of the suffering when determining an award for pain and suffering and emotional
distress. In this case, neither party has raised, nor is the undersigned aware of, any issue
concerning Petitioner’s awareness of suffering. Thus, based on the circumstances of this case,
the undersigned determines Petitioner’s awareness of the injury is not in dispute and she has full
awareness of her suffering.
The factors that particularly influence this Decision are as follows. Regarding duration,
the undersigned finds Petitioner suffered from her injury for more than eight years. Petitioner
received the flu vaccine on September 21, 2017, and approximately 10 days later, on October 1,
2017, she developed Bell’s palsy and she has suffered the residual effects since.
Regarding severity, the undersigned finds Petitioner had a severe injury, for which she
was prescribed pain medication and steroids, underwent an MRI, four years of Botox (three
rounds per year), a total of 21 PT visits, and a speech evaluation, and received medical treatment
from her PCP, neurologists, optometrist and ophthalmologist, ENTs, dentists, and a plastic
surgeon. Petitioner continues to experience ongoing physical sequela, including, but not limited
14

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 15 of 21
to, right-sided facial droop, uneven smile, difficulties speaking, eating, and drinking, inability to
close her right eye resulting in right-eye dryness, and ear pain and hearing loss.
However, some of Petitioner’s assertions are not supported by the medical records.
Petitioner reports hearing loss, but two hearing evaluations determined her hearing was within
normal limits. See Pet. Ex. 6 at 2-4; Pet. Ex. 38 at 1-5. Additionally, Petitioner reports her
Bell’s palsy injury has affected her sense of taste. However, Petitioner complained of a decrease
in taste at one visit in September 2018, and no further visits document any complaints related to
taste. See Pet. Ex. 6 at 1.
Additionally, Petitioner contends her injury affected her employment as well as her
marriage and social life. Regarding her employment, the undersigned finds no evidence in the
records her injury adversely affected her employment. The undersigned is not fully persuaded
by Petitioner’s assertions that her husband left her because of her Bell’s palsy injury.
Petitioner’s husband took pre-planned contract work in Florida that began after her injury onset.
Petitioner did not file evidence from her husband or other objective evidence to show the effects
of her injury on their marriage. Further, Petitioner’s testimony, declarations, and letters from
Petitioner, her mother, and her pastor were submitted after litigation was initiated and a
substantial passage of time after the onset of injury. Case law provides that statements made by
interested parties in anticipation of litigation or years after the events in question are less
persuasive. See Nomick v. Sec’y of Health & Hum. Servs., No. 22-1538V, 2025 WL 2953202,
at *9 (Fed. Cl. Spec. Mstr. Sept. 19, 2025) (“While Petitioner has offered a total of six
declarations, all were signed three or four years after the events in question, and after this matter
was in litigation. The significant gap between the events and the testimony, along with the
litigation context, greatly reduces their evidentiary value.”).
The undersigned has considered prior pain and suffering awards in the parties’ cases to
assist in her determination of an appropriate award. There are two reasoned Bell’s palsy
damages decisions, both from the undersigned.
The first is Sturdevant. Sturdevant, 2024 WL 1045145. There, the undersigned awarded
$100,000.00 for actual pain and suffering. Id. at *1. In that case, petitioner was 51 years of age
at the time of vaccination and injury. Id. at *2. He was unable to raise his eyebrow and had
weakness and difficulty closing his eyelid. Id. at *12. He also had tearing and blurriness in his
affected eye. Id. PT evaluation showed he was unable to close his eye completely and unable to
drink from a cup. Id. After six months of PT, Petitioner’s level of function improved to 90% of
his baseline, however, he was given a facial disability rating of 45 out of 100. Id. He required
eye protection at work and had difficulty with hand-eye coordination and drinking liquids. Id.
Two years after onset, in 2017, his Bell’s palsy was described as “still quite marked.” Id. A
physical examination in 2023, four years later, showed no improvement; the petitioner was still
unable to fully close his affected eye and he had decreased contraction of the relevant eyelid
muscles. Id. He worried about losing his ability to pass the requisite visual tests to maintain his
employment. Id. The award of $100,000.00 acknowledged the petitioner’s long duration of
facial disability (more than eight years), worry about job security, and duration of suffering. Id.
at *13.
