VICP Registry Case Source Bundle
Canonical URL: https://vicp-registry.org/case/USCOURTS-cofc-1_22-vv-01511
Package ID: USCOURTS-cofc-1_22-vv-01511
Petitioner: Muhammad Alqulissi
Filed: 2022-10-13
Decided: 2026-03-16
Vaccine: influenza
Vaccination date: 2019-11-11
Condition: seronegative rheumatoid arthritis
Outcome: dismissed
Award amount USD: 

AI-assisted case summary:
On October 13, 2022, Muhammad Alqulissi filed a petition alleging that a Fluzone Quadrivalent influenza vaccination administered at a CVS Minute Clinic in Houston on November 11, 2019 caused seronegative rheumatoid arthritis and elevated inflammatory markers. He was 36 years old at vaccination, five days short of his thirty-seventh birthday. Respondent opposed compensation.

The record showed a complex medical background, including chronic microcytosis, fatty and mildly enlarged liver, possible thyrotoxic goiter, recurrent tonsillitis, hematuria, positive Helicobacter pylori testing, and GERD. In early December 2019, Mr. Alqulissi sought orthopedic and primary-care evaluation for widespread joint pain and stiffness involving his cervical spine, shoulders, hips, knees, hands, wrists, fingers, and feet. His primary care physician documented severe aching pain worse in the morning, swelling and tenderness in the fingers and hand joints, and a family history that included rheumatoid arthritis and lupus. Rheumatologist Dr. Padma Chimata saw him on December 10, 2019. Mr. Alqulissi reported that most symptoms started around the same time as the flu shot and that he was worried it triggered something; the history also described symptom onset as one to two months earlier. Testing showed elevated ESR and CRP with normal rheumatoid factor and ACPA, and X-rays did not show inflammatory arthropathy. In January 2020, Dr. Chimata diagnosed seronegative RA and treated him with methotrexate, folic acid, sulindac, and later Arava, with improvement by June 2020.

Petitioner relied on Dr. David Axelrod, a clinical immunologist and rheumatologist, who opined that Mr. Alqulissi met criteria for seronegative RA and proposed two possible immune mechanisms: a cytokine-driven innate immune response or an adaptive immune response after vaccination. Respondent relied on Dr. Mehrdad Matloubian, who disputed the causal theory and the evidentiary support for connecting flu vaccination to RA.

Special Master Nora Beth Dorsey found that Mr. Alqulissi had proven the diagnosis of seronegative RA. She denied compensation because the causation proof did not satisfy Althen. The decision found the cytokine and adaptive-response theories insufficiently supported, found that the literature and timing evidence did not establish that influenza vaccination can cause RA, and noted that onset evidence was inconsistent: Mr. Alqulissi's affidavit placed onset eight days after vaccination, medical records suggested widespread pain four days after vaccination, a Motrin request came around fourteen days after vaccination, and Dr. Chimata's history could place onset before vaccination or only one or two days after it. The petition was dismissed on March 16, 2026. An earlier interim attorney-fees decision awarded fees and costs, but no vaccine-injury compensation was awarded.

Theory of causation field:
Fluzone Quadrivalent influenza vaccine November 11, 2019, at age 36, allegedly causing seronegative RA; DISMISSED. Onset evidence conflicted: affidavit 8 days, preliminary finding/records around November 15 (4 days), Motrin request around 14 days, and rheumatology history one to two months or four weeks. Petitioner expert Dr. David Axelrod proposed cytokine-mediated innate immune activation and/or adaptive immune response; respondent expert Dr. Mehrdad Matloubian disputed causation. RF/ACPA negative, ESR/CRP elevated, X-rays unremarkable, rheumatology diagnosed seronegative RA and treated with methotrexate/Arava. SM Nora Beth Dorsey accepted diagnosis but found Althen prongs one and three not proven. Decision March 16, 2026. Attorney: Sean Franks Greenwood.

Public staged source text:

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DOCUMENT 1: USCOURTS-cofc-1_22-vv-01511-cl-extra-10779311
Date issued/filed: 2025-01-13
Pages: 1
Docket text: Supplementary opinion from CourtListener cluster 10312723
--------------------------------------------------------------------------------
            In the United States Court of Federal Claims
                              OFFICE OF SPECIAL MASTERS
                                  Filed: December 18, 2024

* * * * * * * * * * * * * *                  *
MUHAMMAD ALQULISSI,                          *       PUBLISHED
                                             *
               Petitioner,                   *       No. 22-1511V
                                             *
v.                                           *       Special Master Nora Beth Dorsey
                                             *
SECRETARY OF HEALTH                          *       Interim Attorneys’ Fees and Costs.
AND HUMAN SERVICES,                          *
                                             *
               Respondent.                   *
                                             *
* * * * * * * * * * * * * *                  *

Sean Franks Greenwood, The Greenwood Law Firm, Houston, TX, for Petitioner.
Zoe Wade, U.S. Department of Justice, Washington, DC, for Respondent.

              DECISION ON INTERIM ATTORNEYS’ FEES AND COSTS 1

      On October 13, 2022, Muhammad Alqulissi (“Petitioner”) filed a petition for
compensation under the National Vaccine Injury Compensation Program (“Vaccine Act,” “the
Program,” or “the Act”), 42 U.S.C. § 300aa-10 et seq. (2018) 2 alleging that he suffered from
rheumatoid arthritis (“RA”) following the administration of an influenza (“flu”) vaccination on
November 11, 2019. Petition at Preamble (ECF No. 1); Amended Petition at Preamble (ECF No.
22).


1
  Because this Decision contains a reasoned explanation for the action in this case, the
undersigned is required to post it on the United States Court of Federal Claims’ website and/or at
https://www.govinfo.gov/app/collection/uscourts/national/cofc in accordance with the E-
Government Act of 2002. 44 U.S.C. § 3501 note (2018) (Federal Management and Promotion of
Electronic Government Services). This means the Decision will be available to anyone with
access to the Internet. In accordance with Vaccine Rule 18(b), Petitioner has 14 days to
identify and move to redact medical or other information, the disclosure of which would
constitute an unwarranted invasion of privacy. If, upon review, the undersigned agrees that the
identified material fits within this definition, the undersigned will redact such material from
public access.
2
 The National Vaccine Injury Compensation Program is set forth in Part 2 of the National
Childhood Vaccine Injury Act of 1986, Pub. L. No. 99-660, 100 Stat. 3755, codified as amended,
42 U.S.C. §§ 300aa-10 to -34 (2018). All citations in this Decision to individual sections of the
Vaccine Act are to 42 U.S.C. § 300aa.


                                                 1
        On May 15, 2024, Petitioner filed a motion for interim attorneys’ fees and costs,
requesting compensation for the attorney who worked on his case. Petitioner’s Application for
Interim Award of Attorney’s Fees and Expenses (“Pet. Mot.”), filed May 15, 2024 (ECF No. 51).
Petitioner’s request can be summarized as follows:

       Attorneys’ Fees – $20,433.55
       Attorneys’ Costs – $5,567.97

       Petitioner thus requests a total of $26,001.52. Respondent filed his response on May 23,
2024, stating that he “defers to the Special Master as to whether [P]etitioner has made a special
showing to justify an award of interim attorneys’ fees and costs under the particular
circumstances of this case.” Respondent’s Response to Pet. Mot. (“Resp. Response”), filed Feb.
12, 2024, at 3 (ECF No. 52). Petitioner did not file a reply.

       This matter is now ripe for adjudication. For the reasons discussed below, the
undersigned GRANTS IN PART Petitioner’s motion and awards $25,329.52 in attorneys’ fees
and costs.

I.     DISCUSSION

        Under the Vaccine Act, the special master shall award reasonable attorneys’ fees and
costs for any petition that results in an award of compensation. § 15(e)(1). When compensation
is not awarded, the special master “may” award reasonable fees and costs “if the special master
or court determines that the petition was brought in good faith and there was a reasonable basis
for the claim for which the petition was brought.” Id. If a special master has not yet determined
entitlement, she may still award attorneys’ fees and costs on an interim basis. Avera v. Sec’y of
Health & Hum. Servs., 515 F.3d 1343, 1352 (Fed. Cir. 2008). Such awards “are particularly
appropriate in cases where proceedings are protracted and costly experts must be retained.” Id.
Similarly, it is proper for a special master to award interim fees and costs “[w]here the claimant
establishes that the cost of litigation has imposed an undue hardship and that there exists a good
faith basis for the claim.” Shaw v. Sec’y of Health & Hum. Servs., 609 F.3d 1372, 1375 (Fed.
Cir. 2010).

