VICP Registry Case Source Bundle
Canonical URL: https://vicp-registry.org/case/USCOURTS-cofc-1_17-vv-01915
Package ID: USCOURTS-cofc-1_17-vv-01915
Petitioner: Angela Apuzzo
Filed: 2017-12-08
Decided: 2025-04-02
Vaccine: influenza
Vaccination date: 2015-09-17
Condition: chronic inflammatory demyelinating polyneuropathy (CIDP) and Sjögren's syndrome
Outcome: denied
Award amount USD: 

AI-assisted case summary:
Angela Apuzzo received an influenza vaccine on September 17, 2015. She subsequently developed symptoms of numbness and tingling, initially diagnosed as Guillain-Barré Syndrome (GBS) and peripheral demyelinating neuropathy. Over time, her diagnosis evolved, with some physicians suspecting CIDP and others Sjögren's syndrome. Petitioner's experts, a neurologist and a rheumatologist, suggested a 'mosaic of autoimmunity' possibly triggered by the vaccine, with the neurologist noting a change in diagnosis to small fiber neuropathy. Respondent's experts, including neurologists and rheumatologists, disputed the CIDP diagnosis, arguing that the petitioner's symptoms were inconsistent with CIDP and that her condition, likely Sjögren's syndrome, may have predated the vaccination. The Special Master denied compensation, concluding that the preponderance of the evidence indicated Ms. Apuzzo suffered from Sjögren's syndrome, not CIDP, and that causation by the vaccine was not established. The Court of Federal Claims affirmed this decision, finding that the Special Master appropriately evaluated the competing expert opinions and that the petitioner failed to meet her burden of proof for a vaccine-related injury.

Theory of causation field:
Influenza vaccine on September 17, 2015, adult exact age not stated, alleged to cause CIDP and/or Sjogren's syndrome/small fiber neuropathy with symptoms about 18 days later. DENIED. Petitioner Angela Apuzzo relied on neurologic and rheumatologic experts and a mosaic-of-autoimmunity theory. Respondent's experts disputed CIDP diagnosis and attributed symptoms to Sjogren's or non-vaccine causes, possibly predating vaccination. Special Master Horner dismissed the petition September 20, 2024; Senior Judge Loren A. Smith denied review April 2, 2025.

Public staged source text:

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DOCUMENT 1: USCOURTS-cofc-1_17-vv-01915-1
Date issued/filed: 2024-10-18
Pages: 37
Docket text: PUBLIC DECISION (Originally filed: 9/20/2024) regarding 158 DECISION of Special Master. Signed by Special Master Daniel T. Horner. (ksb) Service on parties made.
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Case 1:17-vv-01915-LAS Document 159 Filed 10/18/24 Page 1 of 37
In the United States Court of Federal Claims
OFFICE OF SPECIAL MASTERS
No. 17-1915V
Filed: September 20, 2024
Special Master Horner
ANGELA APUZZO,
Petitioner,
v.
SECRETARY OF HEALTH AND
HUMAN SERVICES,
Respondent.
Ronald Craig Homer, Conway, Homer, P.C., Boston, MA, for petitioner.
Debra A. Filteau Begley, U.S. Department of Justice, Washington, DC, for respondent.
DECISION1
On December 8, 2017, petitioner filed a petition under the National Childhood
Vaccine Injury Act, 42 U.S.C. § 300aa-10, et seq. (2012),2 alleging that she suffered
chronic inflammatory demyelinating polyneuropathy (“CIDP”) as a result of an influenza
(“flu”) vaccine administered on September 17, 2015. (ECF No. 1.) For the reasons set
forth below, I conclude that petitioner is not entitled to an award of compensation.
I. Applicable Statutory Scheme
Under the National Vaccine Injury Compensation Program, compensation
awards are made to individuals who have suffered injuries after receiving vaccines. In
general, to gain an award, a petitioner must make a number of factual demonstrations,
including showing that an individual received a vaccination covered by the statute;
1 Because this document contains a reasoned explanation for the action taken in this case, it must be
made publicly accessible and will be posted 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 document 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, I agree that the identified material fits within this definition, I will redact such material from
public access.
2 All references to “§ 300aa” below refer to the relevant section of the Vaccine Act at 42 U.S.C. § 300aa-
10-34.
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received it in the United States; suffered a serious, long-standing injury; and has
received no previous award or settlement on account of the injury. Finally – and the key
question in most cases under the Program – the petitioner must also establish a causal
link between the vaccination and the injury.
In some cases, the petitioner may simply demonstrate the occurrence of what
has been called a “Table Injury.” That is, it may be shown that the vaccine recipient
suffered an injury of the type enumerated in the “Vaccine Injury Table,” corresponding to
the vaccination in question, within an applicable time period following the vaccination
also specified in the Table. If so, the Table Injury is presumed to have been caused by
the vaccination unless it is affirmatively shown that the injury was caused by some
factor other than the vaccination. § 300aa-13(a)(1)(A); § 300aa-11(c)(1)(C)(i);
§ 300aa-14(a); § 300aa-13(a)(1)(B). In many cases, however, the vaccine recipient
may have suffered an injury not of the type covered in the Vaccine Injury Table. In such
instances, an alternative means exists to demonstrate entitlement to a Program award.
That is, the petitioner may gain an award by showing that the recipient’s injury was
“caused-in-fact” by the vaccination in question. § 300aa-13(a)(1)(B);
§ 300aa-11(c)(1)(C)(ii). In such a situation, of course, the presumptions available under
the Vaccine Injury Table are inoperative. The burden is on the petitioner to introduce
evidence demonstrating that the vaccination actually caused the injury in question.
Althen v. Sec’y of Health & Human Servs., 418 F.3d 1274, 1278 (Fed. Cir. 2005); Hines
ex rel. Sevier v. Sec’y of Health & Human Servs., 940 F.2d 1518, 1525 (Fed. Cir. 1991).
The showing of “causation-in-fact” must satisfy the “preponderance of the
evidence” standard, the same standard ordinarily used in tort litigation.
§ 300aa-13(a)(1)(A); see also Althen, 418 F.3d at 1279; Hines, 940 F.2d at 1525.
Under that standard, the petitioner must show that it is “more probable than not” that the
vaccination was the cause of the injury. Althen, 418 F.3d at 1279. The petitioner need
not show that the vaccination was the sole cause but must demonstrate that the
vaccination was at least a “substantial factor” in causing the condition, and was a “but
for” cause. Shyface v. Sec’y of Health & Human Servs., 165 F.3d 1344, 1352 (Fed. Cir.
1999). Thus, the petitioner must supply “proof of a logical sequence of cause and effect
showing that the vaccination was the reason for the injury[,]” with the logical sequence
being supported by “reputable medical or scientific explanation, i.e., evidence in the
form of scientific studies or expert medical testimony.” Althen, 418 F.3d at 1278; Grant
v. Sec’y of Health & Human Servs., 956 F.2d 1144, 1148 (Fed. Cir. 1992). Ultimately,
petitioner must satisfy what has come to be known as the Althen test, which requires:
(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 proximate temporal relationship between vaccination and
injury. Id.
A petitioner may not receive a Vaccine Program award based solely on his or her
assertions; rather, the petition must be supported by either medical records or by the
opinion of a competent physician. § 300aa-13(a)(1). Medical records are generally
viewed as particularly trustworthy evidence, because they are created
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contemporaneously with the treatment of the patient. Cucuras v. Sec’y of Health &
Hum. Servs., 993 F.2d 1525, 1528 (Fed. Cir. 1993). However, medical records and/or
statements of a treating physician’s views do not per se bind the special master to adopt
the conclusions of such an individual, even if they must be considered and carefully
evaluated. § 300aa-13(b)(1). A petitioner may also rely upon circumstantial evidence.
Althen, 418 F.3d at 1280. The Althen court noted that a petitioner need not necessarily
supply evidence from medical literature supporting petitioner’s causation contention, so
long as the petitioner supplies the medical opinion of an expert. Id. at 1279-80. While
scientific certainty is not required, that expert’s opinion must be based on “sound and
reliable” medical or scientific explanation. Boatmon v. Sec’y of Health & Human Servs.,
941 F.3d 1351, 1359 (Fed. Cir. 2019).
Cases in the Vaccine Program are assigned to special masters who are
responsible for “conducting all proceedings, including taking such evidence as may be
appropriate, making the requisite findings of fact and conclusions of law, preparing a
decision, and determining the amount of compensation, if any, to be awarded.” Vaccine
Rule 3. Special masters must ensure each party has had a “full and fair opportunity” to
develop the record but are empowered to determine the format for taking evidence
based on the circumstances of each case, including having the discretion to decide
cases without an evidentiary hearing. Vaccine Rule 3(b)(2); Vaccine Rule 8(a); Vaccine
Rule (d). Special masters are not bound by common law or statutory rules of evidence
but must consider all relevant and reliable evidence in keeping with fundamental
fairness to both parties. Vaccine Rule 8(b)(1). The special master is required to
consider “all [] relevant medical and scientific evidence contained in the record,”
including “any diagnosis, conclusion, medical judgment, or autopsy or coroner’s report
which is contained in the record regarding the nature, causation, and aggravation of the
petitioner’s illness, disability, injury, condition, or death,” as well as the “results of any
diagnostic or evaluative test which are contained in the record and the summaries and
conclusions.” § 300aa-13(b)(1)(A). The special master is then required to weigh the
evidence presented, including contemporaneous medical records and testimony. See
Burns v. Sec’y of Health & Human Servs., 3 F.3d 413, 417 (Fed. Cir. 1993).
In this case, petitioner has alleged that the flu vaccine caused CIDP. CIDP is not
listed on the Vaccine Injury Table relative to the flu vaccine. Therefore, petitioner must
satisfy the above-described Althen test for establishing causation-in-fact.
II. Procedural History
This case was initially assigned to another special master. (ECF No. 4.) It was
reassigned to the undersigned on August 29, 2019. (ECF No. 69.)
Petitioner filed her medical records between January of 2017 and January of
2018. (ECF Nos. 11-12, 17, 21, 31, 37, 39, 44, 48; Exs. 1-16, 18-27, 30-41.) She also
filed three affidavits. (ECF Nos. 13, 23; Exs. 17, 28-29.) Initially the parties attempted
informal resolution; however, settlement discussions were halted when respondent
concluded that later filed medical records reflected a change in petitioner’s diagnosis.
(ECF Nos. 33, 43.) Respondent filed his Rule 4 report in February of 2019,
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recommending against compensation. (ECF No. 50.) Respondent argued that
petitioner’s medical records alone were inadequate to meet petitioner’s burden of proof
with respect to any vaccine-caused CIDP, but also contended that petitioner’s more
recent medical records indicated her physicians had begun to conclude her condition
was actually explained by systemic lupus erythematosus (“SLE”) and Sjӧgren’s
syndrome, rather than CIDP. (Id. at 11-12.)
In the summer of 2019, petitioner filed an expert report by neurologist Nizar
Souayah, M.D., along with supporting materials. (ECF Nos. 58-65; Exs. 42-100.) Dr.
Souayah opined that petitioner most likely suffered CIDP and that her condition was
vaccine-caused. (Ex. 42, p. 28.) In December of 2019, petitioner filed additional
medical records marked as Exhibit 101. (ECF No. 71.) Respondent filed responsive
reports by neurologist Brian Callaghan, M.D., and rheumatologist Robert Lightfoot, Jr.,
M.D., in February of 2020. (ECF Nos. 74-75; Exs. A-D.) Dr. Callaghan opined that
petitioner did not have CIDP. (Ex. A, p. 4.) Dr. Lightfoot opined that petitioner’s
presentation is consistent with an incomplete form of Sjӧgren’s syndrome, but that he
could not “unequivocally” state that she does have it. (Ex. C, pp. 5-6.) Thereafter,
petitioner filed additional medical records (Exhibits 102-03) and a report by
rheumatologist Samar Gupta, M.D., as well as a supplemental report by Dr. Souayah,
with supporting materials (Exhibits 104-49). (ECF Nos. 76, 78, 84, 86-89.) Dr. Gupta
opined that petitioner likely had an incomplete form of Sjӧgren’s syndrome and that her
neuropathy, whether CIDP or small fiber neuropathy, was likely related. (Ex. 104, p. 4.)
In his supplemental report, Dr. Souayah responded to Dr. Callaghan and, although he
maintained that petitioner suffered CIDP, he also observed that she had small fiber
neuropathy. (ECF No. 84; Ex. 111.)
In November of 2020, I held a Rule 5 conference. (ECF No. 91.) I expressed
concern that the expert reports to date had effectively been siloed by discipline and,
given that petitioner had not alleged vaccine-caused Sjӧgren’s syndrome, that the
parties’ rheumatology opinions appeared to be mismatched to their respective positions.
I directed the parties to have their experts clarify their opinions, by explaining the case
“holistically and with an interdisciplinary approach,” and directed petitioner to clarify
whether she is alleging vaccine-caused CIDP to the exclusion of Sjӧgren’s syndrome;
vaccine-caused CIDP in the presence of unrelated Sjӧgren’s syndrome; Sjӧgren’s
syndrome with associated, but vaccine-caused, neuropathy; or vaccine-caused
Sjӧgren’s syndrome. (Id.)
In April of 2021, petitioner filed supplemental expert reports responsive to my
Rule 5 order. (ECF No. 95; Exs. 150-51.) Dr. Gupta deferred to Dr. Souayah regarding
the nature of petitioner’s neuropathy, but maintained that petitioner also had incomplete
Sjӧgren’s syndrome and that the “mosaic of autoimmunity” therefore best describes her
overall condition. (Ex. 151.) Dr. Souayah maintained that petitioner initially had CIDP,
but indicated that it may have evolved into small fiber neuropathy. He deferred to Dr.
Gupta regarding the presence of Sjӧgren’s syndrome. He indicated that his opinion
regarding vaccine-caused CIDP and small fiber neuropathy is compatible with Dr.
Gupta’s invocation of the mosaic of autoimmunity. (Ex. 150.) Respondent filed a
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responsive expert report by Dr. Callaghan in December of 2021. (ECF No. 111; Ex. E.)
Dr. Callaghan maintained that petitioner did not suffer CIDP and further opined that
petitioner did not have small fiber neuropathy. (Ex. E.)
Petitioner then filed updated medical records (Exhibits 152-56) between May and
October of 2022, as well as additional affidavits (Exhibits 157-58). (ECF Nos. 117, 124,
126, 134-35.) Respondent requested an opportunity to have Dr. Callaghan submit an
opinion reviewing the updated medical records and also requested the opportunity to
substitute an opinion by rheumatologist Mehrdad Matloubian, M.D., Ph.D., in place of
Dr. Lightfoot. (ECF No. 132.) Although petitioner objected to the substitution of experts
(ECF No. 133), I allowed respondent to complete the requested filings after confirming
that Dr. Lightfoot had become unavailable to respondent as a result of winding down his
practice and participation in the program (ECF No. 137). Respondent filed reports by
Drs. Callaghan and Matloubian in October and November of 2022. (ECF Nos. 139-40;
Exs. F-H.) Dr. Callaghan maintained his view, based on his review of the updated
medical records. (Ex. F.) Dr. Matloubian opined that petitioner had Sjӧgren’s syndrome
unrelated to vaccination and that any neuropathy was attributable to that condition. (Ex.
G, pp. 8-9.) Petitioner then filed further updated medical records (Exhibits 159-60) and
a further report by Dr. Gupta responding to Dr. Matloubian’s report (Exhibit 161). (ECF
Nos. 143, 146.) Dr. Gupta maintained his previously stated opinion. (Ex. 161.)
An entitlement hearing had been set for November of 2023 (ECF No. 131);
however, in June of 2023, the parties filed a joint status report expressing a preference
for proceeding with a ruling on the written record in lieu of any hearing and confirming
that the expert presentations were complete (ECF No. 149). Accordingly, the hearing
was cancelled. (ECF No. 150.) Petitioner filed her motion for a ruling on the record on
September 5, 2023. (ECF No. 152.) Respondent filed his response on October 13,
2023, and petitioner filed a reply on October 30, 2023. (ECF Nos. 154-55.)
This matter is now ripe for resolution as to entitlement. I have concluded that the
parties have had a full and fair opportunity to develop the record and that it is
appropriate to resolve this case without an entitlement hearing. See Kreizenbeck ex rel.
C.J.K. v. Sec’y of Health & Human Servs., 945 F.3d 1362, 1366 (Fed. Cir. 2020) (citing
Simanski v. Sec’y of Health & Human Servs., 671 F.3d 1368, 1385 (Fed. Cir. 2012));
see also Vaccine Rule 8(d); Vaccine Rule 3(b)(2).
III. Factual History
a. As reflected in the medical records
Petitioner received the flu vaccine at issue on September 17, 2015. (Ex. 1, pp. 1-
2.) On October 5, 2015, she was seen in the emergency department with complaints of
numbness and tingling in her hands, feet, and the right side of her face. (Ex. 2, pp. 4-5.)
She indicated that she had experienced a “short viral-like illness” following her flu
vaccination and that her numbness began about four days prior to her emergency
department encounter, around the time she had a blood draw. (Id. at 5.) Upon physical
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exam, she had normal reflexes, muscle tone, strength, and gait. (Id. at 6-7.) Neurologic
exam further confirmed full strength and normal reflexes in the extremities, as well as
normal gait. (Id. at 12-13.) However, she had slightly decreased sensation at the fifth
cranial nerve in a V2 distribution and some sensation changes her hands and feet. (Id.)
Petitioner was felt to have mild peripheral neuropathy. (Id. at 16.) Hypothyroidism was
suspected as a cause; however, an outpatient neurology follow up was recommended
to further investigate the cause of petitioner’s neuropathy. (Id.)
Petitioner followed up first with her primary care provider (Ex. 11, p. 60) and then
with a neurologist, Dr. Bronfin, on October 28, 2015 (Ex. 6, p. 4). Dr. Bronfin reviewed
petitioner’s history prior to her emergency department encounter and then explained:
Patent presents with complain[t] of weakness in her hands. Patient has
difficulties [using] her thumbs. Patient noticed diminished dexterity. Patient
reports having pain in her shoulder blades. Patient continues having
numbness in her feet. She recently developed balance difficulties. Patient
denies weakness. Patient does not feel heat. Patient has difficulties
[walking] and uses a c[ane]. Patient reports slow gait.
(Id.) On physical exam, petitioner’s reflexes were absent at the ankle, normal at the
knee, and reduced in the upper extremities. (Id. at 6.) Her plantar reflexes (Babinski
sign) were normal. (Id.) Her gait was ataxic. (Id.) Petitioner underwent NCS/EMG,
which showed “neurophysiologic evidence for acute moderate predominantly motor
demyelinating peripheral polyneuropathy.” (Id. at 1.) Dr. Bronfin diagnosed Guillain-
Barré Syndrome (“GBS”) and peripheral demyelinating neuropathy. (Id. at 6-7.)
Petitioner returned to the emergency department for treatment of her GBS the
same day. (Ex. 2, p. 91.) Petitioner was transferred to inpatient neurology for
observation. (Id. at 99-100.) At the hospital, petitioner’s EMG was characterized as
“nonspecific” and so additional work up was pursued. (Id. at 91.) A lumbar puncture
was attempted to confirm GBS, but was unsuccessful. During the hospitalization,
petitioner’s blood results were significant for positive antinuclear antibodies (“ANA”) and
elevated anti-Sjӧgren’s syndrome-related antigen A antibodies (“SSA”) (also called anti-
“Ro” antibodies). (Id. at 92.) Therefore, petitioner had a consult to address “[p]ossible
[Sjӧgren’s] syndrome in the setting of neuropathy.” (Id. at 132.) Petitioner reported a
history of arthritis in her PIPs3 and MCPs,4 as well as morning stiffness and intermittent
swelling of these joints. Petitioner reported relief with prednisone, which she was taking
3 Proximal interphalangeal (“PIP”) joints are the interphalangeal joints located proximally on any digit.
Proximal interphalangeal joint, DORLAND’S MEDICAL DICTIONARY ONLINE,
https://www.dorlandsonline.com/dorland/definition?id=83592 (last visited Sept. 4, 2024).
4 Metacarpophalangeal (“MCP”) joints, or “the knuckles,” are the articulations between the metacarpus
and the phalanges. Metacarpophalangeal (MCP), STEDMAN’S MEDICAL DICTIONARY (28th ed., 2006).
6