15

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 16 of 21
Like Mr. Sturdevant, Petitioner here has continued weakness in her face, issues with the
affected eye, and difficulty drinking liquids. Both Petitioner and Mr. Sturdevant attended PT and
received steroids, but unlike Mr. Sturdevant, Petitioner has received more treatment, including
three rounds of Botox per year since December 2020 and additional PT. Petitioner and Mr.
Sturdevant, both 51 years of age at the time of injury, also expressed concerns regarding
employment and job security, though neither provided evidence of past or current effects on
employment.
The second case is A.B. v. Secretary of Health & Human Services, No. 17-243V, 2025
WL 3187686 (Fed. Cl. Spec. Mstr. Oct. 20, 2025).14 The petitioner in A.B. was 46 years old at
the time of his Bell’s palsy. A.B., 2025 WL 3187686, at *2. He received limited medical
treatment, including treatment at a local emergency room, an MRI, visits to a neurologist, an
occipital nerve block, prescription medications, and chiropractic care. Id. at *10. He did not
experience ongoing facial weakness; there was no evidence that his eye muscles had been
adversely affected, he did not experience ongoing issues drinking, swallowing, or eating, and he
was noted to have a complete recovery of his facial nerve movements within four years. Id. The
petitioner in A.B. asserted issues with hearing and an uneven smile, but those deficits were not
supported by the medical records. Id. When compared to Mr. Sturdevant, the petitioner in A.B.
was noted to have a less severe physical injury. Id. at 13.
However, the petitioner in A.B. also suffered emotional distress, which led to psychiatric
care for approximately one year, a diagnosis of PTSD, and prescriptions for anxiety and
depression. A.B., 2025 WL 3187686, at *10. After this period, he returned to his psychiatrist
but described other stressors in his life unrelated to his Bell’s palsy that were causing emotional
distress, including marital problems. Id. at *10-11. Additionally, despite his contentions, he did
not lose his employment due to his Bell’s palsy. Id. at *13.
Petitioner here, like the petitioner in A.B., underwent specialized treatment, though the
petitioner in A.B. had a full physical recovery unlike Petitioner here. The petitioner in A.B.
suffered emotional distress and sought treatments and required medication for said distress. Both
Petitioner and the petitioner in A.B. had marital issues, though here Petitioner asserts her marital
issues are due to her injury.
When comparing this case to Sturdevant and A.B., the undersigned finds significant
similarities. All three petitioners were similar in age at the time of injury. Like Mr. Sturdevant,
Petitioner continues to have physical facial deficits and suffered for over eight years. And like
the petitioner in A.B., Petitioner attained specialized care and treatment and suffered emotional
distress, though she did not obtain medical care related to this distress. All three petitioners had
concerns regarding employment, but a lack of objective evidence that their employment was
adversely affected by their injury.
However, there are also differences in Petitioner’s case when compared to Sturdevant and
A.B. Petitioner has objectively received more specialized care and treatment. She has worse
14 This damages decision was made public after the parties completed their briefing on pain and
suffering, and therefore, the parties did not discuss this case in their briefs.
16

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 17 of 21
physical deficits. Petitioner cited to Fu et al. to support that she has undergone more emotional
distress because she is female.
The undersigned has considered the numbers proposed by both parties, however, she does
not agree that the amount suggested by either party is appropriate.
Considering the record as a whole, the undersigned finds that $180,000.00 represents a
fair, reasonable, and appropriate amount of compensation for Petitioner’s pain and suffering and
emotional distress. The undersigned recognizes Petitioner’s duration and severity of suffering.