        The claim appears at this point to have been brought in good faith and built on a
reasonable basis. Moreover, the undersigned finds that an award of interim attorneys’ fees and
costs is appropriate here.

       A.      Attorneys’ Fees

       Counsel must submit fee requests that include contemporaneous and specific billing
records indicating the service performed, the number of hours expended on the service, and the
name of the person performing the service. See Savin v. Sec’y of Health & Hum. Servs., 85 Fed.
Cl. 313, 316-18 (2008). Counsel should not include in their fee requests hours that are
“excessive, redundant, or otherwise unnecessary.” Saxton v. Sec’y of Health & Hum. Servs., 3
F.3d 1517, 1521 (Fed. Cir. 1993) (quoting Hensley v. Eckerhart, 461 U.S. 424, 434 (1983)). It is
“well within the special master’s discretion to reduce the hours to a number that, in [her]



                                                2
experience and judgment, [is] reasonable for the work done.” Id. at 1522. Furthermore, the
special master may reduce a fee request sua sponte, apart from objections raised by Respondent
and without providing the Petitioner notice and opportunity to respond. See Sabella v. Sec’y of
Health & Hum. Servs., 86 Fed. Cl. 201, 209 (2009).

        A special master need not engage in a line-by-line analysis of Petitioner’s fee application
when reducing fees. Broekelschen v. Sec’y of Health & Hum. Servs., 102 Fed. Cl. 719, 729
(2011). Special masters may rely on their experience with the Vaccine Act and its attorneys to
determine the reasonable number of hours expended. Wasson v. Sec’y of Health & Hum. Servs.,
24 Cl. Ct. 482, 484 (Fed. Cl. 1991), rev’d on other grounds and aff’d in relevant part, 988 F.2d
131 (Fed. Cir. 1993). Just as “[t]rial courts routinely use their prior experience to reduce hourly
rates and the number of hours claimed in attorney fee requests . . . [v]accine program special
masters are also entitled to use their prior experience in reviewing fee applications.” Saxton, 3
F.3d at 1521.

               1.      Hourly Rates

        Here, Petitioner requests the following hourly rates for the attorneys, paralegals, and legal
assistant that worked on this matter:

Sean Greenwood – Attorney
      2021: $425.00
      2022: $470.00
      2023: $495.00

Janell Ochoa – Attorney
       2021: $180.00
       2022-2023: $200.00

Anna Carruth – Attorney
      2021: $180.00

Meagan Ward – Paralegal
     2020: $160.00
     2021-2022: $170.00

Jonathan Krupa – Paralegal
      2022: $165.00
      2023: $175.00
      2024: $185.00

Thomas Ambrosio – Legal Assistant
     2023: $161.00

       The undersigned finds that the requested rates are reasonable and in accordance with
what these attorneys and paralegals have previously been awarded for their Vaccine Program



                                                 3
work. See, e.g., Powell v. Sec’y of Health & Hum. Servs., No. 20-1726V, 2024 WL 1996715, at
*2 (Fed. Cl. Spec. Mstr. Apr. 11, 2024); Ambriz v. Sec’y of Health & Hum. Servs., No. 15-
502V, 2024 WL 945688, at *2 (Fed. Cl. Spec. Mstr. Jan. 25, 2024); Torres v. Sec’y of Health &
Hum. Servs., No. 21-1356V, 2023 WL 9177302, at *3 (Fed. Cl. Spec. Mstr. Dec. 19, 2023);
Carre v. Sec’y of Health & Hum. Servs., 20-1613V, 2023 WL 2645840, at *2 (Fed. Cl. Spec.
Mstr. Feb. 24, 2023). The undersigned will therefore award those rates in full.

               2.      Reduction of Billable Hours

        In reducing an award of fees, the goal is to achieve rough justice, and therefore a special
master may take into account their overall sense of a case and may use estimates when reducing
an award. See Florence v. Sec’y of Health & Hum. Servs., No. 15-255V, 2016 WL 6459592, at
*5 (Fed. Cl. Spec. Mstr. Oct. 6, 2016) (citing Fox v. Vice, 563 U.S. 826, 838 (2011)). It is well
established that an application for fees and costs must sufficiently detail and explain the time
billed so that a special master may determine, from the application and the case file, whether the
amount requested is reasonable. Bell v. Sec’y of Health & Hum. Servs., 18 Cl. Ct. 751, 760
(1989). Petitioner bears the burden of documenting the fees and costs claimed.

        Upon review of the submitted billing records, the undersigned finds the majority of the
time billed to be reasonable. The timesheet entries are sufficiently detailed for an assessment to
be made of the entries’ reasonableness. A small reduction, however, is necessary due to time
billed for non-compensable administrative tasks (e.g., filing documents and retrieving,
compiling, and preparing records). 3 See Pet. Exhibit (“Ex.”) 50. “Clerical and secretarial tasks
should not be billed at all, regardless of who performs them.” Paul v. Sec’y of Health & Hum.
Servs., No. 19-1221V, 2023 WL 1956423, at *3 (Fed. Cl. Spec. Mstr. Feb. 13, 2023); see also
Rochester v. United States, 18 Cl. Ct. 379, 387 (1989) (stating that services that are “primarily of
a secretarial or clerical nature . . . should be considered as normal overhead office costs included
within the attorneys’ fee rates”).

        The undersigned also finds excessive and duplicative time billed for some tasks. For
example, Mr. Krupa billed 0.40 hours ($70.00) for drafting notice of intent to remain in the
program, which was one sentence and presumably identical to other notices of intent to remain in
the program filed in other cases. Mr. Krupa also billed 0.20 hours ($35.00) for reviewing the
case docket following reassignment to the undersigned on June 20, 2023, after he already billed
for reviewing the notice of reassignment. Additionally, on October 13 and 14, 2022, both Ms.
Ochoa and Mr. Krupa both billed for drafting, reviewing, and finalizing Petitioner’s petition,
exhibits, and statement of completion, which is duplicative.

      Some of these issues have previously been raised with this firm. See Carre, 2023 WL
2645840, at *2-3; Powell, 2024 WL 1996715, at *2-3. Therefore, given the number of issues,




3
 For example, see entries dated January 31, 2022, October 13, 2022, February 10, 2023,
February 14, 2023, March 23, 2023, April 10, 2023, April 11, 2023, August 18, 2023, November
27, 2023, December 14, 2023, and December 27, 2023. This is not an exhaustive list.


                                                 4
the undersigned finds a reduction of fees by 3% to be reasonable. 4 See Powell, 2024 WL
1996715, at *3 (reducing fees by 5% for same issues). This results in a reduction of $613.00. 5

         B.     Attorneys’ Costs

                1.      Expert Fees

        Petitioner requests $4,500.00 for work performed by Dr. David Axelrod at a rate of
$400.00 per hour. Pet. Ex. 51 at 4. This rate has previously been found reasonable. See Powell,
2024 WL 1996715, at *3; Tipps v. Sec’y of Health & Hum. Servs., No. 16-867V, 2023 WL
2754559, at *3 (Fed. Cl. Spec. Mstr. Apr. 3, 2023). Dr. David Axelrod spent 11.25 hours
reviewing medical records, researching, and preparing one expert report totaling 24 pages. Pet.
Ex. 51 at 4; Pet. Ex. 22. Given the complexity of this case, the undersigned finds this amount of
time to be reasonable. Therefore, Dr. Axelrod will be awarded $4,500.00 in accordance with the
$400.00 hourly rate.

                2.      Miscellaneous Costs

       Petitioner also requests $1,037.97 for miscellaneous costs, including the filing fee,
medical records, and postage. Pet. Ex. 50 at 10; Pet. Ex. 51. The undersigned finds these costs
reasonable. Petitioner has provided adequate documentation for most of these costs. However,
the undersigned finds some discrepancies in the documentation for the expenses requiring
reductions.

        On June 6, 2022, Petitioner invoiced $108.42, when the receipt indicated the total was
$108.02, resulting in a reduction of $0.40. Pet. Ex. 51 at 6-7. On November 7 and November
16, 2023, Petitioner invoiced $46.00 for the same medical records invoice. Pet. Ex. 50 at 10.
Because this is duplicative, the undersigned will deduct $46.00. Petitioner also invoiced for
expenses on March 9, 2023 ($0.60), March 22, 2023 ($6.00), and March 23, 2023 ($6.00);
however, no receipts for these expenses were provided. As such, Petitioner will not be awarded
for these costs, resulting in a further reduction of $12.60. Petitioner may re-request these costs in
her final fees motion along with supportive documentation.