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for asthma. (Id.) Given her history of arthritis5 and positive SSA, as well as the fact that
GBS was not definitively diagnosed, rheumatology considered Sjӧgren’s syndrome as a
possible explanation for petitioner’s peripheral neuropathy and recommended
continuing to treat for GBS while monitoring for Sjӧgren’s syndrome. (Id. at 135.)
During hospitalization, petitioner was treated with four rounds of plasmapheresis, which
petitioner reported had made her feel better, though she complained of side effects. (Id.
at 91, 94, 163-64.) However, rheumatology noted that improvement with
plasmapheresis does not necessarily support the GBS diagnosis. (Id. at 136.) Thus, it
was felt that petitioner should be further evaluated by Dr. Bronfin regarding her correct
diagnosis because she “never lost reflexes as is more typical in GBS.” (Id. at 94.)
Outpatient rheumatology follow up to evaluate for Sjӧgren’s syndrome was also
recommended. (Id. at 136.) Petitioner was discharged on November 3, 2015, with
diagnoses of GBS and peripheral demyelinating neuropathy. (Id. at 91.)
Petitioner returned to Dr. Bronfin on November 17, 2015. (Ex. 6, p. 10.)
Petitioner reported that she felt stronger and with improved balance, but continued to
complain of numbness, tingling, and tremor. She reported being unable to walk for long
distances, requiring the use of a wheelchair at times. (Id. at 11.) Dr. Bronfin maintained
his diagnoses of GBS and peripheral demyelinating neuropathy, but also added
Sjӧgren’s syndrome to his assessment. (Id. at 14.) Dr. Bronfin recommended IVIG
infusion (Gammunex 200 gm), which petitioner underwent beginning December 1,
2015. (Id.; Ex. 20, pp. 47-58.) Petitioner returned to Dr. Bronfin on December 14, 2015,
and January 5, 2016, and reported continued improvement with physical therapy and
IVIG treatment, though she had some side effects from the IVIG. (Ex. 6, pp. 16, 21; see
also Ex. 12, pp. 27-44 (physical therapy records).) By January 5, 2016, she reported
being able to ambulate without assistance. (Ex. 6, p. 21.)
On January 19, 2016, petitioner had an initial evaluation with a rheumatologist,
Dr. Lee. (Ex. 15, p. 1.) In addition to her positive ANA and SSA and suspected GBS,
petitioner’s history included osteoarthritis affecting her knees and hips and a prior left-
side carpal tunnel release. (Id.) However, it was noted that petitioner did not have any
symptoms of systemic lupus erythematosus (“SLE”). (Id.) Petitioner was assessed as
“ANA positive” and it was further noted that she was “Ro+.” (Id. at 5.) Dr. Lee noted
that Sjӧgren syndrome can present with peripheral neuropathy in the absence of the
more classic sicca symptoms6 of Sjӧgren’s syndrome; however, given petitioner’s
response to treatment for GBS, he recommended deferring any further, more invasive,
5 Pertinent to the expert discussion that follows, petitioner argues, however, that bloodwork of January 31,
2012, confirmed that she was negative for antinuclear antibodies and smooth muscle antibodies prior to
the vaccination at issue. (ECF No. 152, p. 6 (citing Ex. 21, p. 21).)
6 Sicca syndrome is characterized as keratoconjunctivitis (i.e. dryness and inflammation of eye) and
xerostomia (i.e. dryness of the mouth) without connective tissue disease. Sicca syndrome, DORLAND’S
MEDICAL DICTIONARY ONLINE, https://www.dorlandsonline.com/dorland/definition?id=111399 (last visited
Sept. 4, 2024); Keratoconjunctivitis, DORLAND’S MEDICAL DICTIONARY ONLINE,
https://www.dorlandsonline.com/dorland/definition?id=26840 (last visited Sept. 4, 2024); Xerostomia,
DORLAND’S MEDICAL DICTIONARY ONLINE, https://www.dorlandsonline.com/dorland/definition?id=53881
(last visited Sept. 4, 2024).
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workup, which would include lip/muscle/nerve biopsy. (Id.) Petitioner was to follow up
for a biopsy if she experienced any recrudescence or flare of her condition. (Id.)
Petitioner then returned to Dr. Bronfin on February 1, 2016. (Ex. 6, p. 26.) She
felt her weakness was increasing and she was experiencing acute shortness of breath.
(Id.) Dr. Bronfin felt her neurologic exam was stable, but that an emergency department
evaluation for her shortness of breath was necessary. (Id.) He also recommended that
petitioner resume IVIG for her acute demyelinating neuropathy. (Id.) Petitioner was
then admitted for an overnight stay at the hospital. The history explains that, following
her IVIG treatment the prior December, petitioner had only residual numbness in her
hands and feet. (Ex. 3, p. 89.) She returned to care due to fatigue, shortness of breath,
and low endurance. She also complained of chest tightness radiating to her neck. (Id.)
However, her neurologic exam confirmed that she had intact reflexes and was not weak
in her extremities. (Id.) It was noted that “[h]er neuro exam is currently normal in terms
of not being Guillain-Barre,” given that she had residual neuropathy but no acute muscle
weakness with reflexes present. (Id. at 90.) Petitioner was felt to be clinically stable
neurologically, and her shortness of breath and fatigue were believed to be unlikely
related to her neurologic condition. A cardiology and pulmonary consultation was
recommended, as well as a second EMG, to assess for CIDP. (Id.) Petitioner returned
to Dr. Bronfin on March 8, 2016, complaining of extremity weakness, poor balance, and
shortness of breath, noting that her condition “is not improving.” (Ex. 6, p. 31.) Dr.
Bronfin recommended further IVIG and his diagnostic impression, including Sjogren’s
syndrome, GBS, and peripheral demyelinating neuropathy, did not change. (Id. at 31,
34.) Petitioner subsequently had IVIG treatment on March 12 and 15, 2025. (Ex. 20,
pp. 94, 102.)
Petitioner sought evaluation by a neuromuscular specialist, Dr. Busono, on
March 21, 2016. (Ex. 7, p. 5.) It was noted that her treating neurologists now disagreed
as to whether she had GBS or CIDP. (Id.) As with prior exams, petitioner had
decreased sensation in her feet, though her upper limbs were normal. (Id. at 7.) She
had normal strength in all extremities and her reflexes were normal. (Id.) Dr. Busono
assessed CIDP and suggested that autonomic dysfunction, as can be seen in CIDP,
might explain petitioner’s shortness of breath. (Id.) He recommended a repeat EMG
and NCS. (Id.) Petitioner returned to Dr. Busono on April 12, 2016, for
electrodiagnostic testing to evaluate for CIDP. (Id. at 9-10.) The EMG and NCS results
were normal, and the study showed no evidence of a generalized polyneuropathy. (Id.
at 10.) Petitioner reported that her energy and endurance improved with IVIG, but her
balance remained poor and she was having memory and concentration issues. (Id. at
3.) Despite the negative electrodiagnostic test, Dr. Busono maintained his CIDP
diagnosis and recommended continued IVIG treatment, as well as neuropsychological
testing. (Id. at 4.) Petitioner followed up again with Dr. Busono in early June of 2016.
(Id. at 1-2.) She reported that she was not improving with IVIG and had additionally
developed allodynia. (Id. at 1.) Accordingly, Dr. Busono noted that he was “beginning
to doubt the diagnosis of CIDP” and referred petitioner for a second opinion by
neuromuscular specialist, Dr. Brannagan. (Id. at 2.) IVIG was discontinued. (Id.)
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Petitioner then began consulting neurologist, Dr. Kapur, in August of 2016. (Ex.
8, pp. 8-13.) Dr. Kapur felt petitioner’s symptoms and examination were consistent with
CIDP. (Id. at 13.) He recommended continuing IVIG and physical therapy, prescribed
gabapentin, and ordered bloodwork. (Id.) Petitioner was to follow up after he obtained
her EMG records.7 (Id.) Petitioner returned to Dr. Kapur on October 4, 2016. (Id. at 1.)
Comparing petitioner’s first and second EMG/NCS studies, Dr. Kapur was concerned
the second study could have resulted from a technical error; however, he also noted
that petitioner’s September 12, 2016 bloodwork also continued to show positive Anti-
SSA. He concluded that petitioner’s symptoms and neurologic exam could be
consistent with either CIDP or small fiber neuropathy related to Sjӧgren’s syndrome.
(Id. at 6.) He recommended continuing petitioner’s treatment plan and following up in a
month to consider whether to repeat the EMG/NCS. (Id. at 6-7.) He added Sjӧgren’s-
related small fiber neuropathy to petitioner’s problem list. (Id. at 7.)
On February 3, 2017, petitioner had an evaluation with another neurologist, Dr.
Vukic. (Ex. 5, pp. 9-12.) Petitioner presented (in a wheelchair) with a chief complaint of
CIDP and described having persistent waxing and waning weakness and numbness
accompanied by overriding fatigue and exertion-related shortness of breath. (Id.)
Petitioner also reported short-term memory problems. (Id.) Physical exam showed
unsteady gait, near normal strength, and absent Achilles reflexes. (Id. at 11.) Dr. Vukic
felt petitioner’s presentation was consistent with CIDP, but ordered further work up
including additional lab work, an MRI of the brain and EEG, and possibly a lumbar
puncture. (Id. at 12.) Petitioner underwent MRI of the brain on February 4, 2017. (Id.
at 14-15.) There was no acute abnormality, but petitioner had patchy foci of T2
prolongation, potentially consistent with either minimal chronic microangiopathic
changes or chronic demyelination. (Id. at 15.) Two days later, an EEG was normal.
(Id. at 16.) Petitioner also underwent a third EMG/NCS study on February 13, 2017.
(Id. at 19.) EMG showed “mild right median mononeuropathy at the wrist consistent
with a clinical diagnosis of carpal tunnel syndrome with a superimposed evidence of
absent F response minimal latencies in the left peroneal nerve.” (Id. at 1, 19.)
Petitioner then had a lumbar puncture on February 28, 2017. (Id. at 17-18.) The results
were normal. (Ex. 4, p. 143.) Dr. Vukic felt the lumbar puncture results were “limited”
and may need to be repeated. He felt the unremarkable EMG was likely attributed to
petitioner’s response to treatment. (Ex. 5, p. 4.) The diagnosis of CIDP was
maintained. (Id.)
On August 22, 2017, petitioner saw another neurologist, Dr. Ma. (Ex. 16, pp.
254-58.) After reviewing petitioner’s history, Dr. Ma felt that petitioner was experiencing
gait dysfunction due to sensory ataxia and dysesthesias from neuropathic pain, both of
which would be related to CIDP. However, “it is also quite likely that patient has a
superimposed predominantly sensory metabolic axonal polyneuropathy, possibly in
7 Of note, the history documented by Dr. Kapur indicates that petitioner did not bring her recent
NCS/EMG results with her, but she reported that they were consistent with CIDP. (Ex. 8, p. 8.) However,
although Dr. Busono maintained the CIDP diagnosis following the electrodiagnostic testing, he interpreted
the study results as normal. (Ex. 7, p. 10.)
9

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association with Sjogren’s syndrome and/or hypothyroidism, which is likely also
contributing to her neuropathy-related issues.” (Id. at 258.)
About a month later, petitioner was admitted to the hospital from September 22
to 25, 2017, for worsening weakness, fatigue, and shortness of breath. (Ex. 16, p. 26.)
She was admitted again from October 2 to 8, 2017. (Ex. 4, p. 196.) The neurology
impression included both CIDP exacerbation and Sjӧgren’s syndrome.8 (Id. at 210.) In
a follow up, petitioner returned to Dr. Vukic, who felt petitioner had improved after
treatment with plasmapheresis during her hospitalization. Petitioner was to resume
IVIG and follow up in six weeks. (Ex. 30, pp. 5-8.) A month later, petitioner reported to
Dr. Vukic that her leg numbness and facial dysesthesias was worsening despite her
ongoing IVIG, though her overall strength was improving. (Id. at 9.) She wanted to stop
treatment and consider alternatives, such as Imuran or CellCept. (Id.) Dr. Vukic
stopped petitioner’s IVIG, but required a repeat EMG and lumbar puncture before
considering whether to start Imuran. (Id. at 12.) As of January 8, 2018, petitioner
reported worsening lower extremity pain and profound fatigue. (Id. at 16.) She
requested an additional course of in-patient plasmapheresis and proposed having a
lumbar puncture at that time. She noted that she intended to see Dr. Brannagan (as
previously recommended by Dr. Busono) in April 2018 for a second opinion as to
diagnosis and future treatment. (Id.) Dr. Vukic agreed with that plan and noted that he
had concerns regarding petitioner’s differential diagnosis. (Id. at 19.) Petitioner was
then admitted for treatment from January 9 to 16, 2018. (Ex. 37, p. 24.) Petitioner felt
her pain and strength improved after plasmapheresis and petitioner ultimately declined
to complete the lumbar puncture. (Id.) It was recommended that petitioner seek an
outpatient rheumatology evaluation for her Sjӧgren’s syndrome. (Id. at 165.) Dr. Vukic
agreed to continue plasmapheresis treatments pending petitioner’s second opinion from
Dr. Brannagan. (Ex. 30, p. 24.)
Petitioner presented to Dr. Brannagan on February 14, 2018, for an EMG/NCS
study. (Ex. 24, pp. 10-11.) Dr. Brannagan noted petitioner had been treated with IVIG
for six months with minimal improvement, but that she had dramatic improvement with
plasmapheresis. (Id. at 10.) Upon presentation, she had some imbalance and
numbness on the right side, but full strength in all extremities and normal reflexes with
the exception of reduced Achilles reflex. She had decreased vibration in her toes and
decreased sensation to light touch on the right side of her body. (Id.) Dr. Brannagan’s
NCS/EMG study found evidence of mild right median mononeuropathy consistent with
carpal tunnel syndrome and borderline findings suggestive of a left phrenic neuropathy.9
However, there was no evidence of large fiber polyneuropathy, demyelination, or
cervical or lumbosacral radiculopathy. (Id. at 11.) Dr. Brannagan concluded during an
8 During this hospitalization, petitioner underwent brain and spinal MRIs. (Ex. 4, pp. 345-47.) The spinal
MRI showed some degenerative changes of the cervical spine without compression, but no indication of
demyelination. The brain MRI showed no significant change since her prior MRI.
9 The phrenic nerve is a motor nerve of the diaphragm, but it also sends sensory fibers to the mediastinal
parietal pleura, the pericardium, the diaphragmatic pleura and peritoneum, and branches that
communicate with branches from the celiac plexus. Phrenic nerve, STEDMAN’S MEDICAL DICTIONARY (28th
ed., 2006).
10

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April 13, 2018 follow up that neither petitioner’s nerve conduction study nor her
neurological examination were consistent with CIDP or any large fiber neuropathy. (Ex.
41, pp. 3-4.) However, he noted that her Sjӧgren’s syndrome could cause small fiber
neuropathy and recommended a skin biopsy and a follow up with rheumatology. Dr.
Brannagan indicated that there are reports in the literature of plasmapheresis being
used to treat Sjӧgren’s syndrome. (Id.) Dr. Vukic then noted that Dr. Brannagan does
not believe petitioner has CIDP and therefore concluded that “[t]he cause of her
symptoms remains elusive.” (Ex. 30, pp. 35, 39.) He withheld further recommendation
pending her formal rheumatologic evaluation. (Id. at 39.) Dr. Vukic agreed that
petitioner’s response to plasmapheresis could point to a rheumatologic process. (Id. at
45.)
Petitioner had a skin biopsy on April 30, 2018. (Ex. 30, p. 40.) Samples were
taken from the lateral thigh and distal leg, both on the left side, and were sent to
Therapath for analysis. (Id.) Both samples showed significantly reduced nerve fiber
density consistent with small fiber neuropathy. (Ex. 154, p. 63.) She was then
evaluated by rheumatologist, Dr. Kepecs, on August 2, 2018. (Ex. 36, pp. 2-4.) Dr.
Kepecs felt there is “fair evidence” for SLE and/or Sjӧgren’s syndrome, given
petitioner’s positive SSA and peripheral neuropathy without a metabolic explanation.
(Id. at 3.) It was noted that petitioner had a family history of SLE (her mother). (Id. at
2.) Her history was not suggestive of Churg-Strauss syndrome.10 He felt that
“[w]hatever the name for the syndrome it is certainly autoimmune.” Accordingly, he felt
it may respond to immunosuppressive treatment such as CellCept or Imuran, though he
did not believe steroids were justified. (Id. at 3.) Dr. Kepecs ordered a trial of CellCept
and directed petitioner to follow up in 5-6 weeks, noting that he may repeat petitioner’s
serology and possibly include a myositis panel. (Id. at 3-4.) Petitioner returned about a
month later and reported that she was tolerating CellCept. (Id. at 5-6.) Petitioner
reported feeling somewhat better, but Dr. Kepecs felt it was too soon for real effect.
(Id.) Dr. Kepecs now felt that a SLE/Sjӧgren’s syndrome overlap with peripheral
neuropathy was “probable.” (Id. at 6.) He continued CellCept and ordered bloodwork.
(Id.)
On October 15, 2018, petitioner was again admitted for treatment when she
presented to the hospital with a “few week history” of progressive generalized
weakness, difficulty swallowing, dyspenea on exertion, and constipation. (Ex. 39, p.
12.) Neurology reviewed petitioner’s history, including her prior presentation for
suspected CIDP (noting diagnosis is “not categorically” made) and subsequent
diagnosis of confirmed small fiber neuropathy and an autoimmune disease (“uncertain if
it’s purely Sjogren’s or Lupus”). (Id. at 28-29.) Petitioner was treated as having a “CIDP
exacerbation” and was treated with five days of plasmapheresis. (Id. at 32.) It was
questioned whether petitioner’s recent decline was related to her CellCept or
coincidental. (Id.) In follow up, Dr. Vukic maintained that petitioner’s condition is
“elusive” but likely a rheumatologic condition. (Ex. 154, p. 52.) He indicated he would
10 Churg-Strauss syndrome is a type of small vessel vasculitis with prominent lung involvement. Churg-
Strauss syndrome, DORLAND’S MEDICAL DICTIONARY ONLINE,
https://www.dorlandsonline.com/dorland/definition?id=110417 (last visited Sept. 13, 2024).
11