Petitioner has required specialized treatment for her injury. She was prescribed pain medication
and steroids. She underwent an MRI, four years of Botox (three rounds per year), a total of 21
PT visits, and a speech evaluation. She also received medical treatment from her PCP,
neurologists, optometrist and ophthalmologist, ENTs, dentists, and a plastic surgeon. She has
already suffered for more than eight years. Although Petitioner described various issues that are
not fully supported by the medical records, the undersigned finds Petitioner suffered a
moderately severe injury. Thus, the undersigned finds Petitioner’s overall course to be
significantly worse than those experienced by the Sturdevant and A.B. petitioners, although
Petitioner here has similarities in clinical course with both the Sturdevant and A.B. petitioners.
The award of $180,000.00 acknowledges that Petitioner experienced the difficulties described
and acknowledges the effects it has on Petitioner’s ability to enjoy certain activities and
emotional distress. The undersigned does not find a future pain and suffering award appropriate
here because her condition is stable, and there is no medical evidence that she will have future
pain and suffering. Future treatment needs are covered by the life care plan for Petitioner.
IV. DISPUTED LIFE CARE PLAN ITEMS
A. Legal Framework
As previously mentioned, Petitioner “bear[s] the burden of proof with respect to each
element of compensation requested.” Brewer, 1996 WL 147722, at *22; see also § 11(e)
(“[P]etitioner shall submit . . . assessments, evaluations, and prognoses and such other records
and documents as are reasonably necessary for the determination of the amount of compensation
to be paid to, or on behalf of, the person who suffered such injury . . . .”).
Compensation awarded pursuant to the Vaccine Act shall also include “[a]ctual
unreimbursable expenses incurred from the date of the judgment awarding such expenses and
reasonable projected unreimbursable expenses” that
(i) result from the vaccine-related injury for which the [P]etitioner seeks
compensation,
(ii) have been or will be incurred by or on behalf of the person who suffered such
injury, and
(iii) (I) have been or will be for diagnosis and medical or other remedial care
determined to be reasonably necessary, or
(II) have been or will be for rehabilitation, developmental evaluation, special
education, vocational training and placement, case management services,
17

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 18 of 21
counseling, emotional or behavioral therapy, residential and custodial care and
service expenses, special equipment, related travel expenses, and facilities
determined to be reasonably necessary.
§ 15(a)(1)(A).
“[R]easonable projected unreimbursable expenses” must be shown to be “reasonably
necessary.” § 15(a)(1)(A)(iii). “Special masters have characterized this phrase as a ‘vague
instruction’ and a standard for which there is ‘no precise’ definition.” Lerwick ex rel. B.L. v.
Sec’y of Health & Hum. Servs., No. 06-847V, 2014 WL 3720309, at *5 (Fed. Cl. Spec. Mstr.
June 30, 2014); see also I.D., 2013 WL 2448125, at *6 (defining “reasonably necessary” to mean
“that which is required to meet the basic needs of the injured person . . . but short of that which
may be required to optimize the injured person’s quality of life” (quoting Scheinfield v. Sec’y of
Health & Human Servs., No. 90-212V, 1991 WL 94360, at *2 (Cl. Ct. Spec. Mstr. May 20,
1991))); Bedell v. Sec’y of Health & Hum. Servs., No. 90-765V, 1992 WL 266285 (Cl. Ct. Spec.
Mstr. Sept. 18, 1992) (defining “reasonably necessary” to mean “more than merely barely
adequate, but less than the most optimal imaginable”); Alonzo v. Sec’y of Health & Hum. Servs.,
No. 18-1157V, 2023 WL 5846682, at *11 (Fed Cl. Spec. Mstr. Aug. 14, 2023).
B. Contentions and Analysis
The parties confirmed the life care plan items in dispute. See Resp. Ex. K; Joint Status
Rept., filed Mar. 25, 2026. The undersigned will address each in turn.
1. Vision Care & Eye Doctor Co-Pay
Petitioner requests the deductible for her yearly eye examination ($10.00), while
Respondent argues this cost is a routine expense and should not be awarded. Resp. Ex. K at 4,
10. Petitioner’s life care planner noted Petitioner reported “increased difficulty seeing due to her
eye dryness, related blurriness, and irritation and uses magnifying classes to read small print.”