         Thus, the undersigned finds a reduction of $59.00 6 to be appropriate.

II.      CONCLUSION

        Based on all of the above, the undersigned finds that it is reasonable to compensate
Petitioner and his counsel as follows:


4
  A special master need not engage in a line-by-line analysis of Petitioner’s fee application when
reducing fees. Broekelschen, 102 Fed. Cl. at 729.
5
    $20,433.55 x 0.03 = $613.00.
6
    $0.40 + $46.00 + 12.60 = $59.00.


                                                  5
       Requested Attorneys’ Fees:                                           $20,433.55
       Reduction of Attorneys’ Fees:                                        - ($613.00)
       Awarded Attorneys’ Fees:                                             $19,820.55

       Requested Attorneys’ Costs:                                          $5,567.97
       Reduction of Attorneys’ Costs:                                       - ($59.00)
       Awarded Attorneys’ Costs:                                            $5,508.97

       Total Attorneys’ Fees and Costs:                                     $25,329.52

       Accordingly, the undersigned awards:

       A lump sum in the amount of $25,329.52, representing reimbursement for
       reasonable interim attorneys’ fees and costs, in the form of a check payable jointly
       to Petitioner and Petitioner’s counsel of record, Mr. Sean Greenwood.

       In the absence of a motion for review filed pursuant to RCFC Appendix B, the Clerk of
Court SHALL ENTER JUDGMENT in accordance with this Decision. 7

       IT IS SO ORDERED.

                                             s/ Nora Beth Dorsey
                                             Nora Beth Dorsey
                                             Special Master




7
 Pursuant to Vaccine Rule 11(a), entry of judgment is expedited by the parties’ joint filing of
notice renouncing the right to seek review.


                                                6


================================================================================
DOCUMENT 2: USCOURTS-cofc-1_22-vv-01511-1
Date issued/filed: 2026-04-10
Pages: 41
Docket text: PUBLIC DECISION (Originally filed: 3/16/2026) regarding 83 DECISION of Special Master. Signed by Special Master Nora Beth Dorsey. (aevw) Service on parties made.
--------------------------------------------------------------------------------
Case 1:22-vv-01511-UNJ Document 86 Filed 04/10/26 Page 1 of 41
In the United States Court of Federal Claims
OFFICE OF SPECIAL MASTERS
Filed: March 16, 2026
* * * * * * * * * * * * * * * * * * * * * * * * *
MUHAMMAD ALQULISSI, * PUBLISHED
*
Petitioner, * No. 22-1511V
*
v. * Special Master Nora Beth Dorsey
*
SECRETARY OF HEALTH * Dismissal; Influenza (“Flu”) Vaccine;
AND HUMAN SERVICES, * Rheumatoid Arthritis (“RA”); Causation-in-
* Fact.
Respondent. *
*
* * * * * * * * * * * * * * * * * * * * * * * * *
Sean Franks Greenwood, The Greenwood Law Firm, Houston, TX, for Petitioner.
Eleanor Hanson, U.S. Department of Justice, Washington, DC, for Respondent.
DECISION1
On October 13, 2022, Muhammad Alqulissi (“Petitioner”) filed a petition for
compensation under the National Vaccine Injury Compensation Program (“Vaccine Act” or “the
Program”), 42 U.S.C. § 300aa-10 et seq. (2018).2 Petitioner alleges that an influenza (“flu”)
vaccination administered to him on November 11, 2019 “was the cause-in-fact” of his
seronegative rheumatoid arthritis (“RA”) and elevated erythrocyte sedimentation. Petition at
1 Because this Decision contains a reasoned explanation for the action in this case, the
undersigned is required to post it on the United States Court of Federal Claims’ website and/or at
https://www.govinfo.gov/app/collection/uscourts/national/cofc in accordance with the E-
Government Act of 2002. 44 U.S.C. § 3501 note (2018) (Federal Management and Promotion of
Electronic Government Services). This means the Decision will be available to anyone with
access to the Internet. In accordance with Vaccine Rule 18(b), Petitioner has 14 days to
identify and move to redact medical or other information, the disclosure of which would
constitute an unwarranted invasion of privacy. If, upon review, the undersigned agrees that the
identified material fits within this definition, the undersigned will redact such material from
public access.
2 The National Vaccine Injury Compensation Program is set forth in Part 2 of the National
Childhood Vaccine Injury Act of 1986, Pub. L. No. 99-660, 100 Stat. 3755, codified as amended,
42 U.S.C. §§ 300aa-10 to -34 (2018) (“Vaccine Act” or “the Act”). All citations in this Decision
to individual sections of the Vaccine Act are to 42 U.S.C.A. § 300aa.

Case 1:22-vv-01511-UNJ Document 86 Filed 04/10/26 Page 2 of 41
Preamble, ¶ 20 (ECF No. 1); Amended (“Am.”) Petition at Preamble, ¶ 31 (ECF No. 22).3
Respondent argued against compensation, stating that “this case is not appropriate for
compensation under the terms of the Act.” Respondent’s Report (“Resp. Rept.”) at 1, 6 (ECF
No. 36) (emphasis omitted).
After carefully analyzing and weighing the evidence presented in this case in accordance
with the applicable legal standards,4 the undersigned finds that Petitioner has failed to provide
preponderant evidence that his flu vaccine caused his seronegative RA, and thus has not satisfied
his burden of proof under Althen v. Secretary of Health & Human Services, 418 F.3d 1274, 1280
(Fed. Cir. 2005). Accordingly, Petitioner is not entitled to compensation.
I. ISSUES TO BE DECIDED
There are two issues in dispute. The first is whether Petitioner suffered a “medically
recognized injury” identified as RA.5 Joint Status Rept. (“Joint Submission”), filed Jan. 14,
2025, at 1 (ECF No. 73). The second dispute is causation, specifically the parties disagree as to
whether Petitioner has provided preponderant evidence of all three Althen prongs. Id. at 1-2.
II. BACKGROUND
A. Medical Terminology
RA is a “systemic autoimmune disease characterized by inflammatory polyarthritis. The
hallmark of RA is symmetric synovial proliferation and tenderness in multiple joints, particularly
the small joints of the hands and feet.” Petitioner’s Exhibit (“Pet. Ex.”) 55 at 1.6 Approximately
3 Petitioner’s amended petition added Petitioner’s pre-vaccination medical history and removed
“seronegative.” See Am. Petition.
4 While the undersigned has reviewed all the information filed in this case, only those filings and
records that are most relevant will be discussed. See Moriarty v. Sec’y of Health & Hum. Servs.,
844 F.3d 1322, 1328 (Fed. Cir. 2016) (“We generally presume that a special master considered
the relevant record evidence even though [s]he does not explicitly reference such evidence in
h[er] decision.”); Simanski v. Sec’y of Health & Hum. Servs., 115 Fed. Cl. 407, 436 (2014)
(“[A] Special Master is ‘not required to discuss every piece of evidence or testimony in her
decision.’” (citation omitted)), aff’d, 601 F. App’x 982 (Fed. Cir. 2015); see also Paterek v.
Sec’y of Health & Hum. Servs., 527 F. App’x 875, 884 (Fed. Cir. 2013) (“Finding certain
information not relevant does not lead to—and likely undermines—the conclusion that it was not
considered.”).
5 Although his petition also alleged that he suffered elevated erythrocyte sedimentation, the
parties appropriately refined the alleged injury as RA in their Joint Submission.
6 Richard D. Brasington & Jonathan J. Miner, Clinical Features of Rheumatoid Arthritis, in
Rheumatology 760 (Marc C. Hochberg et al. eds., 7th ed. 2019).
2