Case 1:17-vv-01915-LAS Document 159 Filed 10/18/24 Page 12 of 37
discuss the case further with Dr. Kepecs. (Id.) Petitioner subsequently switched from
CellCept to Plaquenil, which she felt was helping. (Id. at 42.) As of December 11,
2018, Dr. Vukic noted that petitioner’s symptoms continued to flare. (Id. at 42, 46.) He
concluded that her condition appears to be a mixture of neurologic and rheumatologic
conditions and remarked that “I suspect they are direct result of her prior immunization.”
(Id. at 46.)
After relocating to Florida, petitioner presented to the emergency department with
another flare of her condition on June 30, 2019. (Ex. 101, pp. 12-17.) Petitioner’s chief
complaint was increasing pain and weakness in her left lower extremity. (Id. at 26.)
The pain also spread to include her hands and she also had one week of dysphagia,
urinary retention, and constipation. She reported that she had previously been
receiving plasmapheresis every six months, but that she had not had a treatment since
October of 2018 because she was doing well. She reported chronic weakness as well
as pain from small fiber neuropathy. She was scheduled to see a new neurologist in
Florida beginning in October. (Id.) Upon neurologic exam, Dr. Sonbol indicated that
petitioner’s exam was “not necessarily consistent with CIDP and there are some non-
physiologic exam findings.” (Id. at 29.) Petitioner was admitted for workup, which was
to include MRIs that were ultimately unremarkable. (Id. at 19, 29.) Petitioner was
discharged on July 2, 2019. (Id. at 18.) Although her admission diagnosis was CIDP,
her discharge diagnosis was neuropathy. During hospitalization petitioner was started
on Vimpat,11 which reportedly helped. (Id.) Whereas petitioner reported being
wheelchair bound when initially examined, she was able to stand and walk unassisted
at her discharge exam. (Id. at 19, 28.)
Petitioner had a follow up with neurologist, Dr. Suresh, on July 31, 2019. (Ex.
102, p. 7.) At that time, she reported having “severe” loss of function and pain, along
with bowel and bladder issues and episodes of flushing and sweating in connection with
pain flares. (Id.) On exam, petitioner had full strength and intact reflexes, though her
ankle reflexes were reduced. (Id. at 12.) Dr. Suresh assessed petitioner as having
small fiber neuropathy, suspected to be autoimmune and confirmed by biopsy, with an
autonomic component. (Id.) He further opined that there was “no clear and convincing
evidence of CIDP given lack of response, electrodiagnostic findings at Columbia,
marginally elevated CSF protein to 60, and reflexes that are preserved in the legs.” (Id.)
He felt that petitioner had good prior responses to both plasmapheresis and IVIG and
recommended a trial of IVIG.12 Given that petitioner was having a flare of uncontrolled
pain, he referred petitioner for pain management. (Id.) She was later evaluated by a
pain management specialist in New Jersey. (Ex. 154, pp. 27-31.)
11 Vimpat is an orally or intravenously administered anticonvulsant used as an adjunct in the treatment of
partial seizures. Vimpat, DORLAND’S MEDICAL DICTIONARY ONLINE,
https://www.dorlandsonline.com/dorland/definition?id=53152 (last visited Sept. 4, 2024); Lacosamide,
DORLAND’S MEDICAL DICTIONARY ONLINE, https://www.dorlandsonline.com/dorland/definition?id=27378
(last visited Sept. 4, 2024).
12 Petitioner subsequently presented to the emergency department on September 4, 2019, reporting an
adverse reaction (nausea and vomiting) to her IVIG treatment. (Ex. 101, pp. 168-69.)
12

Case 1:17-vv-01915-LAS Document 159 Filed 10/18/24 Page 13 of 37
Petitioner sought another opinion from neurologists, Drs. Lee (resident) and
Hurst (assistant professor), on January 21, 2020. (Ex. 103, p. 15.) Petitioner was
reportedly concerned with her lack of response to typical treatments for CIDP. (Id. at
20.) Dr. Lee cautioned that sequela of GBS can be persistent, but given the lack of
response she recommended discontinuing IVIG and plasmapheresis. She also
recommended new electrodiagnostic testing, given that prior study was not indicative of
a demyelinating polyneuropathy. She felt petitioner’s pain and hyperesthesia were
more likely due to her small fiber neuropathy. Dr. Lee recommended that petitioner
follow up with a rheumatologist. (Id.) Petitioner questioned whether she could get into
a clinical trial and also raised this issue when she followed up with Dr. Suresh a month
later. (Id. at 9, 22.) When petitioner saw Dr. Suresh in February of 2020, he noted that
her symptoms have been essentially unchanged for about 3-4 years, except for
episodes of chest pressure with hyperventilation. (Id. at 9.) Dr. Suresh maintained his
diagnosis of small fiber neuropathy, but offered to repeat petitioner’s EMG/NCS testing.
(Id. at 14.) However, petitioner declined. He noted that petitioner does not qualify for
plasmapheresis or IVIG, due to her lack of demyelinating features, and indicated that
“we are out of options for her in terms of treatment for [small fiber neuropathy].”
Petitioner was directed to follow up in one year. (Id.)
Petitioner then returned to Dr. Vukic on October 22, 2020. (Ex. 154, p. 2.)
Petitioner reported that her symptoms had worsened while she was in Florida,
describing generalized weakness in the arms and legs, as well as generalized
numbness, including the tongue. (Id.) Dr. Vukic now assessed small fiber neuropathy,
indicating “[t]he etiology of her symptoms is not entirely clear but I am suspicious this is
a manifestation of her underlying rheumatologic condition with a superimposed
component of small fiber polyneuropathy.” (Id. at 6.) He recommended a repeat EMG
to evaluate for large fiber polyneuropathy. (Id.) Her electrodiagnostic study
“demonstrate[d] carpal tunnel syndrome but no other explanation for her numbness
which is different from her typical small fiber neuropathy numbness.” (Id. at 1.) Brain
and cervical spine MRIs were recommended. (Id.) However, Dr. Vukic did not find the
MRIs remarkable and ordered a further study with contrast to evaluate the cranial
nerves, given petitioner’s reported facial numbness. (Ex. 155, pp. 15, 20.) As of
January 5, 2021, Dr. Vukic again opined that petitioner’s symptomatology and prior
response to IVIG were consistent with CIDP, and he recommended resuming IVIG. (Id.
at 20.) As of May 4, 2021, petitioner reported that her strength was improving, but her
facial symptoms persisted. (Id. at 9.) Her MRI showed microvascular changes. (Id.)
Dr. Vukic felt the facial symptoms were manifestations of CIDP, but also recommended
testing for Lyme titer. (Id. at 14.) As of July 6, 2021, petitioner reported increased
confusion and forgetfulness, difficulty controlling her temperature, and altered feeling in
her face radiating over the top of her head. (Id. at 2-3.) Dr. Vukic felt the etiology for
petitioner’s memory symptoms was not clear and ordered further workup, including a
repeat MRI and EEG. (Id. at 7.)
On August 23, 2021, petitioner established care with a new neurologist, Dr.
Dover. (Ex. 153, p. 9.) Dr. Dover remarked that petitioner had a “complicated” history.
13

Case 1:17-vv-01915-LAS Document 159 Filed 10/18/24 Page 14 of 37
(Id. at 12.) Dr. Dover recommended continuing IVIG while Dr. Vukic’s records were
obtained, along with petitioner’s prior autoantibody testing and skin biopsy results. (Id.)
Petitioner saw Dr. Dover again in December of 2021 and February of 2022 with no
change in plan. (Id. at 5-8.) Dr. Dover did not confirm whether she reviewed
petitioner’s prior records, but characterized petitioner as having “a known history of
CIDP.” (Id.) As of May of 2022, petitioner reported that her condition continued to
worsen despite resuming IVIG, noting fatigue in particular. (Id. at 2.) Petitioner wanted
to be assessed for use of rituximab.13 (Id.) Dr. Dover characterized petitioner’s CIDP
as an “established diagnosis, stable.” (Id. at 3.) She explained that “I see no evidence
of objective worsening of [petitioner’s] polyneuropathy. In fact, her symptoms appear to
be well controlled.” (Id.) Dr. Morris would not recommend rituximab because it benefits
only a specific type of polyneuropathy and she did not feel comfortable switching
petitioner from IVIG absent objective signs of decline. She recommended petitioner see
a neuro-immunologist. (Id.) During this period, petitioner was also referred to a neuro-
ophthalmologist due to diplopia. (Ex. 159.) It was concluded that the diplopia was non-
specific, having no finding to suggest myasthenia gravis. (Id. at 7.)
On November 9, 2022, petitioner saw neurologist and multiple sclerosis
specialist, Dr. Sylvester. (Ex. 160, p. 93.) Dr. Sylvester took a history from petitioner,
reviewed petitioner’s prior medical records and results, and conducted a neurologic
exam. (Id. at 93-95.) He characterized petitioner’s diagnosis as being in need of
confirmation, but was willing to prescribe rituximab or another immune suppressive if
ongoing treatment was warranted. (Id. at 95.) As of January 27, 2023, Dr. Sylvester
planned to obtain a new EMG of petitioner’s upper and lower extremities and intended
to discuss the case further with Dr. Dover. (Id. at 22-23.) He was willing to consider
initiating treatment with rituximab. (Id.)
No further records were filed.
b. As reflected in affidavits
Petitioner has filed four affidavits in this case. (Exs. 17, 28, 29, 157.) Her son,
Matthew Bogholtz, also provided an affidavit. (Ex. 158.) These affidavits go into detail
regarding the effect that petitioner’s injury, and the process of pursuing a claim in this
program, have had. Petitioner expresses that her illness “has stripped my life away and
left me with a shell of my former existence.” (Ex. 28, p. 15.) I have reviewed these
affidavits carefully. However, because it is the significance of the medical facts, rather
than the facts themselves, that are at issue, it is not necessary to describe petitioner’s
13 Rituximab is an intravenously administered chimeric murine/human monoclonal antibody that binds the
CD 20 antigen and is used as an antineoplastic in the treatment of CD20-positive, B-cell non-Hodgkin
lymphoma. Rituximab, DORLAND’S MEDICAL DICTIONARY ONLINE,
https://www.dorlandsonline.com/dorland/definition?id=43977 (last visited Sept. 4, 2024). However, it has
also been used to treat CIDP. (Emily K. Mathey et al., Chronic Inflammatory Demyelinating
Polyradiculopathy: From Pathology to Phenotype, 86 J. NEUROLOGY NEUROSURGERY & PSYCHIATRY 973
(2015) (Ex. 74); C.A. Vedeler et al., Chronic Inflammatory Demyelinating Polyneuropathy (CIDP), 127
ACTA NEUROLOGICA SCANDINAVICA SUPPLEMENTUM 48 (2013) (Ex. 98).)
14

Case 1:17-vv-01915-LAS Document 159 Filed 10/18/24 Page 15 of 37
affidavits in detail. With respect to the issues discussed in this decision, these affidavits
primarily have the effect of stressing from petitioner’s own perspective that her condition
arose post-vaccination. Petitioner asserts that she suffers CIDP, Sjӧgren’s syndrome,
tinnitus, and dysphagia. (Ex. 17, p. 4.)
IV. Summary of Expert Opinions
a. Diagnosis
i. Petitioner’s neurology expert, Nizar Souayah, M.D.14
Dr. Souayah explains that CIDP represents a group of acquired polyneuropathies
characterized by symmetric weakness involving the proximal and distal muscles that
progresses over at least two months. (Ex. 42, p. 17.) It has a variable clinical course,
which can be either progressing or relapsing, but is characterized by longstanding
multifocal demyelination affecting the spinal roots, major plexus, and proximal nerve
trunks. (Id. (citing James H. Austin, Recurrent Polyneuropathies and Their
Corticosteroid Treatment: With Five-Year Observations of a Placebo-Controlled Case
Treated with Corticotrophin, Cortisone, and Prednisone, 81 BRAIN 157 (1958) (Ex. 46);
Peter James Dyck et al., Chronic Inflammatory Polyradiculoneuropathy, 50 MAYO CLINIC
PROC. 621 (1975) (Ex. 57); J.W. Prineas & J.G. McLeod, Chronic Relapsing
Polyneuritis, 27 J. NEUROLOGICAL SCIS. 427 (1976) (Ex. 81); Gérard Said, Chronic
Inflammatory Demyelinating Polyneuropathy, 16 NEUROMUSCULAR DISORDERS 293
(2006) (Ex. 91); P.K. Thomas et al., Chronic Demyelinating Peripheral Neuropathy
Associated with Multifocal Central Nervous System Demyelination, 110 BRAIN 53 (1987)
(Ex. 97)).) The most common or “classic” form of CIDP involves both motor and
sensory deficits. (Id. at 18.) However, there are sensory-predominant forms of CIDP
that are characterized by paresthesia and gait dysfunction. (Id. (citing Xavier Ayrignac
et al., Sensory Chronic Inflammatory Demyelinating Polyneuropathy: An Under-
Recognized Entity?, MUSCLE & NERVE, November 2013, at 727 (Ex. 47); Emily K.
Mathey et al., Chronic Inflammatory Demyelinating Polyradiculopathy: From Pathology
to Phenotype, 86 J. NEUROLOGY NEUROSURGERY & PSYCHIATRY 973 (2015) (Ex. 74);
Francisco T. Rotta et al., The Spectrum of Chronic Inflammatory Demyelinating
14 Dr. Souayah received his medical degree from Medical School of Tunis, Tunisia, in 1990, before going
on to complete several internships and residencies in internal medicine and neurology. (Ex. 43, p. 1.) He
also completed clinical and research fellowships in electromyography/neuromuscular diseases and
neuroscience, with a specific focus in neuroinflammation in neurodegenerative disorders. (Id.) Dr.
Souayah has been board certified in neurology, with a subspecialty in electrodiagnostic medicine and
neuromuscular medicine, and he maintains an active medical license in New Jersey. (Id. at 1-2; Ex. 42,
p. 1.) He currently works as a professor of pharmacology and neurology at Rutgers-New Jersey Medical
School and maintains a clinical practice as director of the MDA Clinic, as well as director of the
electromyography laboratory and peripheral neuropathy center, at Rutgers-New Jersey Medical School.
(Ex. 43, p. 2; Ex. 42, p. 1.) In his clinical practice, Dr. Souayah regularly diagnoses and treats patients
with CIDP. (Ex. 42, pp. 1, 4.) In his research capacity, Dr. Souayah has investigated the causal
relationship between vaccines and adverse events, particularly the incidence of neurological adverse
reactions related to vaccines. (Id. at 1.) He has authored several peer-reviewed journal articles that he
contends inform the issues of this case. (Id. at 1-4; see also Ex. 43, pp. 12-24.)
15

Case 1:17-vv-01915-LAS Document 159 Filed 10/18/24 Page 16 of 37
Polyneuropathy, 173 J. NEUROLOGICAL SCIS. 129 (2000) (Ex. 89); C.A. Vedeler et al.,
Chronic Inflammatory Demyelinating Polyneuropathy (CIDP), 127 ACTA NEUROLOGICA
SCANDINAVICA SUPPLEMENTUM 48 (2013) (Ex. 98)).) Despite the sensory predominance,
this form of CIDP can demonstrate distal weakness and motor nerve conduction
abnormalities on electrodiagnostic testing. (Id. (citing Mathey et al., supra, at Ex. 74;
Shin J. Oh et al., “Chronic Sensory Demyelinating Neuropathy”: Chronic Inflammatory
Demyelinating Polyneuropathy Presenting as a Pure Sensory Neuropathy, 55 J.
NEUROLOGY NEUROSURGERY & PSYCHIATRY 677 (1992) (Ex. 80); Vedeler et al., supra, at
Ex. 98).)
In petitioner’s case, Dr. Souayah finds the following features indicative of CIDP:
• numbness starting in the hands and progressing to her feet three days
later;
• subsequent unsteady gait and reduced dexterity;
• reduced deep tendon reflexes upon neurologic examination in both upper
extremities and absent in the ankles bilaterally;
• abnormal vibration sensation;
• positive Romberg sign;
• a relapsing course of neuropathy;
• electrodiagnostic evidence of acute moderate predominantly motor
demyelination; and
• partial improvement with IVIG treatment.
(Id. at 19-20.)
Dr. Souayah agrees with Dr. Callaghan that petitioner does not meet the
European Federation of Neurological Societies/Peripheral Nerve Society (“EFNS/PNS”)
CIDP diagnostic criteria.15 (Ex. 111, p. 2.) However, he indicates that these diagnostic
criteria reflect the typical forms of CIDP and are not very sensitive, especially for
sensory forms of CIDP. (Id.) He is critical of Dr. Callaghan for relying on medical
records from more than two years after the initial onset of her condition to doubt her
diagnosis and for failing to offer any other plausible diagnosis. (Id. at 2-3.)
Nonetheless, he acknowledges that over time petitioner’s neurophysiological evaluation
changed such that she no longer fits the typical manifestations of CIDP or inflammatory
neuropathy. (Id. at 3.) However, contrary to Dr. Callaghan’s interpretation of the
records, Dr. Souyah stresses that he believes petitioner’s condition did respond to IVIG
treatment. (Id.)
Dr. Souayah acknowledges that, as of April 13, 2018, Dr. Brannagan found no
clinical or neurophysiological evidence of large fiber neuropathy and that petitioner
subsequently had a skin biopsy that was positive for small fiber neuropathy, consistent
15 Although both parties’ experts reference the ECFNS/PNS CIDP diagnostic criteria, neither has actually
filed the published criteria. However, because both parties’ experts agree petitioner does not meet these
criteria, this is not a critical omission.
16

Case 1:17-vv-01915-LAS Document 159 Filed 10/18/24 Page 17 of 37
with autonomic neuropathy. (Ex. 150, p. 1.) Thus, to the extent Dr. Callaghan cited
symptoms beyond the scope of CIDP (namely, shortness of breath, chest tightness,
dizziness, lightheadedness, vertigo, constipation, difficulty urinating, and dysphagia), Dr.
Souayah opined that these are likely symptoms of small fiber neuropathy, though he
also observed that autonomic dysfunction is reported in many cases of CIDP. (Ex. 111,
p. 3.) However, Dr. Souayah concedes that petitioner’s diagnosis changed from CIDP
to small fiber neuropathy. (Ex. 150, p. 2.)
ii. Respondent’s neurology expert, Brian Callaghan, M.D.16
Dr. Callaghan acknowledges that petitioner presented with numbness in the
hands and toes that was initially diagnosed as GBS and then CIDP; however, he does
not agree that petitioner suffered CIDP. (Ex. A, p. 3.) Dr. Callaghan indicates that
CIDP is frequently misdiagnosed – with 47% of patients referred for evaluation of CIDP
having a different condition. (Id. (citing Jeffrey A. Allen & Richard A. Lewis, CIDP
Diagnostic Pitfalls and Perception of Treatment Benefit, 85 NEUROLOGY 498 (2015) (Ex.
E, Tab 1)).) He cites the EFNS/PNS CIDP criteria as instructive. (Id.) Those diagnostic
criteria require progressive, symmetric proximal weakness, as well as supportive
findings on EMG/NCS, which he asserts petitioner does not have. (Id.) Dr. Callaghan
cites several factors that inform his diagnostic opinion, specifically:
• Although petitioner’s initial EMG/NCS revealed demyelinating neuropathy,
she had four subsequent EMG/NCS studies that revealed no
demyelinating features;
• Although she has had sensory signs, her physical exams have
consistently shown normal or near normal strength over seven years;
• Her reportedly disabling symptoms (such as not being able to get out of
bed) have a “clear disconnect” from her near normal neurologic
examinations;
• She has numerous symptoms not associated with CIDP, including
shortness of breath, chest tightness, dizziness, lightheadedness,
headache, vertigo, fatigue, memory issues, constipation, difficulty
urinating, dysphagia, rectal pain, tinnitus, loss of smell, shaking,
depression, hopelessness, and weight gain;
16 Dr. Callaghan received his medical degree from the University of Pennsylvania Medical Center in 2004,
before going on to complete a residency in neurology at the University of Pennsylvania Medical Center in
2008, a neuromuscular fellowship at the University of Michigan Health System in 2009, and a Center for
Healthcare Research and Transformation Policy Fellowship at the University of Michigan in 2016. (Ex. B,
p. 1.) In the interim, Dr. Callaghan received a master’s degree in clinical research design and statistical
analysis from the University of Michigan in 2011. (Id.) He is board certified in psychiatry, neurology, and
electrodiagnostic medicine, and he maintains a medical license in Michigan. (Id.) He currently works as
an associate professor of neurology and the director of the ALS Clinic at the University of Michigan Health
System, as well as a staff physician in the Department of Neurology at VA Ann Arbor Health System. (Id.
at 1-2; Ex. A, p. 1.) Dr. Callaghan is a neuromuscular specialist with a primary interest in patients with
neuropathy, such as CIDP. (Ex. A, p. 1.) In his clinical practice, he treats approximately 30-50 GBS and
CIDP patients per year. (Id.) In his research capacity, Dr. Callaghan has authored numerous peer-
reviewed articles, book chapters, and abstracts concerning neuropathy. (Ex. B, pp. 10-17.)
17