Pet. Ex. 109 at 15, 21. The life care planner added that “[Petitioner’s] eyes and vision have been
impacted by Bell’s Palsy, and she is followed by her usual eye doctor/optometrist who has made
recommendations and prescribed care.” Id. at 19. Further, her treating provider (Dr. Esquivel)
“indicated that [Petitioner] has no increased optometry needs beyond her usual follow-up
currently.” Id.
The undersigned made a preliminary finding awarding the co-pay for one eye exam per
year ($10.00 per year). Order dated May 7, 2025, at 1 (ECF No. 137). However, upon review of
the records, the undersigned finds Dr. Esquivel’s statement shows this is a routine expense that
Petitioner would have incurred irrespective of her vaccine injury given her need for corrective
lenses prior to vaccination and lack of “optometry needs beyond her usual follow-up.” Pet. Ex.
109 at 19. Thus, this expense will not be awarded.
18

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 19 of 21
2. NeutraSal Oral Rinse
The parties agree Petitioner is entitled to coverage of NeutraSal, but do not agree with the
price for each carton and the amount of cartons per year. Resp. Ex. K at 19-20. The life care
planners confirmed Petitioner’s insurance and Medicare Part D will not cover this cost.
Petitioner contends her dentist indicated Petitioner requires NeutraSal daily, and thus,
Petitioner requests $4,817.88 per year to life expectancy for daily usage of NeutraSal Oral Rinse.
Resp. Ex. K at 19 (citing Pet. Ex. 118). In calculating this amount, Petitioner uses the non-
discounted price of $395.99. Id. (citing Pet. Ex. 122).
Respondent recommends coverage of NeutraSal at a discounted price of $349.36 for half
the year, totaling $2,096.16 per year to life expectancy. Resp. Ex. K at 19. “Respondent
disagrees that the evidence, including the treater letter ([Pet. Ex.] 118), supports the need for
daily use of this rinse when other items have been provided in the plan to address dry mouth.”
Id. at 20 (citing Pet. Ex. 118). Respondent recommends six cartons (30 packets in each) “as
other products (mouth spray, lozenges[,] & mouthwash) have been provided in the [life care
plan] to address dry mouth.” Id. at 19.
Petitioner’s dentist emailed Petitioner’s life care planner regarding the need for NeutraSal
Oral Rinse. Pet. Ex. 118. In the email, Petitioner’s dentist recommended the following:
Liz, treatment of [Petitioner’s] dry mouth is critical to her oral health.
Without the use of prescription flouride toothpaste like prevident and oral rinses
such as NeutraSal she will develop rampant cervical caries. This could lead to
early tooth loss and multiple unnecessary dental procedures.
I do recommend ongoing prescription rinses and toothpaste due to the
severity of her dry mouth. [Over the counter] rinses, lozenges are a nice adjunct
but do not replace the need for prescription strength.
Id. at 1. While the email does not indicate that daily use is needed given Petitioner’s complaint
of dry mouth, the undersigned finds it is reasonable that she have daily treatment for this
symptom. Therefore, the undersigned finds Petitioner entitled to NeutraSal daily for her life
expectancy.
With regard to the price of NeutraSal, Petitioner filed documentation from GoodRx
showing the non-discounted price of NeutraSal is $395.99, while the discounted price differs at
each pharmacy in Petitioner’s area, ranging from $331.76 to $367.91. Pet. Ex. 112 at 1-12.
Respondent proposes a price of $349.36 per carton. Resp. Ex. K at 19. The undersigned will use
this price per carton.
Therefore, Petitioner is awarded daily NeutraSal from now to life expectancy at the price
of $349.36 per carton.
19

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 20 of 21
3. Dental Floss
Petitioner requests $44.00 per year from now to life expectancy for dental floss;
Respondent disagrees and contends this is a routine expense. Resp. Ex. K at 22. Petitioner’s life
care planner included dental floss in the life care plan because Petitioner’s providers have
instructed her to floss more often than usual (more than three times per day) to account for her
increased dental health issues from food pocketing and food between her teeth. Pet. Ex. 109 at
12, 15, 20.