Case 1:22-vv-01511-UNJ Document 86 Filed 04/10/26 Page 3 of 41
80% of patients with RA test positive for rheumatoid factor (“RF”)7 and/or anti-citrullinated
peptide antibodies (“ACPAs”).8 Id.; Pet. Ex. 24 at 1.9
Diagnostic criteria promulgated by the American College of Rheumatology (“ACR”) and
the European League Against Rheumatism (“EULAR”) in 2010 assess points based on an
algorithm which includes the following findings or serology results: “active synovitis in at least
one joint that cannot be better explained by another diagnosis,” ACPAs, RF, abnormal
inflammatory markers (erythrocyte sedimentation rate (“ESR”)10 and C-reactive protein
(“CRP”)),11 and duration of symptoms of six weeks or greater. Pet. Ex. 23 at 1, 2 tbl.92.1.12
7 RF antibodies are “antibodies directed against antigenic determinants, i.e., Gm, in the Fc region
of the IgG class of immunoglobulins; these are found in the serum of about 80 percent of persons
with classical or definite [RA].” Rheumatoid Factor, Dorland’s Med. Dictionary Online,
https://www.dorlandsonline.com/dorland/definition?id=74591 (last visited Mar. 12, 2026).
8 ACPAs are antibodies against cyclic citrullinated peptide, “a synthetic, citrulline-containing
peptide with a cyclic structure,” that are “highly specific for [RA].” Anti-CCP Antibody,
Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=
56787 (last visited Mar. 12, 2026); Cyclic Citrullinated Peptide, Dorland’s Med. Dictionary
Online, https://www.dorlandsonline.com/dorland/definition?id=97140 (last visited Mar. 12,
2026).
9 Chanchal Gera & Arti Muley, Classification Criteria for Seronegative Rheumatoid Arthritis
Based on Rheumatologist’s Practice and Experience, 19 Curr. Med. Issues 236 (2021).
10 ESR is “the rate at which erythrocytes precipitate out from a well-mixed specimen of venous
blood, measured by the distance the top of the column of erythrocytes falls in a given time
interval under specified conditions; an increase in rate is usually due to elevated levels of plasma
proteins, especially fibrinogen and immunoglobulins, which decrease the zeta potential on
erythrocytes by dielectric shielding and thus promote rouleau formation. It is increased in
monoclonal gammopathy, hypergammaglobulinemia due to inflammatory disease,
hyperfibrinogenemia, active inflammatory disease, and anemia.” Erythrocyte Sedimentation
Rate, Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/dorland/definition?
id=102146 (last visited Mar. 12, 2026).
11 CRP is “a globulin that forms a precipitate with the somatic C-polysaccharide of the
pneumococcus in vitro; it is the most predominant of the acute-phase proteins.” C-Reactive
Protein, Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/dorland/definition?
id=100489 (last visited Mar. 12, 2026).
12 Katherine P. Liao, Rheumatoid Arthritis: Classification and Epidemiology of Rheumatoid
Arthritis, in Rheumatology, supra note 6, at 747-53.
3