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• She did not have a consistent response to IVIG and plasmapheresis,
which are highly effective therapies for CIDP; and
• Her treating neurologists doubted the CIDP diagnosis. In particular, it was
noted as of July 31, 2019, that there is no clear or convincing evidence of
CIDP, given a lack of response to treatment, lack of supportive EMG/NCS
findings, only marginally elevated CSF protein; and preserved reflexes
upon neurologic exam.
(Id. at 3; Ex. F, pp. 3-4.)
Dr. Callaghan acknowledges that he has no alternative diagnosis, but urges that
this does not mean that CIDP must therefore be the diagnosis. (Ex. E, p. 2.) He
asserts that it is not unusual for patients with a multitude of symptoms to lack a clear
explanation. (Id.) Dr. Callaghan disputes Dr. Souayah’s suggestion that petitioner has
a sensory-predominant form of CIDP because she had difficulty getting out of bed and
eventually became wheelchair bound secondary to weakness (Id. at 1), even though he
otherwise questioned whether that symptom could be explained by her neurologic
findings (Ex. A, p. 3; Ex. F, p. 3).
Dr. Callaghan also disagrees that petitioner has small fiber neuropathy. (Ex. E,
p. 2.) He cites the following exclusion criteria for the condition: (i) any sign of large fiber
impairment (light touch and/or vibratory and/or proprioceptive sensory loss and/or
absent deep tendon reflexes); (ii) any sign of motor fiber impairment (muscle waste
and/or weakness); (iii) any abnormality on sensorimotor NCS. (Id. (citing Grazia Devigili
et al., Diagnostic Criteria for Small Fiber Neuropathy in Clinical Practice and Research,
142 BRAIN 3728 (2019) (Ex. F, Tab 1)).) In petitioner’s case, she did have features of
large fiber involvement (decreased vibration sensation at the ankles, and decreased
ankle jerks), as well as motor fiber impairment (4+ left hip flexion strength). (Id.) Dr.
Callaghan also disagrees that petitioner meets the inclusion criteria for small fiber
neuropathy, because she did not have a QST17 performed. (Ex. F, p. 4 (citing Devigili et
al., supra, at Ex. F, Tab 1).) Dr. Callaghan acknowledges petitioner had a skin biopsy
that showed reduced nerve fiber; however, he indicates that, in his experience, the
specific test used for petitioner’s biopsy (Therapath skin biopsy) has a high rate of false
positives. (Id.) And, again, he cites petitioner as having numerous other symptoms that
are not consistent with small fiber neuropathy, ultimately opining that “[n]o known
neurologic disease can account for the multitude of symptoms that the petitioner
experienced.” (Ex. E, p. 2.)
In sum, Dr. Callaghan opines that petitioner’s clinical presentation is
irreconcilable. Her reported symptoms would require “severe” large fiber nerve
involvement; however, she had four normal EMG/NCS studies, which are the “gold
17 Quantitative sensory testing involves applying various tactile stimuli, such as light touch, heat, cold, and
vibrations, and monitoring the patient’s response as compared to either the patient’s response when
stimuli are applied to the other side of the body or a control subject’s response. Quantitative sensory
testing, DORLAND’S MEDICAL DICTIONARY ONLINE,
https://www.dorlandsonline.com/dorland/definition?id=113107 (last visited Sept. 13, 2024).
18

Case 1:17-vv-01915-LAS Document 159 Filed 10/18/24 Page 19 of 37
standard” for evaluating large fiber nerves. (Ex. F, p. 5.) Conversely, a diagnosis of
small fiber neuropathy requires the absence of large nerve involvement; this therefore
means that a small fiber neuropathy diagnosis is incompatible with petitioner’s disabling
symptoms. (Id.)
iii. Petitioner’s rheumatology expert, Samar Gupta, M.D. 18
Although petitioner had an initial presentation suspicious for either GBS or CIDP,
Dr. Gupta observes that she was also found to have high levels of ANA and SSA (or
anti-RO) antibodies, which are specific for Sjӧgren’s syndrome. (Ex. 104, p. 2.) In
contrast to Dr. Matloubian, who opined petitioner’s pre-vaccination ANA test may have
been a false negative (Ex. G, p. 10), Dr. Gupta stresses his view that these antibodies
first arose post-vaccination (Ex. 161, pp. 2-3; Ex. 151, p. 1). Dr. Lightfoot, conversely,
suggested petitioner’s post-vaccination anti-SSA result may have been a false positive.
(Ex. C, p. 5.) Dr. Gupta did not directly respond to that point, but stressed petitioner had
two positive SSA tests post-vaccination. (Ex. 161, p. 2.)
Sjӧgren’s syndrome is usually suspected in individuals with persistent dry eye
and/or dry mouth (also known as sicca symptoms), parotid gland enlargement, and anti-
SSA serology. (Ex. 104, p. 2.) However, though not diagnostic criteria, the 2016
American College of Rheumatology/European League Against Rheumatism
(ACR/EULAR) classification system for primary Sjogren’s syndrome places significant
weight on serology. (Id. (citing Caroline H. Shiboski et al., 2016 American College of
Rheumatology/European League Against Rheumatism Classification Criteria for
Primary Sjӧgren’s Syndrome: A Consensus and Data-Driven Methodology Involving
Three International Patient Cohorts, 76 ANNALS RHEUMATIC DISEASE 9 (2016) (Ex. 106)).)
Although Dr. Lightfoot suggested an anti-centromere pattern of ANA titer is indicative of
a limited scleroderma only, Dr. Gupta opines that the pattern of ANA is usually non-
specific. (Id. at 5.)
Dr. Gupta agrees with Dr. Lightfoot that positive anti-SSA is not alone diagnostic,
but stresses that he finds other features of Sjӧgren’s syndrome in petitioner’s case. (Ex.
18 Dr. Gupta received his medical degree from Maharshi Dayanand University in Rohtak, India, in 1988,
before going on to complete a residency in internal medicine and orthopedic surgery from the same
university, followed by an internship in internal medicine at Rush University Medical Center in Chicago,
Illinois, in 1996; a residency in internal medicine at Wayne State University in Detroit, Michigan, in 1998;
and a rheumatology and immunology fellowship at University of Michigan in 2000. (Ex. 105, p. 1.) He is
a member of the American College of Rheumatology, Arthritis Foundation, Scleroderma Foundation,
national Psoriasis Foundation, and Group for Research and Assessment of Psoriasis and Psoriatic
Arthritis. (Ex. 104, p.1.) He currently works as rheumatology professor at VA Ann Arbor Healthcare
System and the University of Michigan - Ann Arbor and as a co-director of the Rheumatology
Dermatology collaborative clinic at University of Michigan Veterans Affairs Medical Center. (Ex. 105, p. 1;
Ex. 104, p. 1.) His clinical and research interests focus on rheumatic diseases, including Sjӧgren’s
syndrome. (Ex. 104, p. 1.) He has treated over 200 patients with Sjӧgren’s syndrome. (Id.) In his
research capacity, he has authored numerous peer-reviewed articles that have been published in
journals, such as New England Journal of Medicine, The Lancet, and Arthritis & Rheumatism. (Id.)
19

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104, p. 5.) Dr. Gupta opines that petitioner may have had an early or incomplete
presentation of Sjӧgren’s syndrome based on the following features:
• Elevated inflammatory markers;
• Abnormal brain MRI;
• Prednisone responsive inflammatory hand arthritis;19
• Peripheral neuropathy by NCS/EMG and skin biopsy;
• Cutaneous rash;
• Parotid enlargement; and
• Sicca symptoms.
(Id. at 2-3.) Dr. Gupta acknowledges that petitioner does not meet the ACR/EULAR
criteria for Sjӧgren’s syndrome, but stresses that the classification criteria “are intended
to eliminate all but those who have incontrovertible disease.” (Id. at 3.)
Dr. Gupta explains that about 10% of Sjӧgren’s syndrome patients also have
some form of peripheral neuropathy. (Ex. 104, p. 3 (citing P. Brito-Zerón et al.,
Classification and Characterisation of Peripheral Neuropathies in 102 Patients with
Primary Sjӧgren’s Syndrome, 31 CLINICAL & EXPERIMENTAL RHEUMATOLOGY 103 (2013)
(Ex. 107)).) In these cases, neuropathic symptoms can precede diagnosis and can
involve either the large or small fibers. (Id.) Both small fiber neuropathy and CIDP have
been described in patients with Sjӧgren’s syndrome. (Id. (citing Keiko Mori et al., The
Wide Spectrum of Clinical Manifestations in Sjӧgren’s Syndrome-Associated
Neuropathy, 128 BRAIN 2518 (2005) (Ex. 108); Julius Birnbaum et al., Biopsy-Proven
Small-Fiber Neuropathy in Primary Sjӧgren’s Syndrome: Neuropathic Pain
Characteristics, Autoantibody Findings, and Histopathologic Features, 71 ARTHRITIS
CARE & RES. 936 (2019) (Ex. 109)).) Thus, Dr. Gupta opines that petitioner’s peripheral
neuropathy is a part of her Sjӧgren’s syndrome presentation. He defers to Dr. Souayah
on the exact nature of petitioner’s neuropathy (Ex. 151, p. 1); however, given that both
small fiber neuropathy and CIDP are associated with Sjӧgren’s syndrome, he opines
that petitioner’s neuropathy is associated with her Sjӧgren’s syndrome regardless of
diagnosis (Id.; Ex. 104, p 4).
iv. Respondent’s rheumatology expert, Robert Lightfoot, Jr., M.D. 20
19 Dr. Gupta further explained: “Dr. Lightfoot also mentions a history of intermittent arthritis in the small
joints of the hands, occasional swelling, and ‘up to one hour of morning stiffness’ noting that when
[petitioner] took steroids for her asthma, her finger joints felt relieved. This may indicate inflammatory
arthritis. Although osteoarthritis would get better with steroids, . . . osteoarthritis pain generally would not
present with joint swelling in hands.” (Ex. 104, p. 3.) When Dr. Matloubian entered the case, he
suggested that this passage by Dr. Gupta indicated that petitioner’s Sjӧgren’s syndrome would have
necessarily predated her vaccination based on Dr. Gupta’s assessment. (Ex. G, p. 9.) However, Dr.
Gupta indicates that this “overstates” his opinion, noting that there are no pre-vaccination medical records
addressing petitioner’s arthritis and further stressing that the records confirm petitioner was negative for
ANA and ESR prior to vaccination. (Ex. 161, pp. 2-3.)
20 Dr. Lightfoot received his medical degree from Vanderbilt University School of Medicine in 1961, before
going on to complete an internship and residency at Columbia Presbyterian Medical Center in 1962 and
1963, respectively; a residency at Vanderbilt University Hospital in 1964; and a rheumatology fellowship
20

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Dr. Lightfoot indicates,
To me, a crucial aspect of petitioner’s illness is that her symptoms were
entirely subjective (numbness, tingling, pain, weakness), rather than
objective (swelling, warmth, redness, induration, discoloration). Thus, the
outcome of any therapeutic attempt is rendered difficult to measure, and the
provider must rely on ‘patient global’ impression of his/her disease status.
(Ex. C, p. 4.) With regard to Sjӧgren’s syndrome, Dr. Lightfoot indicates that petitioner
does not meet either the ACR or the ACR/EULAR classification criteria. (Id. at 5 (citing
Shiboski et al., supra, at Ex. 106; S.C. Shiboski et al., American College of
Rheumatology Classification Criteria for Sjӧgren’s Syndrome: A Data-Driven, Expert
Consensus Approach in the Sjogren’s International Collaborative Clinical Alliance
Cohort, 64 ARTHRITIS CARE & RES. 475 (2012) (not filed)).) However, he acknowledges
these are stringent and not diagnostic criteria. (Id.) He opines that “[w]hile I cannot say
that petitioner unequivocally HAS Sjogren’s, I also cannot say that she does not have
an incomplete form that has not risen to unequivocality yet.” (Id.)
Dr. Lightfoot raises some concern with respect to petitioner’s serology. First, he
notes that petitioner’s positive ANA titer was 1:320, which is a level that can be seen in
a small number (3%) of normal individuals. (Ex. C, p. 5.) Second, he suggests that
petitioner’s record, which indicates she had “ANA screen with anti-SSA positive” likely
indicate her test was sent to a lab that uses “ANA Direct (screening) assay.” (Id.) This
methodology screens for seven to nine antibodies at once, which Dr. Lightfoot indicates
produces a high likelihood of chance findings. (Id.) Thus, he opines that “[i]t is not
possible to say if the anti-SSA had any pathophysiological role on petitioner’s illness.”
(Id.) For this reason, Dr. Lightfoot indicated that “[t]here is no clear evidence that the
anti-SSA is causally related to the alleged CIDP.” (Id. at 6.) However, because his
report pre-dated Dr. Gupta’s involvement in the case, he did not address Dr. Gupta’s
discussion of the association between Sjӧgren’s syndrome and peripheral neuropathies.
v. Respondent’s rheumatology expert, Mehrdad Matloubian, M.D.,
Ph.D. 21
at Columbia University College of Physicians and Surgeons in 1966. (Ex. D, p. 1.) He is board certified
in internal medicine and rheumatology. (Id.) At the time his expert report was submitted, Dr. Lightfoot
maintained an active medical license in Kentucky, and he worked as a Professor of Medicine Emeritus at
the University of Kentucky, a staff physician at Veterans Administration Medical Center, and active
medical staff at Albert B. Chandler Medical Center. (Id. at 2.) He had also authored several peer-
reviewed articles, book chapters, and abstracts concerning rheumatology. (Id. at 18-26.)
21 Dr. Matloubian received his medical degree and Ph.D. in virology from the University of California in
1996, where he remained to complete an internship in 1997, residency in 1998, rheumatology fellowship
in 2001, and post-doctoral fellowship in 2004. (Ex. H, p. 1.) He is board certified in internal medicine and
rheumatology, and he maintains an active medical license in California. (Id. at 1-2.) Dr. Matloubian
currently works as a professor of medicine at the University of California, as well as an inpatient
rheumatology and molecular medicine consultant. (Id. at 2-3.) He is also a member of the American
College of Rheumatology, Northern California Chapter of Arthritis Foundation, American Association of
21

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Dr. Matloubian suggests that, based on his review of petitioner’s medical history,
“it is quite apparent that there was a lack of consensus among her treating neurologists
regarding specific diagnoses that would explain her symptomology.” (Ex. G, p. 7.) He
defers to Dr. Callaghan regarding any specific neurologic diagnosis. (Id.) However, he
does agree that many patients with rheumatologic diseases do have neurological
manifestations. (Id.) Consistent with Dr. Gupta’s opinion, Dr. Matloubian explained that
both CIDP and small fiber neuropathy can be associated with Sjӧgren’s syndrome and
that the neurological symptoms can be the first manifestations of Sjӧgren’s syndrome.
(Id. at 8 (citing Alen N. Baer & Shamik Bhattacharyya, UpToDate: Neurologic
Manifestations of Sjӧgren’s Syndrome (2022) (Ex. G, Tab 1); Mary Margaretten,
Neurologic Manifestations of Primary Sjӧgren Syndrome, 43 RHEUMATIC DISEASES
CLINICS N. AM. 519 (2017) (Ex. G, Tab 4)).) Thus, although petitioner did not have sicca
symptoms typical of Sjӧgren’s syndrome, this is still compatible with Sjӧgren’s
associated neurological disease. (Id.) Dr. Matloubian opines that, “[i]f petitioner was
diagnosed with CIDP and/or SFN, I think it would be reasonable to attribute them to
Sjogren’s in light of a positive SSA and history of an intermittent inflammatory arthritis
affecting the MCP joints of hands.”22 (Id. at 8-9.) Although petitioner’s neurologic
diagnosis is unsettled, Dr. Matloubian opines that “in the setting of a peripheral
neuropathy and history of arthritis she was appropriately labeled as having Sjogren’s.”
(Id. at 12.) However, based on his assessment of petitioner’s hand arthritis and the
possibility of a false negative ANA result in 2012, Dr. Matloubian opines that petitioner’s
Sjӧgren’s syndrome predated her vaccination. (Id. at 9-10, 12.) Dr. Matloubian
stresses that petitioner was never tested for SSA prior to vaccination. (Id. at 9.)
b. Causation
i. Petitioner’s experts (Drs. Souayah and Gupta)
Dr. Souayah grounds petitioner’s theory of causation first and foremost in the
context of CIDP, suggesting that CIDP patients have often had an infection or
vaccination within the six weeks preceding onset of their condition. (Ex. 42, p. 19 (citing
Pamela A. McCombe et al., Studies of HLA Associations in Male and Female Patients
Immunologists, and American Society for Clinical Investigation. (Id. at 3.) He has authored peer-
reviewed articles concerning innate and adaptive immune responses, including those of T and B cells, to
acute and chronic viral infections. (Ex. G, p. 1; Ex. H, pp. 10-14.)
22 Dr. Matloubian indicated that one of petitioner’s treating physicians “considered her history of arthritis
affecting her MCP and PIP joints with prolonged morning stiffness and intermittent swelling as possible
manifestations of Sjogren’s (Ex. 2 at 132 and 135).” (Ex. G, p. 8.) He explained that,
[a]lthough petitioner does have a history of osteoarthritis, this disease mainly affects the
PIP and DIP [distal interphalangeal joints] of the hands and spares the MCP joints. MCP
joints, which were symptomatic in petitioner are usually involved in inflammatory arthritis,
such as rheumatoid arthritis, lupus and Sjogren’s and not in osteoarthritis . . . .
(Id. (citing James R. O’Dell et al., Chapter 15. Rheumatoid Arthritis, in CURRENT DIAGNOSIS & TREATMENT:
RHEUMATOLOGY (3rd ed., 2013) (Ex. G, Tab 5, fig.15-1)).)
22