The undersigned preliminarily awarded $44.00 per year now to life expectancy for dental
floss. Order dated May 7, 2025, at 2. The undersigned found this item reasonably necessary to
prevent tooth decay due to Petitioner’s condition. Id. The undersigned maintains this finding
and will award $44.00 per year now to life expectancy for dental floss.
4. Tissues
Petitioner requests $77.50 per year from now to life expectancy for tissues, which
Respondent disagrees and contends this is a routine expense. Resp. Ex. K at 22. Petitioner’s life
care planner noted Petitioner “uses multiple tissues each day, to manage drool or food/liquid
spillage, to wipe up after applying drops and ointments to her eyes, to blot nasal discharge, etc.”
Pet. Ex. 109 at 15, 20.
The undersigned preliminarily awarded $77.50 per year now to life expectancy for tissues
as Petitioner provided a particular and specific need for this item in her life care plan report.
Order dated May 7, 2025, at 3. The undersigned will award this expense and maintains this cost
is reasonably necessary. Id. Thus, Petitioner is awarded $77.50 per year now to life expectancy
for tissues.
5. Aquegel Eucalyptus Moisturizer
Petitioner requests $68.50 per year from now to life expectancy for Aquegel eucalyptus
moisturizer. Resp. Ex. K at 22. Respondent contests this cost, arguing it is a routine expense.
Id. Petitioner’s life care planner explained Petitioner uses this moisturizer for her nasal dryness
and to alleviate associated discomfort. Pet. Ex. 109 at 20.
The undersigned preliminarily awarded $68.50 per year now to life expectancy for
Aquegel moisturizer as Petitioner provided a particular and specific need for this item in her life
care plan report. Order dated May 7, 2025, at 3. The undersigned will award this expense and
maintains this cost is reasonably necessary. Id. Thus, Petitioner is awarded $68.50 per year now
to life expectancy for Aquegel moisturizer.
6. Humidifier
Petitioner requests costs of a humidifier ($90.00 now and then $45.00 per year to life
expectancy); Respondent argues this is a routine expense and should not be awarded. Resp. Ex.
20

Case 1:18-vv-01782-UNJ Document 165 Filed 04/28/26 Page 21 of 21
K at 28. Petitioner’s life care planner noted “[s]he uses a humidifier in her bedroom to help with
nasal, mouth, and eye dryness.” Pet. Ex. 109 at 16.
The undersigned preliminarily awarded $90.00 now and every three years to life
expectancy for a humidifier. Order dated May 7, 2025, at 3. The undersigned will award this
expense, finding this cost is reasonably necessary. Thus, Petitioner is awarded $90.00 now and
every three years to life expectancy for a humidifier.
V. CONCLUSION
In determining an award in this case, the undersigned does not rely on a single decision
or case. Rather, the undersigned has reviewed the particular facts and circumstances in this case,
giving due consideration to the circumstances and damages in other cases cited by the parties and
other relevant cases, as well as her knowledge and experience adjudicating similar cases.
In light of the above analysis, and in consideration of the record as a whole, the
undersigned finds that Petitioner should be awarded (1) $180,000.00 for pain and suffering and
(2) and an amount sufficient to fund the life care plan items agreed upon by the parties as well as
those awarded herein.
The parties are to file a joint status report within 30 days, by Monday, April 27, 2026,
(1) providing a complete and final life care plan which takes into consideration the items
adjudicated herein, (2) providing a joint status report confirming the amount of damages the
parties previously agreed upon for lost wages and out-of-pocket expenses, and (3) confirming
that all items of damages have now been resolved and that no issues remain outstanding.
In the absence of a motion for review filed pursuant to RCFC Appendix B, the Clerk of
the Court SHALL ENTER JUDGMENT herewith.15
IT IS SO ORDERED.
s/Nora Beth Dorsey
Nora Beth Dorsey
Special Master
15 Pursuant to Vaccine Rule 11(a), entry of judgment is expedited by the parties’ joint filing of
notice renouncing the right to seek review.
21