Case 1:22-vv-01511-UNJ Document 86 Filed 04/10/26 Page 4 of 41
The cause of RA is not known. See, e.g., Pet. Ex. 30 at 1;13 Pet. Ex. 58 at 2 (explaining
the “key biologic pathways that drive initial autoimmunity and then [] transition to a more
pathogenic stated and clinically identifiable [RA] are not known”);14 Resp. Ex. A-2 at 1.15 Risk
factors include family history, female sex, smoking, obesity, lung disease, and periodontal
inflammation. Pet. Ex. 23 at 3-5; Pet. Ex. 58 at 6 tbl.2; Resp. Ex. A-2 at 3-6. Genome studies
have shown associations between seropositive RA and the human leukocyte antigen (“HLA”)
region (HLA-DR alleles).16 Resp. Ex. A-20 at 3, 5, 7;17 see also Pet. Ex. 30 at 1-2 (discussing
the genetic basis of RA).
Studies have suggested that certain infectious pathogens may play a role in the etiology
of RA, notably Porphyromonas gingivalis (“P. gingivalis”) (periodontal disease), Proteus
mirabilis, Escherichia coli, and Epstein Barr Virus (“EBV”). Pet. Ex. 63 at 6.18 Other infectious
agents have been associated with RA, including parvovirus, human immunodeficiency virus
(“HIV”), and hepatitis B and C viruses. Id. It has also been suggested that in the context of
infectious agents, molecular mimicry may play “a critical role” in the pathogenesis of RA. Id.
Lastly, “[i]t should be noted that in sharp contrast, seronegative RA is enigmatic and distinct
from seropositive RA.” Id.
13 Ernest Choy, Understanding the Dynamics: Pathways Involved in the Pathogenesis of
Rheumatoid Arthritis, 51 Rheumatology v3 (2012).
14 Kevin D. Deane & V. Michael Holers, Rheumatoid Arthritis Pathogenesis, Prediction, and
Prevention: An Emerging Paradigm Shift, 73 Arthritis & Rheumatol. 181 (2021).
15 Cynthia S. Crowson, Epidemiology of, Risk Factors for, and Possible Causes of Rheumatoid
Arthritis, UpToDate, https://www.uptodate.com/contents/epidemiology-of-risk-factors-for-and-
possible-causes-of-rheumatoid-arthritis (last updated Apr. 30, 2019).
16 HLA are “histocompatibility antigens governed by genes of the HLA complex (the human
major histocompatibility complex), a region on the short arm of chromosome 6 containing
several genetic loci, each having multiple alleles.” Human Leukocyte Antigens, Dorland’s Med.
Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=56923 (last visited
Mar. 12, 2026). HLA-DR loci “are [] associated with antigenic determinants on class II antigen
molecules,” which are “major histocompatibility antigens found only on immunocompetent cells,
primarily B lymphocytes and macrophages; they are found on molecules consisting of two
noncovalently bound chains.” Class II Antigens, Dorland’s Med. Dictionary Online,
https://www.dorlandsonline.com/dorland/definition?id=56885 (last visited Mar. 12, 2026).
17 Vivianne Malmström et al., The Immunopathogenesis of Seropositive Rheumatoid Arthritis:
From Triggering to Targeting, 17 Nature Revs. Immunol.60 (2017).
18 Manuel Rojas et al., Molecular Mimicry and Autoimmunity, 95 J. Autoimmun. 100 (2018).
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B. Procedural History
Petitioner filed his petition on October 13, 2022. Petition. From October 2022 to April
2023, Petitioner filed medical records,19 an affidavit from Petitioner, and an amended petition.
Pet. Exs. 1-18; Am. Petition. This case was assigned to the undersigned in June 2023. Notice of
Reassignment dated June 15, 2023 (ECF No. 26). Respondent filed his Rule 4(c) report arguing
against compensation on October 24, 2023. Resp. Rept. at 1, 6.
From December 2023 to June 2024, Petitioner filed expert reports from Dr. David
Axelrod and Respondent filed an expert report from Dr. Mehrdad Matloubian. Pet. Exs. 22, 53;
Resp. Ex. A.
On October 1, 2024, pursuant to the parties’ request, the undersigned held a Rule 5
conference. Rule 5 Order dated October 3, 2024 (ECF No. 66). The undersigned preliminarily
found Petitioner’s diagnosis to be seronegative RA. Id. at 2. The undersigned also preliminarily
found onset to be November 15, 2019, within four days of vaccination. Id. However, the
undersigned was unable to provide any preliminary opinions as to the Althen prongs. Id.
Thereafter, Respondent indicated he wished to defend the case, and the parties requested a
briefing schedule from the Court for resolution of entitlement on the record. Resp. Status Rept.,
filed Nov. 13, 2024 (ECF No. 68).
Petitioner filed a motion for a ruling on the record on February 3, 2025, and Respondent
filed a response on May 9, 2025. Pet. Mot. for Ruling on the Record (“Pet. Mot.”), filed Feb. 3,
2025 (ECF No. 77);20 Resp. Response to Pet. Mot. (“Resp. Response”), filed May 9, 2025 (ECF
No. 81). Petitioner did not file a reply.
This matter is now ripe for adjudication.
C. Factual History
1. Medical History21
Petitioner was thirty-six years old when he received a flu vaccination (Fluzone
Quadrivalent) on November 11, 2019 at a CVS Minute Clinic in Houston, Texas. Pet. Ex. 13 at
11-12. Petitioner’s medical history was significant for chronic microcytosis, fatty and mildly
19 Medical records were filed throughout litigation.
20 Petitioner, sua sponte, filed a brief in support of a damages award along with his motion for a
ruling on the record. See Pet. Supplemental Brief in Support of Damages Award, filed Feb. 3,
2025 (ECF No. 77-2). This brief was prematurely filed since entitlement to compensation was
not yet adjudicated. As such, it is not relevant to the issues in dispute resolved by this Decision.
21 This medical history is taken from Respondent’s Responsive Brief as the undersigned finds it
accurately reflects the medical records. See Resp. Response at 2-5. The undersigned has made
edits, deleted less relevant entries, and included additional information and definitions.
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enlarged liver, ultrasound suggestive of thyrotoxic goiter, recurrent acute tonsillitis, hematuria,
and positive tests for Helicobacter pylori and gastroesophageal reflux disease (“GERD”). Pet.
Ex. 6 at 2, 9, 11, 31, 53-54, 56.
On December 3, 2019, Petitioner saw orthopedist, Steven Nolan, M.D., with complaints
of pain in his cervical spine, shoulders, hips, knees, and hands. Pet. Ex. 3 at 9. Petitioner stated
he noticed pain and weakness in both knees and hips “on occasion,” but his hips had improved,
and that most of his pain was now in his right knee, which would occasionally give way. Id. Dr.
Nolan noted that Petitioner had a previous X-ray on the right knee with normal results. Id. He
assessed Petitioner with a “probable torn meniscus of the right knee” and referred Petitioner for a
magnetic resonance imaging (“MRI”). Id.
Petitioner presented to his primary care physician (“PCP”), Chante Ellison-Hodges,
M.D., on December 5, 2019, complaining of pain “all over joints for the past few weeks.” Pet.
Ex. 19 at 266. He reported “severe aching pain” in his wrists, fingers, knees, and feet that was
worse in the morning. Id. He also had stiffness but no numbness or tingling. Id. Petitioner
advised that his mother was diagnosed with RA, and that he was seen by an orthopedist about
three weeks prior and given Motrin without relief. Id. at 267. A physical examination revealed
swelling in the fingers, tenderness of the interphalangeal (“IP”) joints of both thumbs and distal
IP (“DIP”) joints of both index fingers, as well as pain in all joints in both hands. Id. at 270. Dr.
Ellison-Hodges ordered laboratory tests, referred Petitioner to rheumatology, and ordered
dexamethasone tablets. Id.
The following day (December 6), Petitioner sent an email to Dr. Ellison-Hodges
regarding questions about possible thalassemia.22 Pet. Ex. 19 at 261. He had never previously
been informed about thalassemia but had felt fatigued for the past three years and had shortness
of breath when he exercised. Id. Laboratory testing to evaluate Petitioner for thalassemia was
ordered. Id. Three days later (December 9), Petitioner emailed Dr. Ellison-Hodges to inquire
about laboratory testing for systemic lupus erythematosus (“lupus”), stating that his mother and
aunt were diagnosed with lupus. Id. at 248. Testing revealed Petitioner’s antinuclear antibody
(“ANA”)23 results were negative. Id. at 248, 271-72.
On December 10, 2019, Petitioner presented to rheumatologist, Padma Chimata, M.D.,
for an initial evaluation. Pet. Ex. 4 at 23. Petitioner reported that most of his symptoms started
around the same time he received a flu vaccination and that he was worried that might have
triggered something. Id. Petitioner advised his symptoms began one-to-two months ago,
gradually starting with pain in his neck and shoulders, then hips, then knees and hands and feet.
22 Thalassemia is “a heterogeneous group of hereditary hemolytic anemias that have in common
a decreased rate of synthesis of one or more hemoglobin polypeptide chains.” Thalassemia,
Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=
49484 (last visited Mar. 12, 2026).
23 ANA are “antibodies directed against nuclear antigens” that “are frequently found in [RA].”
Antinuclear Antibodies, Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/
dorland/definition?id=56804 (last visited Mar. 12, 2026).
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Id. Petitioner had joint pain in both hands, rated a 1/10, with redness, but no warmth or
tenderness. Id. Dr. Chimata noted that Petitioner’s CRP and ESR were abnormal,24 and that
prior to the onset of Petitioner’s symptoms, he had a sore throat, “had taken flu shots [in]
November,” and had a strong family history of lupus and RA. Id. Dr. Chimata diagnosed
polyarthritis, noting that Petitioner was on steroids. Id. at 24. Dr. Chimata prescribed sulindac
(nonsteroidal anti-inflammatory) and famotidine. Id. at 25.