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with Guillain-Barré Syndrome (GBS) and Chronic Inflammatory Demyelinating
Polyradiculoneuropathy (CIDP), 180 J. NEUROIMMUNOLOGY 172 (2006) (Ex. 76); Said,
supra, at Ex. 91).) Dr. Souyah indicates that, like GBS, CIDP is a B cell mediated
condition of humeral immunity responsive to unknown antigens; however, unlike GBS,
CIDP has a more persistent or recurrent course, that is likely explained by T-cell
dysfunction. (Id. at 19-20 (citing Richard A.C. Hughes et al., Pathogenesis of Chronic
Inflammatory Demyelinating Polyradiculneuropathy, 11 J. PERIPHERAL NERVOUS SYS. 30
(2006) (Ex. 65); Sandra Bick et al., Intravenous Immunoglobulin Inhibits BAFF
Production in Chronic Inflammatory Demyelinating Polyradiculoneuropathy – A New
Mechanism of Action?, 256 J. NEUROIMMUNOLOGY 84 (2013) (Ex. 49); Simon Rinaldi &
David L.H. Bennett, Pathogenic Mechanisms in Inflammatory and Paraproteinaemic
Peripheral Neuropathies, 27 CURRENT OP. NEUROLOGY 541 (2014) (Ex. 88)).) Dr.
Souayah cites a number of case reports for the proposition that CIDP has been
identified following several different vaccines, including the flu vaccine. (Id. at 21-22
(citing Claude Vital et al., Postvaccinal Inflammatory Neuropathy: Peripheral Nerve
Biopsy in 3 Cases, 7 J. PERIPHERAL NERVOUS SYS. 163 (2002) (Ex. 100); Karissa L.
Gable et al., Distal Acquired Demyelinating Symmetric Neuropathy After Vaccination, 14
J. CLINICAL NEUROMUSCULAR DISEASE 117 (2012) (Ex. 60); Krista Kuitwaard et al.,
Recurrences, Vaccinations and Long-Term Symptoms in GBS and CIDP, 14 J.
PERIPHERAL NERVOUS SYS. 310 (2009) (Ex. 69); J.M. Brostoff et al., Post-Influenza
Vaccine Chronic Inflammatory Demyelinating Polyneuropathy, 37 AGE & AGEING 229
(2008) (Ex. 51); Praful Kelkar, Chronic Inflammatory Demyelinating Polyneuropathy
(CIDP) with Rapid Progression After Influenza Vaccination: A Report of Three Cases, 8
J. CLINICAL NEUROMUSCULAR DISEASE 20 (2006) (Ex. 67); Gauthier Remiche et al.,
Chronic Inflammatory Demyelinating Polyradiculoneuropathy (CIDP) Associated to
Hereditary Neuropathy with Liability to Pressure Palsies (HNPP) and Revealed After
Influenza AH1N1 Vaccination, 113 ACTA NEUROLOGICA BELGICA 519 (2013) (Ex. 85);
Shee Ten Tay & Wing P. Chan, A 9-Year-Old Femail with Bilateral Leg Weakness After
Influenza Vaccination, 43 PEDIATRIC ANNALS 440 (2014) (Ex. 96)).) Dr. Souayah
suggests that the same concepts that support vaccine-causation of GBS – molecular
mimicry, epitope spreading, bystander activation, and polyclonal activation – can
support vaccine causation of CIDP. (Id. at 24-26 (citing Nancy Agmon-Levin et al.,
Vaccines and Autoimmunity, 5 NATURE 648 (2009) (Ex. 44); Penina Haber et al.,
Vaccines and Guillain-Barré Syndrome, 32 DRUG SAFETY 309 (2009) (Ex. 62)).) In his
second report, Dr. Souyah further defended his application of these concepts to CIDP in
response to Dr. Callaghan’s criticism that his theory relied primarily on case reports.
(Ex. 111, pp. 4-6.) Thus, in his first two reports, Dr. Souayah posited a direct causal
relationship between petitioner’s vaccination and her proposed CIDP. (Id. at 6; Ex. 42,
pp. 26-27.)
However, Dr. Gupta subsequently opined on petitioner’s behalf that her
neurologic condition, whatever its diagnosis, was an aspect of her separately diagnosed
Sjӧgren’s syndrome. (Ex. 104, p. 4.) Dr. Gupta indicated that “[a] mechanism between
peripheral neuropathies and [Sjӧgren’s syndrome] is unresolved,” but stressed that
Sjӧgren’s syndrome, CIDP, and small fiber neuropathy, are all autoimmune conditions.
(Ex. 151.) Accordingly, he opined that petitioner’s entire presentation is “consistent with
23

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a vaccine induced illness in the mosaic of autoimmunity.” (Id.) However, Dr. Gupta did
not explain any direct causal relationship between vaccination and Sjӧgren’s syndrome.
(Exs. 104, 151.) Instead, he deferred to Dr. Souayah with respect to any theory of
causation linking petitioner’s peripheral neuropathy to her vaccination. (Ex. 161, p. 3.)
Thus, Dr. Souayah opined that Dr. Gupta’s reference to the mosaic of autoimmunity is
consistent with this theory of causation, explaining:
Importantly, the mechanisms I previously outlined regarding the
development of [petitioner’s] vaccine-related CIDP/inflammatory
neuropathy are best summarized as the loss of immunological tolerance to
self-antigens. The mosaic of autoimmunity best describes the interplay of
[petitioner’s] diagnoses, clinical presentation, electrodiagnostic testing and
ANA/SSA serologies.
(Ex. 150, p. 2.) In his final report, Dr. Souayah reiterated that his opinion is premised on
the notion that petitioner “most likely developed an inflammatory neuropathy/CIDP
variant after vaccination.” (Id. at 1.) Dr. Souayah did not in any of his reports explain
any direct causal relationship between vaccination and small fiber neuropathy. (Exs.
42, 111, 150.) Neither Dr. Souyah nor Dr. Gupta explain exactly what they mean by
“mosaic of autoimmunity.” This may simply refer to the notion that autoimmunity is
believed to be multifactorial, involving both genetic and environmental factors. (Agmon-
Levin et al., supra, at Ex. 44 (citing reference 27, a publication by Shoenfeld et al., titled
“The Mosaic of Autoimmunity: Genetic Factors Involved in Autoimmune Disease”).)
Ultimately, Dr. Souayah opines that “[n]one of these conditions were present
prior to [petitioner’s] vaccination, and all can be attributable to a loss of immunological
tolerance to self-antigens.” (Ex. 150, p. 2.) Dr. Souayah finds causal significance in the
fact that petitioner experienced onset of numbness and tingling in her hands, feet, and
face within approximately two weeks of her vaccination and evidence of motor
demyelinating peripheral neuropathy upon electrodiagnostic testing as of October 28,
2015. (Id.) Dr. Souayah opines this is consistent with the timing of an antibody
response to vaccination leading to nerve damage. (Ex. 42, pp. 24, 26.) Dr. Gupta
further stresses that petitioner’s positive serology likewise first occurred post-
vaccination. (Ex. 161, p. 1.)
ii. Respondent’s experts (Drs. Callaghan, Lightfoot, and Matloubian)
Dr. Callaghan contends that the link Dr. Souayah proposes between CIDP and
vaccination is based merely upon case reports. (Ex. A, p. 4.) However, case reports
show only proximate temporal relationship, which does not establish causation. (Id.)
Moreover, Dr. Callaghan calls into question any parallel between GBS and CIDP,
explaining that, in addition to other pathogenic differences, CIDP is rarely preceded by
infection, reducing the likelihood that it is explained by the triggering of molecular
mimicry. (Id. (citing Eroboghene E. Ubogu, Inflammatory Neuropathies: Pathology,
Molecular Markers and Targets for Specific Therapeutic Intervention, 130 ACTA
NEUROPATHOLOGICA 445 (2015) (Ex. A, Tab 1); Marinos C. Dalakas, Pathogenesis of
24