X-rays of Petitioner’s hands, wrists, knees, and pelvis were performed on December 13,
2019, and were noted to be unremarkable. Pet. Ex. 4 at 29. X-rays of the hands/wrists did not
show findings of inflammatory arthropathy. Id. X-ray of the bilateral knees revealed intact
alignment and no evidence of inflammatory arthropathy. Id. The same was true of the pelvis X-
ray. Id.
On January 8, 2020, Petitioner attended a follow-up appointment with Dr. Chimata to
discuss test results. Pet. Ex. 4 at 20-22. Dr. Chimata diagnosed Petitioner with seronegative RA.
Id. at 21. Petitioner’s RF and ACPA were normal. Pet. Ex. 19 at 276; Pet. Ex. 4 at 44. Dr.
Chimata prescribed methotrexate25 and folic acid, refilled sulindac and famotidine, and advised
Petitioner to follow up in four to six weeks. Pet. Ex. 4 at 21-22. Petitioner attended a follow-up
appointment with Dr. Chimata on February 5, 2020, and no changes were noted. Id. at 17-19.
By June 11, 2020, when Petitioner returned to see Dr. Chimata, he reported he was
“doing much better.” Pet. Ex. 4 at 14. His laboratory results were also improved. Id. Petitioner
denied any aching, pain, or joint stiffness, but complained of fatigue. Id. Petitioner’s
prescription for methotrexate was discontinued, and he was started on Arava.26 Id. Dr. Chimata
recommended he continue Sulindac as needed. Id.
Petitioner established care with Dr. Saiyada Mirza as his new PCP on June 24, 2020. Pet.
Ex. 19 at 217-18. At that time, Petitioner reported malaise/fatigue, weight loss, and joint pain.
Id. at 220. Dr. Mirza’s assessment included elevated red blood cells, low mean corpuscular
volume (“MCV”), hyperlipidemia, fatigue, and Vitamin D deficiency. Id. at 221-22. Petitioner
was referred to hematology/oncology specialist, Monica Desai, M.D., for further evaluation of
his MCV and red blood cell count, and for possible thalassemia. Id. at 154, 221-22.
24 His CRP (25; reference range 0-10 mg/L) and ESR (50; reference range 0-15 mm/hr) were
elevated. Pet. Ex. 19 at 273, 276-77.
25 Methotrexate is “a folic acid antagonist that acts by inhibiting synthesis of DNA, RNA,
thymidylate, and protein” and is “used as an antipsoriatic and antiarthritic in the treatment of
severe, recalcitrant, disabling psoriasis and severe [RA] and psoriatic arthritis.” Methotrexate,
Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=
30930 (last visited Mar. 12, 2026).
26 Arava (leflunomide) is “an immunomodulator that inhibits pyrimidine synthesis, used as a
disease-modifying antirheumatic drug in treatment of [RA].” Leflunomide, Dorland’s Med.
Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=27821 (last visited
Mar. 12, 2026).
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Petitioner’s next follow up with Dr. Chimata was September 9, 2020. Pet. Ex. 4 at 11.
He was doing well on Arava with minimal stiffness in the mornings. Id. His anemia was also
stable. Id. Dr. Chimata noted that Petitioner was seen by Dr. Desai who was also monitoring
Petitioner for thalassemia. Id.
On September 22, 2020, Petitioner underwent an MRI of his left knee which revealed a
chronic anterior cruciate ligament (“ACL”) tear. Pet. Ex. 5 at 28.
Petitioner attended a tele-health visit with Dr. Mirza on November 2, 2020, with
complaints of a sore throat and inflamed tonsils with pus. Pet. Ex. 19 at 132. He had
discontinued taking Arava due to this acute infection on instruction from his rheumatologist. Id.
at 133. Petitioner was diagnosed with tonsillitis and prescribed amoxicillin. Id. at 135-36.
On December 9, 2020, Petitioner attended a follow-up appointment with Dr. Chimata and
was reportedly doing well on Arava. Pet. Ex. 4 at 8. Dr. Chimata advised Petitioner he would
need to stop his medications for 90 days to plan a pregnancy, otherwise his treatment plan
remained unchanged. Id. at 8-10. He returned to see Dr. Chimata on March 10, 2021 for refills
and bloodwork. Id. at 5. He was noted to be stable. Id.
Petitioner received a Covid-19 vaccine on April 1, 2021. Pet. Ex. 5 at 1. He immediately
developed symptoms, including fever, fatigue, chest pain, and sore throat. Pet. Ex. 19 at 90-91.
He then began to develop abdominal pain, diarrhea, low grade fever, and chills three days post-
vaccination, followed by sore throat and fever. Id. at 91. He was seen by his PCP on April 9,
2021, complaining of nasal congestion, sore throat, cough, and right-sided chest pain and had a
temperature of 102.9ºF. Id. Physical examination was positive for erythema of the throat. Id. at
93. Petitioner tested positive for Covid-19. Id. at 120-21; Pet. Ex. 18 at 92. He received
monoclonal antibody infusions due to his immunosuppressant therapy (Arava). Pet. Ex. 18 at
12-81; Pet. Ex. 4 at 2.
On May 4, 2021, Petitioner followed up with Dr. Chimata. Pet. Ex. 4 at 2. Petitioner
reported his recent Covid vaccination and infection, for which he temporarily discontinued his
Arava, as well as increased fatigue. Id. His pain level was a 0/10. Id. He received refills of his
medications. Id.
Petitioner saw Dr. Mirza for his annual physical on June 10, 2021. Pet. Ex. 19 at 21.
Petitioner reported that he recovered well from Covid-19. Id. On that date, it was documented
that he continued to see Dr. Chimata for RA and that he took Arava daily. Id. at 21, 24. No
musculoskeletal complaints were noted on review of systems or physical examination. Id. at 24-
26. Assessment included seronegative RA. Id. at 27-28.
No additional relevant records have been filed.
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2. Petitioner’s Declaration27
Petitioner filed an undated declaration on October 14, 2022. Pet. Ex. 1. Petitioner
averred that he was born November 16, 1982. Id. at ¶ 1. He received the flu vaccination at issue
on November 11, 2019. Id. at ¶ 2. Approximately eight days later, he began to have “severe and
painful muscle and joint stiffness all over [his] body.” Id. at ¶ 3. His “arms, fingers, hands,
knees, shoulders, hips, thighs, legs, and feet were so stiff [he] had difficulty moving them.” Id.
His condition became progressively worse. Id. Petitioner sought care from an orthopedic
physician group and was diagnosed with a “possible torn meniscus.” Id. at ¶¶ 4-5. Since this
diagnosis did not explain his other pain, Petitioner sought a second opinion. Id. at ¶ 5.
On December 10, 2019, Petitioner saw rheumatologist Dr. Chimata and reported his
symptoms and the progression of his illness. Pet. Ex. 1 at ¶ 7. In January 2020, Dr. Chimata
diagnosed him with seronegative RA and elevated ESR. Id. at ¶ 9. She prescribed methotrexate
and sulindac. Id. Petitioner expressed his concern that the flu vaccine triggered his RA. Id. His
medication was changed to Arava and sulindac. Id. at ¶ 14.
Petitioner explained that he continues to suffer from “debilitating joint stiffness.” Pet.
Ex. 1 at ¶ 17. His illness “interferes with every aspect of his life.” Id. Because Arava causes a
risk of birth defects, in order to have another child, he will have to quit taking the medication.
Id. Further, he is unable to “enjoy vacationing at ski resorts because [his] physical limitations
are made worse in higher elevations and cold weather.” Id. His “immune system in also highly
compromised” and this makes him fearful of illnesses. Id. In conclusion, Petitioner averred that
his “vaccination injury has made [him] undergo painful, stressful, and devasting life
experiences” and “has deteriorated [his] quality of life.” Id.
Petitioner maintained that he did not experience any of these symptoms prior to his flu
vaccination, that his symptoms continued for more than six months, and continued to the day he
executed the declaration. Pet. Ex. 1 at ¶ 18.
D. Expert Reports28
1. Petitioner’s Expert, Dr. David Axelrod29
a. Background and Qualifications
Dr. Axelrod is a clinical immunologist board certified in internal medicine, adult
rheumatology, and allergy and immunology. Pet. Ex. 22 at 1. He received his M.D. at the
27 Although titled an affidavit, this document was not notarized, and therefore, it is referenced
herein as a declaration.
28 For the sake of brevity, the undersigned discusses only the most relevant portions of the expert
reports and only the most pertinent references.
29 Dr. Axelrod submitted two expert reports. Pet. Exs. 22, 53.
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University of Michigan Medical School and his M.S. in Clinical Research Design and Statistical
Analysis at the University of Michigan School of Public Health. Id.; Pet. Ex. 48 at 1. He then
completed an internal medicine residency at University of Toronto School of Medicine and
William Beaumont Hospital. Pet. Ex. 48 at 1. Dr. Axelrod completed a fellowship in clinical
immunology, which included adult rheumatology, allergy and immunology, and medical
laboratory immunology, at McGill University. Id. He also worked as a medical staff fellow in
the clinical immunology laboratory at the National Institutes of Health (“NIH”). Id. Dr. Axelrod
held academic appointments from 1982 to 2010, as well as other non-academic positions
throughout his career before retiring in January 2018. Id. at 2. Although he is currently retired
from patient care, as a clinician he was “involved with the diagnosis and treatment of individuals
with drugs reactions (including to vaccines).” Pet. Ex. 22 at 1. Dr. Axelrod has authored or co-
authored several publications. Pet. Ex. 48 at 3-4.
b. Diagnosis
Dr. Axelrod defined RA as an “autoimmune disease that may result in destruction of
synovial joints, with resultant severe disability and premature mortality.” Pet. Ex. 22 at 7
(emphasis omitted). Although joint damage is not usually seen in the early stages of RA, as the
disease progresses, “the classification criteria tend to accumulate over time.” Id. Criteria for
diagnosis include “at least [one] joint with definite clinical synovitis (swelling)” that is “not
better explained by another disease.” Id.
Citing the 2010 ACR/EULAR diagnostic criteria, Dr. Axelrod explained that patients
with a score less than six (out of ten) do not have definite RA, but subsequent assessments may
establish criteria that are “fulfilled cumulatively over time.” Pet. Ex. 22 at 7 (citing Pet. Ex. 23
at 2 tbl.92.1). These criteria are set forth below:
Id. (citing Pet. Ex. 23 at 2 tbl.92.1).
Reviewing Petitioner’s medical records, Dr. Axelrod noted that on December 10, 2019,
Petitioner saw Dr. Chimata for joint pain. Pet. Ex. 22 at 8. Dr. Chimata noted wrist tenderness,
tenderness at the metacarpophalangeal (“MCP”) and proximal IP (“PIP”) joints of the first,
second, third, fourth and fifth digits, and swelling and tenderness at the metatarsophalangeal
(“MTP”) joints of both feet. Id. (emphasis omitted). Although Petitioner tested negative/normal
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for RF and ACPA, he had elevated CRP and ESR levels. Id. Applying the 2010 ACR/EULAR
criteria, Dr. Axelrod calculated a score of 7, based on swelling of at least one joint, no other
disease implicated, more than 10 joints involved, elevated CRP and ESR, and duration of greater
than six weeks. Id. Thus, Dr. Axelrod opined that Petitioner met the diagnostic criteria for RA.
Id.; Pet. Ex. 53 at 5.
Dr. Axelrod further explained that Petitioner underwent a diagnostic work up, including
labs and X-rays, which was negative for an “alternative cause” of his synovitis. Pet. Ex. 22 at 8-
9. Dr. Axelrod acknowledged that while negative tests are not conclusive as to other causes,
they “provide[] a low probability” of alternative causes. Id. at 9.
Moving to the fact that Petitioner had seronegative RA, Dr. Axelrod described relevant
diagnostic criteria developed by Gera and Muley. Pet. Ex. 22 at 9 (citing Pet. Ex. 24). Gera and
Muley explained that the diagnosis of seronegative RA is challenging because “chronic synovitis
is nonspecific” and found in many diseases. Pet. Ex. 24 at 1. Due to this difficulty, and the need
to identify patients with seronegative RA early to institute treatment, the authors developed
classification criteria. Id. at 1-2. They sent questionnaires to rheumatologists to obtain
information about how they made the diagnosis of seronegative RA in their patients. Id. The
responses of 50 rheumatologists were analyzed and used to develop recommended diagnostic
criteria, which require (1) chronic inflammatory polyarthritis30 (five or more joints on
examination), (2) elevated ESR and/or CRP, (3) absence of RF and ACPAs, and (4) one to three
of the following: (a) absence of spondyloarthropathy,31 (b) synovitis confirmed by
ultrasonography or MRI, (c) absence of clinical features of connective tissue disease and
negative ANA, and (d) absence of hepatitis C virus, hepatitis B surface antigen, HIV,
tuberculosis, and leprosy. Id. at 3-4.
Dr. Axelrod opined Petitioner met the Gera and Muley diagnostic criteria. Pet. Ex. 22 at
10. Petitioner had chronic inflammatory polyarthritis in more than five32 joints, he had elevated
CRP and ESR, he was negative for RF and ACPAs, and his records did not suggest
spondylarthritis, psoriasis, or connective tissue disease, his ANA was negative, and he did not
have hepatitis B or C, HIV, tuberculosis, or leprosy. Id.
30 Polyarthritis is “inflammation of several joints together.” Polyarthritis, Dorland’s Med.
Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=40045 (last visited
Mar. 12, 2026).
31 Spondyloarthropathy is the “disease of the joints of the spine.” Spondyloarthropathy,
Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=
46736 (last visited Mar. 12, 2026).
32 Dr. Axelrod’s report stated Petitioner had “chronic inflammatory polyarthritis with
documented joint swelling of more than 4 joints on examination.” Pet. Ex. 22 at 10 (emphasis
added). This appears to be a typographical error. If it is not, this fact is not determinative to the
undersigned’s Decision.
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Respondent’s expert, Dr. Matloubian, questioned the diagnosis of RA due to Petitioner’s
“atypical presentation.” Resp. Ex. A at 7-9. In response, Dr. Axelrod referenced portions of
Petitioner’s medical records showing the presence of joint swelling of the fingers, tenderness of
the IP joints of thumb and index fingers, and elevated CRP and ESR inflammatory markers. Pet.
Ex. 53 at 1. Petitioner had morning stiffness, especially in his feet and neck, indicating
inflammation. Id. Additionally, Petitioner had swelling of the knee and MTP joints of both feet.
Id. Dr. Axelrod also observed that Dr. Chimata documented that Petitioner’s small and medium
joints were involved, which is “typical of [RA]” and not osteoarthritis. Id.
Another point raised by Dr. Matloubian was the acute nature of Petitioner’s onset, which
he opined was not consistent with RA. Resp. Ex. A at 9. Dr. Axelrod disagreed and cited
Brasington and Miner, who noted that 10-25% of RA patients experience sudden onset instead of
gradual progression. Pet. Ex. 53 at 2 (citing Pet. Ex. 55 at 6 (“The clinical course of RA follows
an onset of disease that may be abrupt and acute, gradual and insidious, or subacute between
these extremes. A gradual onset is most common (at least 50% of cases); a sudden onset is much
less common (10%–25%).”)).
Dr. Matloubian also questioned Petitioner’s complaints of muscle pain, which he stated
was not typical of RA. Resp. Ex. A at 7. In response, Dr. Axelrod explained that RA can begin
with “an extra-articular or non-articular manifestation, such as myalgia (pain in the muscles).”
Pet. Ex. 53 at 2 (citing Pet. Ex. 55 at 6 (noting RA “may [] start as an extraarticular or
nonarticular manifestation”)).
Dr. Axelrod also disagreed with Dr. Matloubian’s opinion that that fact Petitioner’s
symptoms did not worsen when he stopped taking Arava undermined the diagnosis of RA. Resp.
Ex. A at 8-9; Pet. Ex. 53 at 2. Petitioner held Arava during periods he was ill with acute
streptococcal tonsilitis (diagnosed on November 2, 2020) and Covid-19 (April 2021). Resp. Ex.
A at 8-9; Pet. Ex. 53 at 2. Dr. Axelrod noted, however, that subsequent records show Petitioner
restarted Arava once his fever and infection symptoms subsided and he has continued to require
Arava, which he opined is evidence that Petitioner continued to require treatment for his RA.
Pet. Ex. 53 at 2.
c. Causation
i. Althen Prong One
Dr. Axelrod offered two mechanistic theories of causation. The first is “[v]accine
induced cytokine damage to the synovium.” Pet. Ex. 22 at 11. In his first expert report, Dr.
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Axelrod did not discuss this theory and instead referenced six papers, discussed in more detail
below.33 Id.
Choy explained the cause of RA is “unknown.” Pet. Ex. 30 at 1. The pathogenesis is
complex, involving “T cells, B cells[,] and the orchestrated interaction of pro-inflammatory
cytokines” including TNF-α and IL-6. Pet. Ex. 30 at 12. “These cytokines are messengers that
activate and differentiate effector cells that cause local and systemic symptoms associated with
the disease.” Id. at 7. IL-17 was also identified as a “potent cytokine that promotes synovitis.”
Id. at 1. Choy detailed the complex process whereby bones are destroyed in RA. Id. at 5. Choy
did not identify vaccines or the flu vaccine in his paper, nor specifically as a cause of RA or a
cause of cytokine induction.
Continuing with cytokines, Foti34 described them as “cell-signaling proteins that affect
the biological function of cells and processes such as inflammation, a variety of immune
responses, and [] wound healing activity.” Pet. Ex. 27 at 1. Foti provided a brief description of
cytokine activity in RA and discussed the effectiveness of agents that block certain cytokines.
Id. at 19-23. Biologic agents that block cytokines IL-6 and TNF-α have had some success in the
treatment of RA; however, the results are not uniform. Id. at 19-21. Approximately “one-third
of patients with RA treated with anti-TNFα agents did not respond.” Id. Foti did not discuss
vaccines or offer an opinion about whether vaccines can induce or activate cytokines to cause
RA.
Yamaguchi et al.35 examined the role of IL-6 in synovial fluid following the “induction
of ischemic osteonecrosis” in children with ischemic osteonecrosis of the femoral head. Pet. Ex.
29 at 1, 8. Hip MRIs revealed the presence of synovitis and additional studies showed elevated
33 Some studies were less relevant than others. Papoudas et al. described a novel way to study
complex concepts related to gene position (i.e. linear proximity), gene regulation, and gene
expression, “through the combination of topological and functional information into bipartite
networks.” Pet. Ex. 28 at 1 (Stylianos Mavropoulos Papoudas et al., Monitoring the Prolonged
Tnf Stimulation in Space and Time with Topological-Functional Networks, 18 Comput. &
Struct. Biotech. J. 220 (2020)). The study used RNA sequencing of “sustained [tumor necrosis
factor (“TNF”)] stimulation of mouse synovial fibroblasts” to “identify unexpected regulatory
changes taking place in the cells” after “prolonged exposure of fibroblasts to [TNF].” Id. at 1-3.
The authors do not suggest that this experiment, or the use of prolonged exposure of fibroblasts
to TNF was meant to simulate the effects of vaccination. See id. at 1-9. Instead, the goal of the
study was to determine whether the “bipartite networks” described provided “insight on the
functional modularity of gene expression profiles” and “genome organization.” Id. at 9.