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Immune-Mediated Neuropathies, 1852 BIOCHIMICA ET BIOPHYSICA ACTA 658 (2015) (Ex.
A, Tab 2)).) Dr. Callaghan further cites one study that investigated, but failed to detect,
a causal association between CIDP and vaccination. (Id. (citing P.E. Doneddu et al.,
Risk Factors for Chronic Inflammatory Demyelinating Polyradiculoneuropathy (CIDP):
Antecedent Events, Lifestyle and Dietary Habits. Data from the Italian CIDP Database,
27 EUR. J. NEUROLOGY 136 (2020) (Ex. A, Tab 3)).) Dr. Callaghan agrees that CIDP is
“definitely” an autoimmune disease, but stresses that vaccine causation does not
necessarily follow from that fact. (Ex. E, p. 3.) He asserts that Dr. Souayah provided no
evidence to substantiate that mechanisms such as molecular mimicry or bystander
activation explain the flu vaccine as a cause of either CIDP or small fiber neuropathy.
(Id.)
Although Dr. Lightfoot did not address the causes of Sjӧgren’s syndrome (Ex. C),
Dr. Matloubian subsequently opined that the cause of Sjӧgren’s syndrome is unknown
(Ex. G, p. 9). However, he stressed that Sjӧgren’s syndrome is not known to follow
infection, including influenza infection, which makes it very unlikely that the flu vaccine
could cause Sjӧgren’s syndrome via molecular mimicry. (Id.) Further, Dr. Matloubian
challenges Dr. Souayah’s suggestion that loss of immune tolerance is generalizable.
(Id. at 11.) He indicates that
This argument is based more on temporal association than on a coherent
medical theory. Most autoimmune diseases, such as rheumatoid arthritis,
psoriasis, and Sjogren’s are not associated with acute infection and
therefore, are not considered to be initiated by an acute infection in a matter
of weeks . . . . most individuals with clinical diagnosis of Sjogren’s are found
to have anti-SSA autoantibodies for many years prior to disease
presentation. This is also true for rheumatoid arthritis and lupus, indicating
that breakdown of immunological tolerance leading to autoimmunity occurs
years before the autoimmune disease becomes clinically apparent. An
external environmental factor (trigger) for transition from a pre-clinical state
to clinically apparent disease for these conditions has not been identified.
(Id. (internal footnote omitted).)
V. Analysis
a. Diagnosis
The Vaccine Act requires a petitioner to present a claim for compensation for a
“vaccine-related injury or death,” as well as preponderant evidence supporting her
claim. § 300aa-11(c); § 300aa-13(a)(1)(A); Stillwell v. Sec’y of Health & Human Servs.,
118 Fed. Cl. 47, 56 (2014), aff’d, 607 F. App’x 997 (Fed. Cir. 2015). Accordingly, a
petitioner must specify her “vaccine-related injury and shoulder the burden of proof on
causation.” Broekelschen v. Sec’y of Health & Human Servs., 618 F.3d 1339, 1346
(Fed. Cir. 2010). Where the identity and nature of the vaccine-related injury is in
dispute, the Federal Circuit has concluded that it is “appropriate for the special master
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to first determine what injury, if any, [is] supported by the evidence presented in the
record before applying the Althen test to determine causation.” Lombardi v. Sec’y of
Health & Human Servs., 656 F.3d 1343, 1352-53 (Fed. Cir. 2011). However, “the
function of a special master is not to ‘diagnose’ vaccine-related injuries.” Andreu ex rel.
Andreu v. Sec’y of Health & Human Servs., 569 F.3d 1367, 1382 (Fed. Cir. 2009).
Instead, the special master must determine, “based on the record evidence as a whole
and the totality of the case, whether it has been shown by a preponderance of the
evidence that a vaccine caused the [petitioner’s] injury.” Id. (quoting Knudsen ex rel.
Knudsen v. Sec’y of Health & Human Servs., 35 F.3d 543, 549 (Fed. Cir. 1994)).
Petitioner “maintains that she suffered an autoimmune inflammatory neuropathy,
described as a CIDP variant, at outset. She subsequently developed small fiber
neuropathy. . . .” (ECF No. 152, p. 1 n.2.) Petitioner acknowledges in her brief that she
“also had serologic testing consistent with Sjogren’s syndrome” (Id.), but stresses that
she does not fulfill the diagnostic criteria for Sjӧgren’s syndrome (Id. at 107). However,
petitioner does acknowledge that she developed a rheumatologic condition. (Id. at 107-
09.) As noted above, petitioner confirms in her affidavit that she considers herself to be
suffering Sjӧgren’s syndrome. (Ex. 17, p. 4.) Respondent disputes that petitioner has
established that she suffered either CIDP or small fiber neuropathy. (ECF No. 154, pp.
19-24.) Instead, he asserts that petitioner suffers Sjӧgren’s syndrome. (Id. at 24.) And,
further, any CIDP or small fiber neuropathy, if present, would be attributable to her
Sjӧgren’s syndrome. (Id.)
i. There is preponderant evidence that petitioner suffers Sjӧgren’s
syndrome
First, I confirm that the record evidence preponderates in favor of a finding that
petitioner suffers Sjӧgren’s syndrome. As explained above, petitioner tested positive for
ANA and SSA antibodies. (Ex. 2, pp. 132, 135.) And, as Dr. Gupta explained, SSA
antibodies are specific for Sjӧgren’s syndrome. (Ex. 104, p. 2.) Thus, both parties have
presented expert rheumatology opinions (by Drs. Gupta and Matloubian) confirming that
petitioner suffered Sjӧgren’s syndrome. (Id. at 2-3; Ex. G, pp. 8-9.) Further, although
Dr. Lightfoot felt petitioner may have had only an equivocal “incomplete” form of
Sjӧgren’s syndrome (Ex. C, p. 5), Dr. Gupta explained that petitioner’s presentation was
not limited to her serology result, given that she had, inter alia, associated peripheral
neuropathy (Ex. 104, p. 4). This is consistent with how petitioner’s case was viewed by
her treating rheumatologists. (Ex. 2, pp. 135-36 (opining Sjӧgren’s syndrome may
explain both serology and neurologic symptoms); Ex. 15, p. 5 (noting petitioner’s
positive SSA and explaining peripheral neuropathies can present without classic signs
of sicca); Ex. 36, p. 12 (indicating petitioner has Sjӧgren’s with neurological
manifestations).) Respondent’s rheumatology expert, Dr. Matloubian, likewise agrees.23
(Ex. G, p. 8.)
23 Respondent argues that Dr. Matloubian’s opinion should be given greater weight than Dr. Lightfoot’s
opinion because Dr. Matloubian was able to consider more evidence than Dr. Lightfoot was able to
review. (ECF No. 154, p. 29 n.15.) Petitioner disagrees. (ECF No. 155, pp. 2-6.) The potential import of
this would be that Dr. Matloubian was more forceful in opining that petitioner suffered Sjӧgren’s syndrome
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Accordingly, there is preponderant evidence that petitioner suffers Sjӧgren’s
syndrome with neurological manifestations. Whether those neurological manifestations
can be further categorized is discussed in the two sections that follow.
ii. There is preponderant evidence that petitioner suffered small fiber
neuropathy as a sequela of her Sjӧgren’s syndrome
The diagnostic inclusion criteria for small fiber neuropathy as cited by Dr.
Callaghan include: (1) clinical signs of small fiber impairment; (2) abnormal warm or
cold thresholds at the foot, assessed by quantitative sensory testing (“QST”); and (3)
reduced nerve fiber density at the distal leg. (Devigili et al., supra, at Ex. F, Tab 1, p. 2.)
Respondent stresses that petitioner never underwent QST, suggesting this precludes a
small fiber neuropathy diagnosis. (ECF No. 154, p. 23.) However, the diagnostic
criteria requires only that a patient demonstrate two of these three criteria. (Devigili et
al., supra, at Ex. F, Tab 1, p. 2.) There is no dispute that petitioner has clinical signs of
small fiber impairment. (Ex. G, p. 7; Ex. 161, p. 1.) Accordingly, if petitioner’s biopsy
result is credited, the fact that petitioner never underwent QST is immaterial. Given that
the skin biopsy result was accepted by the treating physicians (Ex. 154, p. 42), I do not
find Dr. Callaghan’s anecdotal experience with false positives (Ex. F, p. 4), standing
alone, as sufficient basis for discounting that result. Dr. Callaghan did not identify any
specific methodologic deficiency by Therapath nor did he identify any issue with
petitioner’s own biopsy collection (see Ex. 30, p. 40). The actual results showed
“significant” reduction in nerve fiber density such that petitioner’s results were
“abnormal” (as opposed to “low normal”) (Ex. 154, p. 63), suggesting it was not an
equivocal finding. Thus, petitioner meets the inclusion criteria for small fiber
neuropathy.
Ordinarily, under the diagnostic criteria for small fiber neuropathy cited by Dr.
Callaghan, patients are excluded from diagnosis if they have: (1) any clinical sign of
large fiber involvement; (2) any abnormality on nerve conduction study. (Devigili et al.,
supra, at Ex. F, Tab 1, p. 2.) Dr. Callaghan cites these criteria as a reason for doubting
petitioner’s small fiber neuropathy diagnosis. (Ex. F, p. 4.) However, petitioner has filed
medical literature demonstrating that, in the context of Sjӧgren’s syndrome, 45% of
patients will have “mixed,” rather than “pure,” small fiber neuropathy. (Birnbaum et al.,
supra, at Ex. 109, p. 1.) Patients with “mixed” small fiber neuropathy will have some
evidence of large fiber involvement. Specifically, the patients reviewed by Birnbaum et
al. demonstrated: “areflexia, positive Romberg test, gait ataxia, and absent sensory
nerve action potentials.” (Id. at 4.) Some patients will even have evidence of motor
and that Sjӧgren’s syndrome would explain her neuropathy. However, petitioner acknowledges that “the
dispute here is between respondent’s experts . . . this does not appear to be a disputed matter between
opposing parties that requires the Court’s adjudication.” (ECF No. 152, p. 103 n.28.) Dr. Lightfoot’s
opinion, though equivocal, was explicit in opining that he could not rule out Sjӧgren’s syndrome (Ex. C, p.
5), and petitioner’s own expert, Dr. Gupta, affirmatively opined, in complete agreement with Dr.
Matloubian, that petitioner did have Sjӧgren’s syndrome and that her peripheral neuropathy was
associated with her Sjogren’s syndrome (Ex. 104, p. 4).
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involvement on NCS but no detectable weakness on physical examination, suggesting a
subclinical motor nerve involvement. (Id.) Notably, these same features – areflexia,
positive Romberg, and gait ataxia – have been stressed by petitioner as otherwise
indicating a sensory variant CIDP. (ECF No. 152, pp. 88-89 (discussing Dr. Souayah’s
opinion at Ex. 42, p. 19 and Ex. 111, pp. 2-3).)
Finally, to the extent Dr. Callaghan cites various other symptoms as confounding
of a small fiber neuropathy diagnosis, this is also not persuasive. At least some of the
other symptoms are compatible with her Sjӧgren’s syndrome. (Raphaèle Seror et al.,
EULAR Sjӧgren’s Syndrome Disease Activity Index: Development of a Consensus
Systemic Disease Activity Index for Primary Sjӧgren’s Syndrome, 69 ANNALS RHEUMATIC
DISEASE 1103 (2010) (Ex. G, Tab 2) (identifying fatigue and mild cognitive dysfunction
as potential features of Sjӧgren’s syndrome with neurologic manifestations);
Margaretten, supra, at Ex. G, Tab 4.) And, as Dr. Lightfoot stressed, petitioner’s
constellation of other symptoms is largely subjective. (Ex. C, p. 4.) In any event, the
fact that the small fiber neuropathy does not explain petitioner’s entire constellation of
symptoms does not necessary suggest it is not present. Petitioner was diagnosed as
having small fiber neuropathy by several treating physicians who were all aware of her
overall constellation of symptoms. (Ex. 8, pp. 6-7 (Dr. Kapur); Ex. 41, pp. 3-4 (Dr.
Brannagan); Ex. 102, pp. 12 (Dr. Suresh); Ex. 103, p. 20 (Dr. Lee); Ex. 154, p. 6 (Dr.
Vukic).) In fact, to the extent some of these symptoms could be the result of autonomic
dysfunction, one of petitioner’s treating physicians, Dr. Suresh, diagnosed petitioner as
having small fiber neuropathy with autonomic involvement. (Ex. 102, p. 12; see also
Baer & Bhattacharyya, supra, at Ex. G, Tab 1, p. 6 (discussing autonomic symptoms as
occurring in the context of Sjӧgren’s-related small fiber neuropathy); Margaretten,
supra, at Ex. G, Tab 4, p. 5 (discussing autonomic neuropathy as a feature of Sjӧgren’s
syndrome).) Moreover, the fact that there is otherwise preponderant evidence that
petitioner has Sjӧgren’s syndrome with neurologic manifestations further contributes to
this conclusion, given that small fiber neuropathy is known to be associated with that
condition. There is no debate between Drs. Gupta and Matloubian that small fiber
neuropathy, in particular, can be associated with Sjӧgren’s syndrome. (Ex. 104, p. 3;
Ex. 161, p. 1; Ex. G, p. 9.) Respondent’s other rheumatology expert, Dr. Lightfoot,
doubted that petitioner’s anti-SSA antibodies would be associated with CIDP, but did
not address small fiber neuropathy. (Ex. C.)
Accordingly, there is preponderant evidence that petitioner has small fiber
neuropathy as sequela of her Sjӧgren’s syndrome.
iii. There is not preponderant evidence that petitioner suffered CIDP
Throughout the course of her treatment history, petitioner was evaluated on an
outpatient basis by ten different neurologists. On the whole, the neurology evaluations
reflect an evolution in thinking whereby the initial suspicion of CIDP gave way to small
fiber neuropathy related to Sjӧgren’s syndrome as a more likely explanation for
petitioner’s condition. Dr. Brofin first suspected GBS. (Ex. 6, pp. 30, 34.) However, Dr.
Busono subsequently believed petitioner’s condition would constitute CIDP, though by
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the conclusion of his course of treatment with petitioner he felt that diagnosis was in
doubt. (Ex. 7, p. 2.) Thereafter, Dr. Kapur felt the condition was either CIDP or
Sjӧgren’s-related small fiber neuropathy (Ex. 8, p. 6), and Dr. Ma then opined petitioner
had both conditions (Ex. 16, p. 258). However, Dr. Suresh and Dr. Lee (with Dr. Hurst)
then concluded that petitioner had Sjӧgren’s-related small fiber neuropathy without good
evidence of CIDP. (Ex. 102, p. 12; Ex. 103, p. 20.) Throughout this course of
treatment, Dr. Vukic equivocated. He initially diagnosed CIDP, but then doubted the
diagnosis and referred petitioner to a rheumatologist. (Ex. 5, p. 12; Ex. 30, pp. 35-39;
Ex. 154, p. 62.) Thereafter, he concluded petitioner had Sjӧgren’s-related small fiber
neuropathy. (Ex. 154, pp. 52, 57.) However, he would later revert to believing
petitioner’s symptomatology was consistent with CIDP. (Id. at 46.) Dr. Dover
subsequently treated petitioner on the basis that her CIDP diagnosis was previously
established and, finally, Dr. Sylvester indicated petitioner’s diagnosis was yet to be
confirmed. (Exs. 153, p. 3; Ex. 160, p. 95.)
Petitioner’s own expert, Dr. Souayah, agrees that petitioner did not meet the
diagnostic criteria for CIDP, that her later neurophysiological evaluations did not fit
CIDP, and that her diagnosis changed from CIDP to small fiber neuropathy. (Ex. 111,
p. 3; Ex. 150, pp. 1-2.) Citing Dr. Souayah’s opinion, petitioner argues that the change
in diagnosis reflects that petitioner’s condition evolved in itself (ECF No. 152, p. 90);
however, based on my review of the medical records, the change in diagnosis more
likely reflects continued reassessment based on accumulating evidence. I disagree with
Dr. Souayah’s implicit assertion that the later medical assessments should not be
weighed against the earlier treatment records in considering the correct diagnosis.
Accordingly, while some of petitioner’s treating neurologists did opine that petitioner
suffered CIDP, the evidence, considered as a whole, does not preponderate in favor of
a diagnosis of CIDP.
Several features of petitioner’s clinical history cited by Dr. Souayah as indicative
of CIDP do not actually provide a clear-cut distinction, especially when considering that
Dr. Souayah readily admits that petitioner does not meet the criteria for a “classic” form
of CIDP and instead opines that petitioner suffered a sensory-predominant form of the
condition characterized by paresthesia and gait dysfunction. (Ex. 111, p. 2; Ex. 42, pp.
18-19.) Specifically, Dr. Souayah cites numbness starting in petitioner’s hands and
progressing to her feet three days later as indicative of CIDP. (Ex. 42, pp. 18-19.)
What petitioner first reported was tingling and numbness. (Ex. 2, p. 5; Ex. 6, p. 4.)
Thus, when petitioner first presented for her condition, her symptoms were felt to be
indicative of peripheral neuropathy. (Ex. 2, p. 16.) Regardless of whether numbness
can also be seen in CIDP, sensation loss (specifically pin prick and thermal), as well as
tingling or pins and needles, are consistent with small fiber neuropathy. (Devigili et al.,
supra, at Ex. F, Tab 1, pp. 2, 5 tbls.1 & 2; Birnbaum et al., supra, at Ex. 109, pp. 5-7
tbl.2.) Symptoms beginning in petitioner’s hands then progressing to her feet is atypical
for either CIDP or small fiber neuropathy; however, the overall pattern of symptoms is
consistent with small fiber neuropathy. (Birnbaum et al., supra, at Ex. 109, p. 9.) Dr.
Souayah also stresses petitioner’s unsteady gait and reduced reflexes (absent at the
ankles), positive Romberg, and abnormal vibration sensation. (Ex. 42, pp. 18-19.)
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Again, however, as discussed in the preceding section, this may be consistent with a
“mixed” small fiber neuropathy as specifically seen in Sjӧgren’s syndrome. (Birnbaum
et al., supra, at Ex. 109, p 4; see also Margaretten, supra, at Ex. G, Tab 4, p. 2 (noting
that small fiber neuropathy in Sjӧgren’s syndrome may have “concomitant large fiber
neuropathy”).) Thus, for example, one study that Dr. Souayah cites as demonstrating
the concept of a sensory-variant of CIDP specifically excluded Sjӧgren’s syndrome
patients from its study. (Ayrignac et al., supra, at Ex. 47, p. 1.)
Perhaps the most challenging aspect of petitioner’s history is her initial
electrodiagnostic finding of evidence of demyelination (Ex. 6, p. 1), followed by several
subsequent EMG/NCS tests that were entirely negative for demyelination (Ex. 7, pp. 9-
10; Ex. 5, p. 19; Ex. 24, pp. 10-11). Dr. Souayah finds significance in the first
electrodiagnostic test (Ex. 111, p. 2) and views the later evaluations as indicating of a
change in petitioner’s condition over time, leading to the subsequent small fiber
neuropathy diagnosis (Id. at 3). Dr. Callaghan, however, views the electrodiagnostic
studies collectively and opines that the later normal studies point away from CIDP or
any peripheral nervous system pathology. (Ex. A, p. 3.) He opines that the
electrodiagnostic evidence taken as a whole indicates that petitioner never had large
fiber involvement. (Ex. F, p. 4.) While petitioner’s first electrodiagnostic study does
cloud her overall clinical picture, I ultimately find Dr. Callaghan more persuasive in
assessing the electrodiagnostic studies holistically. Based on my review of Dr.
Souayah’s reports, he does not reconcile the change in petitioner’s electrodiagnostic
findings (from which he seemingly implies resolution of demyelination) with petitioner’s
subsequent prolonged clinical course.
Another puzzling aspect of petitioner’s history is her persistent symptom of
weakness that, as Dr. Callaghan stressed, consistently lacked any corresponding
finding of significant weakness upon neurologic exam. (Ex. A, p. 3). Dr. Souayah’s
proposed CIDP diagnosis does not neatly resolve this issue, however, because Dr.
Souayah agrees that petitioner’s lack of progressive, symmetric, proximal weakness
points to a sensory form of CIDP rather than “classic” CIDP. (Ex. 111, pp. 1-2.) In that
regard, the literature filed by respondent reflects that primary Sjӧgren’s syndrome can
manifest with weakness as a feature of rheumatic disease, rather than as a neurologic
manifestation of the condition. (Margaretten, supra, at Ex. G, Tab 4, p. 7.)
Finally, the experts disagree regarding the significance, if any, of petitioner’s
response to IVIG and plasmapheresis, as well as the apparent relapsing nature of
petitioner’s condition. However, this aspect of petitioner’s history does not clearly favor
any particular diagnosis. Petitioner’s records are inconsistent with respect to whether
her condition responded to treatment. Although the records reflect that petitioner
responded well to treatment in some instances on a short-term basis, the records
otherwise reflect dissatisfaction with petitioner’s response to treatment over the longer
course. And, although petitioner reported variations in her symptom presentation over
time, she appears to have remained continuously symptomatic, and I do not see where
her symptoms ever had a relapsing/remitting pattern. This aspect of petitioner’s history
is difficult to assess because many of her symptoms were subjective and some doubt
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was expressed by her treating physicians regarding some of her reported relapses. For
example, during her June 2019 hospitalization, Dr. Sonbol felt that, upon neurologic
examination, some of petitioner’s symptoms may have been non-physiologic. (Ex. 101,
p. 29.) In that regard, Dr. Lightfoot’s assertion that petitioner may have been
susceptible to a placebo effect is not entirely unreasonable. (Ex. C, p. 4.) There was
also some suspicion that the acute shortness of breath petitioner experienced may have
been panic attacks. (Ex. 101, p. 9.) Later, when petitioner reported to Dr. Dover that
she was experiencing worsening of symptoms, Dr. Dover pressed for clarification and
elicited that petitioner was suffering only an increase in fatigue, which is fairly non-
specific. (Ex. 153, p. 2)
Considering all of the above, there is not preponderant evidence that petitioner
suffered CIDP.
b. Medical theory of causation (Althen prong one)
Under Althen prong one, petitioner must provide a “reputable medical theory,”
demonstrating that the vaccine received can cause the type of injury alleged. Pafford v.
Sec’y of Health & Human Servs., 451 F.3d 1352, 1355-56 (Fed. Cir. 2006) (quoting
Pafford v. Sec’y of Health & Human Servs., No. 01-0165V, 2004 WL 1717359, at *4
(Fed. Cl. Spec. Mstr. July 16, 2004)). Such a theory must only be “legally probable, not
medically or scientifically certain.” Knudsen, 35 F.3d at 548-49. Petitioner may satisfy
the first Althen prong without resort to medical literature, epidemiological studies,
demonstration of a specific mechanism, or a generally accepted medical theory. See
Andreu, 569 F.3d at 1378-79 (citing Capizzano v. Sec’y of Health & Human Servs., 440
F.3d 1317, 1325-26 (Fed. Cir. 2006)). However, “[a] petitioner must provide a
‘reputable medical or scientific explanation’ for [her] theory. While it does not require
medical or scientific certainty, it must still be ‘sound and reliable.’” Boatmon, 941 F.3d
at 1359 (quoting Moberly ex rel. Moberly v. Sec’y of Health & Human Servs., 592 F.3d
1315, 1322 (Fed. Cir. 2010); Knudsen, 35 F.3d at 548-49).
As explained above, petitioner’s theory of causation is largely predicated on the
notion that CIPD can be vaccine-caused in the same manner as GBS. Thus, my finding
that petitioner did not suffer CIDP dramatically undercuts petitioner’s claim, leaving her
with virtually no remaining theory of causation.24 “Because causation is relative to the
injury, a petitioner must provide a reputable medical or scientific explanation that
pertains specifically to the petitioner’s case, although the explanation need only be
‘legally probable, not medically or scientifically certain.’” Broekelschen, 618 F.3d at
1345 (quoting Knudsen, 35 F.3d at 548-49). Absent the link Dr. Souayah posited
between CIDP and the flu vaccine, petitioner’s experts offer nothing more than a vague
24 Although I do not find it necessary to reach the question of whether the flu vaccine can cause CIDP, it
is worth noting that prior cases in which petitioners have alleged that the flu vaccine-caused CIDP have
led to mixed results. See, e.g., Nieves v. Sec’y of Health & Human Servs., No. 18-1602V, 2023 WL
3580148, at *36 (Fed. Cl. Spec. Mstr. May 22, 2023) (explaining the history of CIDP cases in the
program).
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reference to the “mosaic of autoimmunity” and a general “loss of immunological
tolerance” to support vaccine causation.
However, without more, reliance on an unspecified autoimmune process fails on
a fundamental level. There are various pathways to autoimmunity and many
autoimmune conditions have little to no suspicion of vaccine causation. E.g., Kelly v.
Sec’y of Health & Human Servs., No. 16-1548V, 2023 WL 3274159, at *9 (Fed. Cl.
Spec. Mstr. May 5, 2023) (explaining that “[t]here is little debate that myasthenia gravis
is an autoimmune neuromuscular disorder and there is little debate that molecular
mimicry is, in general, a viable theory of autoimmunity that can in at least some contexts
implicate vaccination. Importantly, however, these predicates are not enough to meet
petitioner’s burden of proof.”); Casazza v. Sec’y of Health & Human Servs., No. 17-
947V, 2023 WL 6214984, at *10 (Fed. Cl. Spec. Mstr. Aug 30, 2023) (explaining “there
is no dispute that [rheumatoid arthritis] is an autoimmune condition of uncertain cause”
and that [v]ery little on this record apart from Dr. Gershwin’s say-so associates any
vaccine with [rheumatoid arthritis] whereas much more purports to refute Dr. Gershwin’s
opinion”). Thus, it is not enough, as Dr. Gupta implies, to simply rely on the fact that
Sjӧgren’s syndrome, CIDP, and small fiber neuropathy are all autoimmune conditions.
(Ex. 151.) Simply, it is too vague to preponderantly support a theory of causation.
Accord J.F. v. Sec’y of Health & Human Servs., No. 13-799V, 2022 WL 5434214, at *32
(Fed. Cl. Spec. Mstr. Sept. 9, 2022) (finding that “petitioner is not persuasive in
identifying ASIA as a sound and reliable means of identifying the presence of an
autoimmune injury in those who are not suffering a defined autoimmune condition.
Given that petitioner did not suffer any recognized autoimmune condition, this is fatal to
petitioner's Althen prong one showing.”); Kinney v. Sec’y of Health & Human Servs., No.
18-1522V, 2024 WL 2831616, at *18 (Fed. Cl. Spec. Mstr. May 8, 2024) (explaining that
“[t]he fact that a person may be prone to autoimmunity or experience multiple
autoimmune conditions does not automatically lead to the conclusion that the one
autoimmune condition is causally related to the other(s)” and rejecting as speculative
the expert’s premise that “the presence of one autoimmune condition in itself simply
raises a suspicion that the same autoimmune process also explains any other condition
or symptoms petitioner may have”). For example, prior cases have explained with
respect to molecular mimicry, as cited by Dr. Souayah, that it “is a generally accepted
scientific principle, [but] mere invocation of the scientific term does not carry a
petitioner’s burden in a Program case.” Deshler v. Sec’y of Health & Human Servs., No.
16-1070V, 2020 WL 4593162, at *20 (Fed. Cl. Spec. Mstr. July 1, 2020) (citing Forrest
v. Sec’y of Health & Human Servs., No. 14-1046V, 2019 WL 925495, at *3 (Fed. Cl.
Spec. Mstr. Jan. 18, 2019)). Ultimately, nothing requires the acceptance of an expert’s
conclusion “connected to existing data only by the ipse dixit of the expert,” especially if
“there is simply too great an analytical gap between the data and the opinion proffered.”
Snyder ex rel. Snyder v. Sec’y of Health & Human Servs., 88 Fed. Cl. 706, 743 (2009)
(quoting Gen. Elec. Co. v. Joiner, 522 U.S. 136, 146 (1997)); see also Isaac v. Sec’y of
Health & Human Servs., No. 08-601V, 2012 WL 3609993, at *17 (Fed. Cl. Spec. Mstr.
July 30, 2012), aff’d, 108 Fed. Cl. 743 (2013), aff’d, 540 F. App’x 999 (Fed. Cir. 2013).
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Here, neither Dr. Souayah nor Dr. Gupta provided any explanation or
substantiation of a causal theory for Sjӧgren’s syndrome and/or small fiber neuropathy.
Moreover, Dr. Matloubian is persuasive in explaining that Dr. Souayah’s attempt to rely
generically on a loss of immune tolerance is not persuasive in the context of Sjӧgren’s
syndrome. (Ex. G, p. 11.) Dr. Matloubian explains that, while autoimmune, the
underlying cause of Sjӧgren’s syndrome is unknown and not associated with infectious
triggers. (Id.) Dr. Callaghan is also persuasive in observing that Dr. Souayah did not
substantiate that mechanisms such as molecular mimicry or bystander activation
implicate the flu vaccine as a cause of small fiber neuropathy. (Ex. E, p. 3.) Although
CIDP, small fiber neuropathy, and GBS are all peripheral neuropathies, they cannot
simply be conflated, and the cause of one does not imply a cause of the others, absent
some substantiation. See, e.g. McGill v. Sec’y of Health & Human Servs., No. 15-
1485V, 2023 WL 3813524, at *26 (Fed. Cl. Spec. Mstr. May 11, 2023) (explaining that
“[w]hile Dr. Tornatore is correct that there is some overlap between GBS and [small
fiber neuropathy], he is not persuasive in equating the causes of GBS to the causes of
[small fiber neuropathy]. In contrast to GBS, [small fiber neuropathy] is generally
considered to be caused by underlying systemic conditions, including autoimmune
conditions, diabetes, and toxic causes. Only a subset of idiopathic [small fiber
neuropathy] cases is suspected to result from tissue-specific dysimmunity in a manner
that could potentially be compared to GBS.” (internal citation omitted)).
Accordingly, petitioner has not met her burden of proof under Althen prong one.
c. Logical sequence of cause and effect (Althen prong two)
The second Althen prong requires proof of a logical sequence of cause and
effect, usually supported by facts derived from a petitioner’s medical records. Althen,
418 F.3d at 1278; Andreu, 569 F.3d at 1375-77; Capizzano, 440 F.3d at 1326-27;
Grant, 956 F.2d at 1147-48. Medical records are generally viewed as particularly
trustworthy evidence. Cucuras, 993 F.2d at 1528. However, medical records and/or
statements of a treating physician’s views do not per se bind the special master. See
§ 300aa-13(b)(1) (providing that “[a]ny such diagnosis, conclusion, judgment, test result,
report, or summary shall not be binding on the special master or court”); Snyder, 88
Fed. Cl. at 745 n.67 (2009) (“[T]here is nothing . . . that mandates that the testimony of
a treating physician is sacrosanct—that it must be accepted in its entirety and cannot be
rebutted.”). A petitioner may support a cause-in-fact claim through either medical
records or expert medical opinion. § 300aa-13(a). The special master is required to
consider all the relevant evidence of record, draw plausible inferences, and articulate a
rational basis for the decision. Winkler v. Sec’y of Health & Human Servs., 88 F.4th
958, 963 (Fed. Cir. 2023) (citing Hines, 940 F.2d at 1528).
There are three issues that warrant attention under Althen prong two. First,
respondent contends that to the extent the evidence preponderantly establishes that
petitioner suffers small fiber neuropathy, then that small fiber neuropathy should be
attributed to her Sjӧgren’s syndrome, rather than her vaccination. Second, petitioner’s
treating physicians did not otherwise support the notion that her Sjӧgren’s syndrome
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and small fiber neuropathy were causally related to her vaccination. Third, respondent
further contends that petitioner’s Sjӧgren’s syndrome predated the vaccination at issue.
If petitioner’s condition developed prior to vaccination, then logically it could not have
been caused by that vaccine. E.g., L.Z. v. Sec’y of Health & Human Servs., No. 14-
920V, 2018 WL 5784525, at *18 (Fed. Cl. Spec. Mstr. Aug. 24, 2018) (explaining that
“[p]etitioner’s direct causation claim cannot succeed, as she cannot demonstrate a
vaccine ‘caused’ an illness predating vaccination”).
Both Dr. Matloubian and Dr. Gupta explain that small fiber neuropathy may be a
feature of Sjӧgren’s syndrome. (Ex. 104, p. 3 (citing Birnbaum et al., supra, at Ex. 109);
Ex. G, pp. 7-8.) And, importantly, the medical literature filed in this case supports the
proposition that peripheral neuropathies in Sjӧgren’s syndrome, such as small fiber
neuropathy (or CIDP25), are causally-related manifestations of the Sjӧgren’s syndrome
and not merely comorbidities. (Mori et al., supra, at Ex. 108; Birnbaum et al., supra, at
Ex. 109; Margaretten, supra, at Ex. G, Tab 4.) Thus, with respect to petitioner herself,
Dr. Gupta opines that “it is more likely than not that the SSA antibodies and Sjogren’s
Syndrome were associated with the neuropathy in her case.” (Ex. 104, p. 4.) And,
while Dr. Gupta nonetheless opined that this would remain compatible with a “mosaic of
autoimmunity,” that opinion is not substantiated for the reasons discussed under Althen
prong one, above. Neither Dr. Gupta nor Dr. Souayah have presented a theory of
causation directly implicating petitioner’s vaccination as a cause of Sjӧgren’s syndrome.
Accordingly, the fact that petitioner’s small fiber neuropathy is a result of her Sjӧgren’s
syndrome means there is no logical sequence of cause and effect connecting her
vaccination to her small fiber neuropathy. Winkler, 88 F.4th at 963 (quoting Stone v.
Sec’y of Health & Human Servs., 676 F.3d 1373, 1379 (Fed. Cir. 2012), for the
proposition that “evidence of other possible sources of injury can be relevant . . . to
whether a prima facie showing has been made that the vaccine was a substantial factor
in causing the injury in question” (emphasis omitted)); see also McGill, 2023 WL
3813524, at *31-33 (finding that petitioner’s small fiber neuropathy was more likely
related to preexisting rheumatoid arthritis than to the subject vaccinations).
Notably, petitioner’s medical records reflect a very long history of evaluation
directed at finding a workable diagnosis for petitioner’s condition. Throughout that
process, petitioner repeatedly presented her post-vaccination onset of symptoms as a
pertinent part of her history. However, despite extensive consideration regarding the
underlying cause of petitioner’s condition, only one of her treating physicians, Dr. Vukic,
opined that petitioner’s condition was vaccine-caused. (Ex. 154, p. 46.) There are
several reasons why Dr. Vukic’s opinion is not strong evidence supporting petitioner’s
claim. As an initial matter, the basis for Dr. Vukic’s opinion is not well explained and it
appears that it is merely reflective of the fact that petitioner’s symptoms arose post-
vaccination. However, the Federal Circuit has explained that “[a]lthough probative,
neither a mere showing of a proximate temporal relationship between vaccination and
25 Because both the medical literature and expert opinions support CIDP as among the potential
neurologic sequela of Sjӧgren’s syndrome, the presence of Sjogren’s syndrome would pose a significant
issue with respect to Althen prong two, even if I had concluded that petitioner did suffer CIDP and even if
I had concluded that CIDP can in some instances be caused by the flu vaccine.
34

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injury, nor a simplistic elimination of other potential causes of the injury suffices, without
more, to meet the burden of showing actual causation.” Althen, 418 F.3d at 1278 (citing
Grant, 956 F.2d at 1149). Thus, “[a] treating physician’s recognition of a temporal
relationship does not advance the analysis of causation.” Isaac, 2012 WL 3609993, at
*26. Moreover, to the extent Dr. Vukic’s opinion does include anything beyond post hoc
ergo propter hoc reasoning, his opinion appears to have been predicated on his
unwillingness to abandon the prior CIDP diagnosis, even after petitioner’s Sjӧgren’s
syndrome and small fiber neuropathy were diagnosed. (Ex. 154, p. 46.) However, Dr.
Vukic’s determination to maintain the CIDP diagnosis does not appear to be reliable,
given that he had referred petitioner for rheumatologic evaluation precisely because he
had already doubted the CIDP diagnosis. (Id. at 62.) Indeed, Dr. Vukic’s subsequent
records confirm that his diagnostic assessment continued to be equivocal. (Compare
id. at 6 (indicating symptoms due to small fiber neuropathy related to rheumatologic
condition), with Ex. 155, p. 20 (indicating symptomatology consistent with CIDP).) And,
in any event, petitioner was evaluated by numerous other specialists, neurologists and
rheumatologists, who did not express any similar opinion, leaving Dr. Vukic as an outlier
among petitioner’s treating physicians.
Finally, in opining that petitioner suffered Sjӧgren’s syndrome, Dr. Gupta
specifically highlighted that among the potentially diagnostic aspects of her history,
petitioner had a history of “prednisone responsive inflammatory hand arthritis.” (Ex.
104, p. 4.) This had been reported by petitioner as part of her prior, pre-vaccination
history when she first presented for a rheumatologic evaluation and was considered a
potential feature of Sjӧgren’s syndrome. (Ex. 2, p. 135.) Given this, Dr. Matloubian
opined that petitioner’s Sjӧgren’s syndrome pre-dated her vaccination. Specifically, Dr.
Matloubian agreed that petitioner’s arthritis is consistent with Sjӧgren’s syndrome
because inflammatory arthritis (as opposed to osteoarthritis) would present with joint
swelling and would be more likely to affect the MCP joints. (Ex. G, p. 9; see also Seror
et al., supra, at Ex. G, Tab 2, p. 4.) Dr. Gupta contended that Dr. Matloubian
“overstates” his opinion. He notes that his review of petitioner’s clinical history was
equivocal in explaining that petitioner “may” have inflammatory arthritis. (Ex. 161, p. 1.)
However, while Dr. Gupta may have been more measured in his recitation of petitioner’s
history, he was unambiguous in his ultimate conclusion that petitioner had inflammatory
arthritis as one of “several other features consistent with [Sjӧgren’s syndrome].” (Ex.
104, p. 4.) Accordingly, I agree with Dr. Matloubian’s interpretation that Dr. Gupta’s
assessment effectively places petitioner’s Sjӧgren’s syndrome pre-vaccination.
Dr. Matloubian further notes that petitioner was never tested for anti-SSA
antibodies prior to vaccination, so it is unknown (and entirely possible) that these
antibodies were present prior to vaccination and dating as far back as her arthritis. (Ex.
G, p. 9.) Dr. Gupta disagrees, stressing petitioner’s prior negative ANA. (Ex. 161, p. 2
(citing Ex. 21, p. 21).) However, the Sjӧgren’s syndrome literature filed by respondent
indicates that “ANA should not be used as a screening test for [Sjӧgren’s syndrome] or
[Sjӧgren’s syndrome]-related antibodies, since some patients may have anti-Ro/SSA
and/or anti-La/SSB antibodies despite a negative immunofluorescence assay for ANA.”
(Baer & Bhattacharyya, supra, at Ex. G, Tab 1, p. 10.) Dr. Gupta asserts that when an
35

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ANA panel undergoes cascade testing, a negative ANA result would usually also
indicate a negative SSA result. (Ex. 161, p. 2.) Dr. Matloubian points out, however, that
the record of petitioner’s 2012 ANA result is inadequate to determine what method of
testing was used. (Ex. G, p. 10.) Given all of this, the evidence preponderates in favor
of a finding that petitioner’s Sjӧgren’s syndrome likely predated her vaccination based
on her prior history of inflammatory arthritis, which her own expert opines is consistent
with her diagnosed Sjӧgren’s syndrome.
For all these reasons, petitioner has not met her burden of proof under Althen
prong two.
d. Proximate temporal relationship between vaccination and significant
aggravation (Althen prong three)
The third Althen prong requires establishing a “proximate temporal relationship”
between the vaccination and the injury alleged. Althen, 418 F.3d at 1278. A petitioner
must offer “preponderant proof that the onset of symptoms occurred within a timeframe
for which, given the medical understanding of the disorders etiology, it is medically
acceptable to infer causation-in-fact.” de Bazan v. Sec’y of Health & Human Servs.,
539 F.3d 1347, 1352 (Fed. Cir. 2008). The explanation for what is a medically
acceptable timeframe must coincide with the theory of how the relevant vaccine can
cause an injury (Althen prong one’s requirement). Id.; Shapiro v. Sec’y of Health &
Human Servs., 101 Fed. Cl. 532, 542 (2011), mot. for recons. den’d after remand, 105
Fed. Cl. 353 (2012), aff’d, 503 F. App’x 952 (Fed. Cir. 2013); Koehn v. Sec’y of Health &
Human Servs., No. 11-355V, 2013 WL 3214877, at *26 (Fed. Cl. Spec. Mstr. May 30,
2013), aff’d, 773 F.3d 1239 (Fed. Cir. 2014).
Because petitioner’s condition predated her vaccination, there is no temporal
association between her vaccination and her injury as petitioner asserts. However,
even assuming that petitioner satisfied Althen prong three based on her preferred timing
of onset, that alone would not satisfy petitioner’s overall burden of proof. Veryzer v.
Sec’y of Health & Human Servs., 100 Fed. Cl. 344, 356 (2011) (explaining that a
“temporal relationship alone will not demonstrate the requisite causal link and that
petitioner must posit a medical theory causally connecting the vaccine and injury”);
Hibbard v. Sec’y of Health & Human Servs., 698 F.3d 1355, 1364-65 (Fed. Cir. 2012)
(holding the special master did not err in resolving the case pursuant to prong two when
respondent conceded that petitioner met prong three).
VI. Conclusion
Petitioner has clearly suffered much over the course of a number of years. She
has my sympathy and nothing in this decision is intended to minimize what she has
experienced. However, for all the reasons discussed above, I cannot conclude that
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there is preponderant evidence causally linking petitioner’s vaccination to her condition.
Accordingly, this case is dismissed.26
IT IS SO ORDERED.
s/Daniel T. Horner
Daniel T. Horner
Special Master
26 In the absence of a timely-filed motion for review of this Decision, the Clerk of the Court shall enter
judgment accordingly.
37

================================================================================
DOCUMENT 2: USCOURTS-cofc-1_17-vv-01915-2
Date issued/filed: 2025-04-02
Pages: 10
Docket text: JUDGE VACCINE REPORTED OPINION & ORDER (PUBLIC VERSION) denying 160 Petitioner's Motion for Review. Signed by Senior Judge Loren A. Smith. (ajd) Service on parties made.
--------------------------------------------------------------------------------
Case 1:17-vv-01915-LAS Document 174 Filed 04/02/25 Page 1 of 10
In the United States Court of Federal Claims
No. 17-1915V
(Filed Under Seal: March 18, 2025)1
Reissued: April 2, 2025
)
ANGELA APUZZO, )
)
Petitioner, )
)
v. )
)
SECRETARY OF HEALTH AND )
HUMAN SERVICES, )
)
Respondent. )
)
OPINION & ORDER
Meredith Daniels, Conway Homer, P.C., Boston, MA, for petitioner. Also represented
by Ronald Craig Homer.
Debra A. Filteau Begley, Vaccine/Torts Branch, Civil Division, United States
Department of Justice, Washington, D.C., for respondent.
SMITH, Senior Judge
This case concerns how the Office of Special Masters at the United States Court
of Federal Claims must evaluate competing expert opinions in vaccine injury cases.
Special Master Daniel T. Horner denied compensation to petitioner, Ms. Angela
Apuzzo, because he concluded—after reviewing the respective expert reports submitted
by both respondent, the Secretary of Health and Human Services, and Ms. Apuzzo—that
she suffers from Sjögren’s Syndrome, rather than her alleged acute-onset chronic
inflammatory demyelinating polyneuropathy (“CIDP”), caused by an influenza
vaccination on September 17, 2015. See generally Apuzzo v. Sec’y of Health & Hum.
Servs., No. 17-1915V, 2024 WL 4534200 (Off. Spec. Mstr. Sept. 20, 2024). To Ms.
Apuzzo, the Special Master’s conclusion violates binding precedent instructing special
masters not to “conduct a differential diagnosis” by choosing one expert’s opinion over
another, “or over a combination of” expert and treating physicians’ opinions. See
generally Petitioner’s Memorandum in Support of Her Motion for Review the Special
Master’s September 20, 2024, Decision, ECF No. 166 [hereinafter Pet’r’s Mot.].
1 This opinion was issued under seal on March 18, 2025. The parties were given an opportunity to propose
redactions before public release, but no such proposals were made.

Case 1:17-vv-01915-LAS Document 174 Filed 04/02/25 Page 2 of 10
The Court disagrees. Special Master Horner was required to evaluate the
reliability of the parties’ expert reports because, in contrast to respondent’s experts,
neither Ms. Apuzzo’s treating physicians nor her experts agreed on the proper diagnosis
for her symptoms. See, e.g., Pafford v. Sec’y of Health & Hum. Servs., 451 F.3d 1352,
1356 (Fed. Cir. 2006) (holding that it is not arbitrary and capricious for a special master
to conclude that a claimant did not prove causation by reviewing and comparing the
expert evidentiary record); Lombardi v. Sec’y of Health & Hum. Servs., 656 F.3d 1343,
1353–54 (Fed. Cir. 2011) (same). The Special Master’s decision is therefore affirmed.
I
On September 17, 2015, Ms. Apuzzo received the influenza vaccination at issue.
Apuzzo, 2024 WL 4534200, at *4. On October 5, 2015, Ms. Apuzzo was reviewed by
emergency health professionals after she complained of four days of numbness and
tingling in her hands, feet, and the right side of her face. Id. The emergency health
professionals “suspected” hypothyroidism but suggested that she follow up with a
neurologist due to her mild peripheral neuropathy. Id. On October 28, 2015, Ms.
Apuzzo met with Dr. Bronfin,2 a neurologist. Id. “Dr. Bronfin diagnosed Guillain-
Barré Syndrome . . . and peripheral demyelinating neuropathy.” Id. (acronym omitted).
That same day, based on Dr. Bronfin’s diagnosis, Ms. Apuzzo returned to the
emergency health professionals and was transferred to inpatient neurologic observation
at a hospital. Id. During her hospitalization, Ms. Apuzzo’s blood test results “were
significant for positive antinuclear antibodies . . . and elevated anti-Sjögren's syndrome-
related antigen A antibodies,” but no tests definitively determined that she suffered
from Guillain-Barré Syndrome. Id. Ms. Apuzzo then had a rheumatological
consultation to address possible Sjögren's Syndrome. Id. “Given her history of arthritis
and positive Sjögren's Syndrome antibodies, as well as the fact [Guillain-Barré
Syndrome] was not definitively diagnosed, rheumatology considered Sjögren's
[S]yndrome as a possible explanation for petitioner's peripheral neuropathy and
recommended continuing to treat for [Guillain-Barré Syndrome] while monitoring for
Sjögren's [S]yndrome.” Id. The consultant recommended that Ms. Apuzzo follow-up to
determine if Sjögren's Syndrome was main cause of her symptoms. Id. On November
3, 2015, Ms. Apuzzo was discharged from the hospital with a diagnosis of Guillain-
Barré Syndrome and peripheral demyelinating neuropathy. Id.
On November 17, 2025, Ms. Apuzzo returned to Dr. Bronfin because she was
still experiencing numbness, tingling, and a tremor. Id. at *5. After reviewing Ms.
Apuzzo, “Dr. Bronfin maintained his diagnoses of [Guillain-Barré Syndrome] and
peripheral demyelinating neuropathy, but also added Sjögren's [S]yndrome to his
assessment.” Id. Dr. Bronfin then prescribed a series of treatments that tended to cause
improvements in Ms. Apuzzo’s condition. Id.
2 Special Master Horner’s decision only uses last names for certain physicians. Where a first name is used,
the Court does so as well.
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Case 1:17-vv-01915-LAS Document 174 Filed 04/02/25 Page 3 of 10
On January 19, 2016, Ms. Apuzzo was evaluated by a rheumatologist, Dr. Lee.
Id. Finding Ms. Apuzzo to be positive for Sjögren's Syndrome antibodies, Dr. Lee
determined that her condition could be presented with peripheral neuropathy, but
decided to wait on performing more tests to confirm this diagnosis, given Ms. Apuzzo’s
apparent improvement in response to Dr. Bronfin’s treatment plan. Id. Ms. Apuzzo
was to contact Dr. Lee again if her condition stopped improving or became worse. Id.
On February 1, 2016, Ms. Apuzzo returned to Dr. Bronfin, complaining of
increased weakness and shortness of breath. Id. He found that Ms. Apuzzo was
neurologically stable but refered her to emergency health services due to her shortness
of breath. Id. The hospital conducted a series of tests, which ruled out Guillain-Barré
Syndrome, and now offered CIDP as a possible cause for Ms. Apuzzo’s symptoms. Id.
On March 8, 2016, Ms. Apuzzo once again returned to Dr. Bronfin due to her condition
“not improving,” and Ms. Apuzzo continued her treatment plan under Dr. Bronfin’s
unchanged diagnosis of Sjögren's Syndrome, Guillain-Barré Syndrome, and peripheral
demyelinating neuropathy. Id. (internal quotation marks omitted).
Between March 21, 2016, and August 22, 2017, Ms. Apuzzo saw at least four
different specialists. Id. at *6–7. On March 21, 2016, Ms. Apuzzo visited Dr. Busono,
a neuromuscular specialist, who, after diagnostic testing, began to “doubt the diagnosis
of CIDP,” and Dr. Bronfin’s treatment plan was discontinued as a result. Id. at *6
(internal quotation marks omitted). In August of 2016, Ms. Apuzzo consulted Dr.
Kapur, a neurologist, who restarted Dr. Bronfin’s treatment with additional treatments
prescribed, and Ms. Apuzzo was to return to Dr. Kapur once he received her medical
records. Id. On October 4, 2016, Ms. Apuzzo visited Dr. Kapur for a second time. Id.
During the visit, Dr. Kapur noted that Ms. Apuzzo still had Sjögren's Syndrome
antibodies, so her symptoms “could be consistent with either CIDP or small fiber
neuropathy related to Sjögren's [S]yndrome,” and recommended that Ms. Apuzzo
continue her already prescribed treatment plan. Id. On February 3, 2017, Ms. Apuzzo
met with another neurologist, Dr. Vukic, who ordered a series of examinations. Id.
After this series of examinations in February of 2017, Dr. Vukic “maintained” the
CIDP diagnosis. Id. On August 22, 2017, Ms. Apuzzo saw a different neurologist, Dr.
Ma, who determined that her symptoms might be associated with either CIDP, Sjögren's
Syndrome, or hypothyroidism. Id. at *7.
From September 22 to 25 to October 2 to 8, 2017, Ms. Apuzzo twice visited a
hospital for worsening weakness, fatigue, and shortness of breath. Id. The hospital’s
neurological “impression” believed her to be suffering from CIDP and Sjögren's
Syndrome. Id. After these hospital visits, she returned to Dr. Vukic and a
neuromuscular specialist, Dr. Brannagan multiple times, where her treatment plan
changed repeatedly from late 2017 until spring of 2018. Id.
On April 13, 2018, Ms. Apuzzo visited Dr. Brannagan again. Id. Dr. Brannagan,
in consultation with Dr. Vukic, concluded that her symptoms were not consistent with
CIDP and therefore recommended a skin biopsy for Sjögren's Syndrome. Id. (“Dr.
Vukic then noted that Dr. Brannagan does not believe petitioner has CIDP and therefore
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Case 1:17-vv-01915-LAS Document 174 Filed 04/02/25 Page 4 of 10
concluded that [t]he cause of her symptoms remains elusive.” (internal quotation marks
omitted)). On April 30, 2018, Ms. Apuzzo had a skin biopsy for Sjögren's Syndrome.
Id. at *8. On August 2, 2018, a rheumatologist, Dr. Kepecs, diagnosed Ms. Apuzzo
with, at least, Sjögren's Syndrome based on review of her medical record, biopsy
results, and a family history of autoimmune issues. Id. Dr. Kepecs put Ms. Apuzzo on
an autoimmune treatment plan. Id.
On October 15, 2018, Ms. Apuzzo was again admitted to the hospital, where
hospital staff treated her for assumed CIDP issues. Id. Dr. Vukic was informed of Ms.
Apuzzo’s hospital visit and considered her condition “elusive.” Id. (internal quotation
marks omitted). On December 11, 2018, Dr. Vukic remarked that he believed her
condition was a “direct result of her prior [influenza] immunization.” Id. (internal
quotation marks omitted).
On June 30, 2019, after moving to the State of Florida, Ms. Apuzzo visited
emergency health services and informed the staff of her previous diagnoses. Id.
Between July 2019, and February 2020, Ms. Apuzzo visited multiple physicians: Dr.
Sonbol; Dr. Suresh; Dr. Lee; and Dr. Hurst. Id. at *8–9. All four physicians treated
Ms. Apuzzo for either CIDP or generalized neuropathy. Id.
On October 22, 2020, Ms. Apuzzo returned to Dr. Vukic. Id. at *9. Based on the
symptoms she had while in Florida, Dr. Vukic determined Ms. Apuzzo to have some
type of small fiber polyneuropathy, and recommend she undergo a series of medical
tests. Id. But these tests resulted in nothing medically “remarkable.” Id. On January
5, 2021, Dr. Vukic recommended treatment for CIDP. Id. Until July 6, 2021, Ms.
Apuzzo’s condition was seemingly improving, but she started to have increased
neurological issues, like memory lapses, so Dr. Vukic ordered more medical tests. Id.
Shortly thereafter, on August 23, 2021, Ms. Apuzzo switched neurologists from Dr.
Vukic to Dr. Dover. Id. at *10. Dr. Dover ordered more medical testing and did not
change Ms. Apuzzo’s medical treatment plan during his examinations of her in
December 2021 and in February 2022. Id. Dr. Dover eventually diagnosed Ms.
Apuzzo with CIDP. Id.
On November 9, 2022, Ms. Apuzzo saw a multiple sclerosis specialist, Dr.
Sylvester, who conduct a neurological exam and was willing to prescribe additional
autoimmunity condition treatments. Id. The record does not state whether these
treatments were ever administered.
II
On December 8, 2017, Ms. Apuzzo filed her petition against respondent, wherein
she claimed that her September 17, 2015, influenza vaccine caused CIDP. See
generally Petitioner’s Petition at 1, ECF No. 1. Ms. Apuzzo made no other vaccine
injury claim. Id. After completing discovery, in June of 2023, the parties moved for a
ruling on the record. Apuzzo, 2024 WL 4534200, at *4. After the briefing completed,
on September 20, 2024, Special Master Horner issued his decision denying entitlement
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Case 1:17-vv-01915-LAS Document 174 Filed 04/02/25 Page 5 of 10
to Ms. Apuzzo because he determined that the record showed that she suffers from
Sjögren's Syndrome, not CIDP, caused by her influenza vaccination on September 17,
2015. See generally id. In making this decision, he reviewed Ms. Apuzzo’s two expert
reports and respondent’s three expert reports. See generally id.
A
Ms. Apuzzo’s experts are Dr. Nizar Souayah, M.D., and Dr. Samar Gupta, M.D.
Each expert’s findings are discussed in turn.
Dr. Nizar Souayah’s Findings. Dr. Souayah is a neurologist. Apuzzo, 2024 WL
4534200, at *10. Dr. Souayah agrees that Ms. Apuzzo does not fit the traditional CIDP
diagnostic criteria and concedes that her “diagnosis changed from CIDP and to small
fiber neuropathy.” Id. at *11. That said, Dr. Souayah believes that the only plausible
temporal reason of when Ms. Apuzzo’s symptoms appeared was the recent injection of
the influenza vaccination. Id. at *16. So, with a “mosaic of autoimmunity” symptoms
associated with CIDP (and other conditions), the cause must have been the influenza
vaccination. Id. at *16–17. “[M]osaic of autoimmunity” was never defined, but
presumably “refer[s] to the notion that autoimmunity is believed to be multifactorial,
involving both genetic and environmental factors.” Id. at *17.
Dr. Samar Gupta’s Findings. Dr. Gupta is a rheumatologist. Id. at *13. While
Dr. Gupta defers to Dr. Souayah on Ms. Apuzzo’s neuropathic symptoms, he disagrees
that her condition’s cause is solely CIDP when her symptoms track with Sjögren's
Syndrome, especially with the presence of Sjögren's Syndrome antibodies in her body.
Id. at *14. Dr. Gupta concludes that Ms. Apuzzo’s symptoms are “consistent with a
vaccine induced illness.” Id. at *17 (internal quotation marks omitted). That said, “Dr.
Gupta did not explain any direct causal relationship between vaccination and Sjögren's
syndrome,” and instead deferred to Dr. Souayah’s “mosaic of autoimmunity” causation
theory, and to a generalized sense that Ms. Apuzzo’s symptoms appeared post-influenza
vaccination and thus must be connected to the immunization. Id.
B
Respondent’s experts are: Dr. Brian Callaghan, M.D.; Dr. Robert Lightfoot, Jr.,
M.D.; and Dr. Mehrdad Matloubian, M.D. Each expert’s findings are discussed in turn.
Dr. Brian Callaghan’s Findings. Dr. Callaghan is a neurologist. Id. at *11.
Dr. Callaghan acknowledges that Ms. Apuzzo was initially diagnosed with Guillain-
Barré Syndrome and later CIDP; but, to him, Ms. Apuzzo was falsely diagnosed with
CIDP due to her series of symptoms not being aligned with current understandings of
CIDP diagnoses. Id. at *12–13. Nonetheless, he does not present “alterative
diagnosis,” and urges that the lack of a “clear explanation” for Ms. Apuzzo “does not
mean that CIDP must therefore be the diagnosis.” Id. at *12.
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Case 1:17-vv-01915-LAS Document 174 Filed 04/02/25 Page 6 of 10
Dr. Robert Lightfoot, Jr.’s Findings. Dr. Lightfoot was a rheumatologist; he is
now deceased. Id. at *14. Dr. Lightfoot’s reasoning is consistent with Dr. Gupta’s
report in that Dr. Lightfoot agrees that the presence of Sjögren's Syndrome antibodies
alone does not immediately mean a patient has that condition. Id. at *15. But to Dr.
Lightfoot, that point is medically irrelevant because Ms. Apuzzo claims that her
influenza vaccination caused CIDP, and there is no causal relationship exemplified by
her experts between Sjögren's Syndrome antibodies and CIDP. Id. Without further
evidence that the Sjögren's Syndrome antibodies are an indicator of a
pathophysiological role in Ms. Apuzzo’s alleged CIDP illness, “[t]here is no clear
evidence that the [antibodies are] causally related to the alleged CIDP.” Id. (internal
quotation marks omitted).
Dr. Mehrdad Matloubian’s Findings. Dr. Matloubian is a rheumatologist. Id.
Dr. Matloubian believes that Ms. Apuzzo—who was never tested for Sjögren's
Syndrome antibodies prior to her September 17, 2015, influenza vaccination—started
exemplifying symptoms of Sjögren's Syndrome prior to her immunization because of
known hand arthritis. Id. at *16. Moreover, “[c]onsistent with Dr. Gupta's opinion, Dr.
Matloubian explained that both CIDP and small fiber neuropathy can be associated with
Sjögren's [S]yndrome.” Id. Therefore, given her hand arthritis as well as the
association between Sjögren's Syndrome and CIDP, and other conditions, it is
“appropriate[]” to label Ms. Apuzzo’s condition as Sjögren's Syndrome, not CIDP. Id.
Nevertheless, Sjögren's Syndrome “is not known to follow infection, including
influenza infection, which makes it very unlikely that the [influenza] vaccine could
cause Sjögren's [S]yndrome.” Id. at *18.
III
On October 21, 2024, Ms. Apuzzo moved for review of Special Master Horner’s
decision. See generally Petitioner’s Motion for Review of the Special Master’s
Decision, ECF No. 160. On November 15, 2024, Ms. Apuzzo filed the operative
version of her Memorandum in Support of her Motion for Review. See generally
Pet’r’s Mot. On December 5, 2024, Respondent filed its Response in Opposition to Ms.
Apuzzo’s Motion for Review. See generally Respondent’s Response to Petitioner’s
Motion for Review of the Special Master’s Decision, ECF No. 169 [hereinafter Resp’t’s
Mot]. On January 22, 2025, the Court held oral argument in this case.
IV
Under the Vaccine Act, this Court reviews a Special Master’s decision upon the
timely request of either party. 42 U.S.C. § 300aa-12(e)(1)–(2). In reviewing such a
request, this Court may:
(A) uphold the findings of fact and conclusions of law . . . ,
(B) set aside any findings of fact or conclusion of law . . . found to be arbitrary,
capricious, an abuse of discretion, or otherwise not in accordance with law . . . , or
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(C) remand the petition to the special master for further action in accordance with
the court’s direction.
Id. § 300aa-12(e)(2)(A)–(C). “Fact findings are reviewed . . . under the arbitrary and
capricious standard; legal questions under the ‘not in accordance with law’ standard;
and discretionary rulings under the abuse of discretion standard.” Munn v. Sec’y of
Dep’t of Health & Hum. Servs., 970 F.2d 863, 870 n.10 (Fed. Cir. 1992). When
reviewing findings of fact, the Court cannot “substitute its judgment for that of the
special master merely because it might have reached a different conclusion.” Snyder v.
Sec’y of Health & Hum. Servs., 88 Fed. Cl. 706, 718 (2009). Instead, if the special
master’s decision is “based on evidence in the record that [is] not wholly implausible,
[the Court is] compelled to uphold that finding as not being arbitrary or capricious,”
Cedillo v. Sec’y of Health & Hum. Servs., 617 F.3d 1328, 1338 (Fed. Cir.
2010)(quotation removed), because the Court will neither relitigate the factual record
nor “assess whether the special master correctly evaluated the evidence, or examine the
probative value of the evidence or the credibility of the witnesses,” Porter v. Sec’y of
Health & Hum. Servs., 663 F.3d 1242, 1249 (Fed. Cir. 2011). In turn, “if the special
master has considered the relevant evidence of record, drawn plausible inferences and
articulated a rational basis for the decision,” the Court will rarely find reversible error.
Lampe v. Sec’y of Health & Hum. Servs., 219 F.3d 1357, 1360 (Fed. Cir. 2000) (internal
quotation marks omitted).
V
Ms. Apuzzo makes three arguments in favor of reversing Special Master
Horner’s decision. See Pet’r’s Mot. at 11–20. First, Special Master Horner’s review of
the factual record was illegitimate because he supposedly diagnosed her as not suffering
from CIDP, instead of simply determining whether her claimed injury was caused by
her September 17, 2015, influenza vaccination. Second, Special Master Horner failed
to give preferential weight to Ms. Apuzzo’s treating physicians compared to the parties’
expert reports. Third, Special Master Horner incorrectly accepted the parties’ expert
opinions that her symptoms preceded her receiving the influenza vaccination at issue.
Effectively, as summarized by Ms. Apuzzo, all three issues amount to a single
argument: Did Special Master Horner’s review of the factual record, inclusive of the
parties’ expert reports, contravene binding precedent instructing special masters to not
“conduct a differential diagnosis” by choosing one expert’s opinion over another, “or
over a combination of” expert and her treating physicians’ opinions? See generally
Pet’r’s Mot. He did not for three reasons.
One. Special Master Horner was required to evaluate the reliability of the
parties’ expert reports because, in contrast to respondent’s experts, Ms. Apuzzo’s
experts did not agreed on the proper diagnosis for her symptoms. Pafford, 451 F.3d at
1356; see, e.g., Apuzzo, 2024 WL 4534200, at *16–17. Both of her experts, Dr.
Souayah and Dr. Gupta, have differing explanations for her symptoms—with Dr.
Souayah apprising that Ms. Apuzzo’s condition could be CIDP, and Dr. Gupta agreeing
with the majority of respondent’s experts that Ms. Apuzzo’s condition could be
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Sjögren's Syndrome—and both experts, at bottom, generalize her medical condition as a
“mosaic of autoimmunity,” see, e.g., Apuzzo, 2024 WL 4534200, at *16–17, a phrase
neither of her experts define nor link to a “recognized ‘injury’” of the influenza
vaccine, Lombardi., 656 F.3d at 1353. Instead, Dr. Souayah, for instance, merely notes
the temporal relationship between when Ms. Apuzzo received her influenza vaccination
and the onset of a “mosaic of autoimmunity” symptoms associated with CIDP (and
other conditions), and how that would lead to a rational conclusion that the
immunization caused her medical injury. Apuzzo, 2024 WL 4534200, at *16. But
evidence of a temporal relationship between Ms. Apuzzo’s symptoms and the
immunization is insufficient when Ms. Apuzzo’s experts never presented a logical and
consistent “medical theory causally connecting the vaccination and the injury” in her
expert reports. Althen v. Sec’y of Health & Hum. Servs., 418 F.3d 1274, 1278 (Fed. Cir.
2005).
Of note, respondent’s experts—Dr. Callaghan, Dr. Lightfoot, and Dr.
Matloubian—further highlight the inconclusivity of Ms. Apuzzo’s symptoms. E.g.,
Apuzzo, 2024 WL 4534200, at *12–16, *18. All three agree with Ms. Apuzzo’s expert
Dr. Gupta that her symptoms are inconclusive, potentially being Sjögren's Syndrome or
another condition, and may have even occurred prior to vaccination. Compare id., with
id. at *25 (explaining that Ms. Apuzzo’s expert, Dr. Gupta, determined that
“petitioner’s Sjögren's syndrome [originated] pre-vaccination.”).
This case’s facts are identical to Lombardi, where the petitioner’s motion for
review was denied, so precedent directs this case’s outcome. There, “two experts that
Lombardi retained specifically for this litigation differ[ed] in their opinions as to her
injury.” Lombardi, 656 F.3d at 1352 (internal quotation marks omitted). Here, Ms.
Apuzzo’s two experts retained specifically for this litigation differ in their opinions as
to her injury. See, e.g., Apuzzo, 2024 WL 4534200, at *16–17. There, “Lombardi ha[d]
not argued that the three conditions [were] so similar that doctors consider[ed] them to
be conditions along a spectrum of diseases.” Lombardi, 656 F.3d at 1352 (internal
quotation marks omitted). Here, Apuzzo’s two experts have also not argued that her
“mosaic of autoimmunity” conditions exist on a spectrum. As a result, Special Master
Horner had to assume the phrase “may simply refer to the notion that autoimmunity is
believed to be multifactorial, involving both genetic and environmental factors.”
Apuzzo, 2024 WL 4534200, at *17. There, “the government's experts refuted each of
[Lombardi’s supposed] diagnoses and proposed five other possible conditions that
Lombardi may have suffered from.” Lombardi, 656 F.3d at 1352. Here, respondent’s
experts did the same. E.g., Apuzzo, 2024 WL 4534200, at *12–16, *18.
Consequently, like in Lombardi, “[i]n the face of such extreme disagreement
among well-qualified medical experts . . . it was appropriate for the special master to
first determine what injury, if any, was supported by the evidence presented in the
record.” Lombardi, 656 F.3d at 1352–53. Special Master Horner did just that, and no
more, by determining that the preponderance of the evidence pointed to Sjögren's
Syndrome, not CIDP, because the undefined term “mosaic of autoimmunity” was
insufficient to establish causation due to immunization. See generally Apuzzo, 2024
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WL 4534200. Doing so does not amount to diagnosing Ms. Apuzzo. Rather, like in
Lombardi, “the special master merely found that [Ms. Apuzzo] had failed to meet her
burden to show by a preponderance of the evidence that she suffered from” CIDP, “not
merely a symptom or manifestation of an unknown injury.” Lombardi, 656 F.3d at
1353. Special Master Horner, in short, properly evaluated this case under precedent.
Id.
Two. Special Master Horner gave sufficient weight to the opinion of Ms.
Apuzzo’s treating physicians, and even assuming that he did not, the error was
harmless. No treating physician ever definitively concluded that Ms. Apuzzo suffered
from CIDP. E.g., Apuzzo, 2024 WL 4534200, at *4–10; see also id. at *11 (noting that
Dr. Souayah admitted that Ms. Apuzzo’s “diagnosis changed from CIDP and to small
fiber neuropathy.”). Instead, CIDP was always only suspected, and her diagnosis
changed constantly. Id. at *4–10; see also id. at *11. Indeed, at times, Ms. Apuzzo’s
physicians tentatively ruled out CIDP as a cause of Ms. Apuzzo’s symptoms. Id. at *7
(“Dr. Vukic then noted that Dr. Brannagan does not believe petitioner has CIDP and
therefore concluded that [t]he cause of her symptoms remains elusive.” (internal
quotation marks omitted)). In other words, the treating physician record is as “elusive”
and uncertain as Dr. Souayah and Dr. Gupta’s expert opinions. Id. Special Master
Horner reasonably weighed the evidence before him, with special attention paid to the
treating physician record, to determine that the record did not support a CIDP injury,
see, e.g., id. at *20–22, a determination “well within the discretion granted to the
special master under the vaccine program,” Lombardi, 656 F.3d at 1352 (citations
omitted); see also Cedillo, 617 F.3d at 1338 (determining that, if a special master’s
decision is “based on evidence in the record that [is] not wholly implausible, [the Court
is] compelled to uphold that finding as not being arbitrary or capricious.” (quotation
omitted)). Ms. Apuzzo’s argument to the contrary is therefore misplaced.
Three. Special Master Horner did not violate precedent by determining that Ms.
Apuzzo’s condition existed prior to her September 15, 2017, influenza vaccination by
choosing one expert’s opinion over another, “or over a combination of” expert and her
treating physicians’ opinions. See generally Pet’r’s Mot. Quite the opposite. Special
Master Horner noted that both Ms. Apuzzo’s expert, Dr. Gupta, and respondent’s
expert, Dr. Matloubian, agreed that her condition likely predated her immunization.
Apuzzo, 2024 WL 4534200, at *16, 25–26. Finding a less arbitrary determination
would be near impossible.
In sum, Special Master Horner neither violated precedent nor made arbitrary
findings or fact. Munn, 970 F.2d at 870 n.10. Ms. Apuzzo’s Motion for Review of
Special Master Horner’s decision, ECF No. 160, is therefore DENIED, and the Office
of Special Master’s decision, ECF Nos. 158, 159, is AFFIRMED. The clerk is directed
to enter judgment accordingly.
IT IS SO ORDERED.
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Loren A. Smith
s/
Loren A. Smith,
Senior Judge
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