34 Maria Foti, Introduction to Cytokine as Tissue Regulators in Health and Disease, in Cytokine
Effector Functions in Tissues 3 (Maria Foti & Massimo Locati eds., 2017).
35 Ryosuke Yamaguchi et al., HIF-1-Dependent IL-6 Activation in Articular Chondrocytes
Initiating Synovitis in Femoral Head Ischemic Osteonecrosis, 98 J. Bone & Joint Surgery 1122
(2016).
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IL-6 in synovial fluid. Id. at 8. The study suggested a “link between the induction of femoral
head ischemia and the production of IL-6 from articular chondrocytes due to HIF-1α activation,
which stimulates an inflammatory response from synovial cells.” Id. However, Dr. Axelrod
does not explain how ischemia resulting in death and necrosis of the femoral head, leading to the
production of IL-6 activation, is comparable to vaccination. See Pet. Ex. 22 at 11. There is no
suggestion here that RA involves an ischemic mechanism which leads to bone death, thus
stimulating cytokine activation.
Moving to the flu vaccine, Dr. Axelrod cited Christian et al.,36 a study that compared
cytokine responses after vaccination in 28 pregnant and 28 non-pregnant women. Pet. Ex. 26 at
1. The study showed there were significant increases in cytokine IL-6, and an increase in TNF-
α, with peak responses at day one post-vaccination. Id. There were no differences in the
cytokine responses between pregnant and non-pregnant women. Id. From a clinical viewpoint,
the results were “consistent with prior data showing that inflammatory responses to [trivalent flu]
vaccination [were] mild and transient in pregnant women.” Id. at 6. The authors did not address
any association between the flu vaccination and induction of RA.
Although Dr. Axelrod cited the above papers in support of his proffered cytokine theory,
he did not offer any opinions based on these papers in his first report. See Pet. Ex. 22 at 11. For
example, he did not opine that the flu vaccine produces or activates cytokines such that they
cause or significantly contribute to the induction of RA. See id. Further, he did not state that he
held his opinions to a preponderant or more likely than not standard. See generally id. In his
second report, relevant to cytokines, Dr. Axelrod stated that “[w]ith regard to damage to the
synovia, it is possible that the elevated cytokine levels caused damage to the synovia.” Pet. Ex.
53 at 6 (citing Pet. Ex. 22 at 11). Regarding his opinions related to his cytokine theory, Dr.
Axelrod did not state that he held the opinions to a preponderant standard. See generally Pet.
Exs. 22, 53.
The second mechanism offered by Dr. Axelrod is molecular mimicry. Pet. Ex. 22 at 12-
16. Dr. Axelrod cited papers that discuss molecular mimicry, some of which are general in
nature and some that are more specific; however, none address the question of whether the flu
vaccine can cause RA via molecular mimicry. See id. He referenced Xia et al.37 who “showed
that [flu] hemagglutinin [(“HA”)38] could inhibit binding of type II collagen to the T-cell
receptor, suggesting a possible role of [flu] [HA] in the activation of autoreactive T-cells[] in
36 Lisa M. Christian et al., Serum Proinflammatory Cytokine Responses to Influenza Virus
Vaccine Among Women During Pregnancy Versus Non-Pregnancy, 70 Am. J. Reprod.
Immunol. 45 (2013).
37 L. Xia et al., Altered Influenza Virus Haemagglutinin Peptides Inhibit T Cell Responses to
Type II Collagen in Rheumatoid Arthritis, 64 Ann. Rheum. Dis. 1790 (2005).
38 HA is “an agglutinin, e.g., an antibody or lectin, that agglutinates erythrocytes.”
Hemagglutinin, Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/dorland/
definition?id=21684 (last visited Mar. 12, 2026).
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[RA].” Id. at 12 (citing Pet. Ex. 34). Xia et al. did not study the flu vaccine; they examined the
effect of altered flu virus HA with respect to T-cell receptors/T-cell responses to type II collagen
in RA. See Pet. Ex. 34. Dr. Axelrod did not explain how the study is comparable to vaccination.
See Pet. Ex. 22 at 12. Further, Dr. Axelrod characterized the conclusion he derived from Xia et
al. as “possible” and not likely or probable. Id.
Next, Dr. Axelrod suggested “there is an expectation that vaccine peptides are likely to
align with human peptides, including those that act as target autoantigens for [RA].” Pet. Ex. 22
at 12. However, Dr. Axelrod did not provide foundational literature which suggested that
vaccines in general, or the flu vaccine specifically, can induce RA via peptide homology.
In lieu of articles that discuss a role for vaccines in the pathogenesis of RA, Dr. Axelrod
generally referenced articles about molecular mimicry. Pet. Ex. 22 at 12-13. Johnson et al.39
define autoimmune illnesses as rare conditions “in which immune responses to specific self-
antigens contribute the ongoing tissue damage.” Pet. Ex. 31 at 1. These are adaptive immune
responses, “usually directed against exogenous antigens—but its targets are autoantigens.” Id.
Although the foreign antigens may be structurally different from self-antigens, they may share
“significant similarity in focal regions,” which may allow for cross-reactive responses. Id. at 6.
This is a broad general statement about molecular mimicry that does not speak to vaccination or
vaccine-induced RA.
Next, Dr. Axelrod cited Kanduc et al.40 for the proposition that “viruses (including [flu]
virus) share proteomes (peptides) with the human proteome.” Pet. Ex. 22 at 12 (citing Pet. Ex.
32). Kanduc et al. wrote molecular mimicry is a hypothesis, suggesting that when viruses (and
bacteria) share proteins with a host, “an immune response against the infectious agent may result
in formation of cross-reacting antibodies that bind the shared epitopes on the normal cell and
result in the auto-destruction of the cell.” Pet. Ex. 32 at 11. Dr. Axelrod similarly cited Trost et
al.41 for the proposition that “bacteria share proteomes with the human proteome.” Pet. Ex. 22 at
12 (citing Pet. Ex. 33).
Dr. Axelrod cited Rojas et al., which discussed molecular mimicry and autoimmunity in
various autoimmune diseases. Pet. Ex. 22 at 12 (citing Pet. Ex. 63). Although the authors
discussed RA, they do not discuss vaccines in the context of RA or otherwise provide an opinion
about any association between vaccines, and particularly the flu vaccine, and RA. Dr. Axelrod
did not explain how the paper was relevant to RA. Dr. Axelrod similarly cited a review of
39 Tory P. Johnson et al., Mechanisms of Autoimmunity, in Clinical Immunology: Principles and
Practice 649 (Robert R. Rich et al. eds., 6th ed. 2022).
40 Darja Kanduc et al., Massive Peptide Sharing Between Viral and Human Proteomes, 29
Peptides 1755 (2008).
41 Brett Trost et al., Bacterial Peptides Are Intensively Present Throughout the Human Proteome,
1 Self/Nonself 71 (2010).
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molecular mimicry from Martins et al.,42 which does not mention or discuss RA, nor did Dr.
Axelrod explain its relevance to RA. Id. (citing Pet. Ex. 35).
Dr. Axelrod cited other papers about T-cell function and recognition, antigen
presentation, and major histocompatibility complex (“MHC”) molecules43 (including discussion
of the design and effectiveness of vaccines), the optimum length of peptides, and other related
subjects, but these papers did not discuss how the flu vaccine could cause RA by the mechanism
of molecular mimicry. See Pet. Ex. 36;44 Pet. Ex. 37;45 Pet. Ex. 38;46 Pet. Ex. 39;47 Pet. Ex.
40.48
More specific to RA, Dr. Axelrod cited Yoshida et al.,49 stating that “the authors found
evidence to suggest that human Type II Collagen acts as an autoantigen” in RA patients. Pet. Ex.
22 at 14 (citing Pet. Ex. 41); see also Pet. Ex. 53 at 7. Yoshida et al. explained that RA is
“associated with citrullination, which is the conversion of arginine residues into citrulline
residues.” Pet. Ex. 41 at 1. Citrullination is important in protein degradation, “as molecular
interactions that are mediated by positively charged arginine residues are lost upon
citrullination.” Id. The study showed that type II collagen was citrullinated in joints affected by
RA, and that these patients had autoantibodies to citrullinated type II collagen. Id. at 1, 4.
42 Yuri Chaves Martins et al., Visiting Molecular Mimicry Once More: Pathogenicity, Virulence,
and Autoimmunity, 11 Microorganisms 1 (2023).
43 MHC is “the genes determining the major histocompatibility antigens, in all species a group of
closely linked multiallelic genes located in a small region on one chromosome.” Major
Histocompatibility Complex, Dorland’s Med. Dictionary Online,
https://www.dorlandsonline.com/dorland/definition?id=66341 (last visited Mar. 12, 2026).
44 Abul K. Abbas et al., Cellular and Molecular Immunology 117-44 (9th ed. 2018).
45 Andrea J. Sant, Overview of T-Cell Recognition: Making Pathogens Visible to the Immune
System, in Clinical Immunology: Principles and Practice 93 (Robert R. Rich et al. eds., 5th ed.
2019).
46 J. Linsday Whitton et al., Molecular Analyses of a Five-Amino-Acid Cytotoxic T-Lymphocyte
(CTL) Epitope: An Immunodominant Region Which Induces Nonreciprocal CTL Cross-
Reactivity, 63 J. Virol. 4303 (1989).
47 Bernhard Hemmer et al., Minimal Peptide Length Requirements for CD4+ T Cell Clones—
Implications for Molecular Mimicry and T Cell Survival, 12 Int’l Immunol. 375 (2000).
48 Sune Frankild et al., Amino Acid Similarity Accounts for T Cell Cross-Reactivity and for
“Holes” in the T Cell Repertoire, 3 PLoS ONE e1831 (2008).
49 Mamoru Yoshida et al., Autoimmunity to Citrullinated Type II Collagen in Rheumatoid
Arthritis, 16 Mod. Rheumatol. 276 (2006).
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“Immunocomplexes[50] composed of fragments of citrullinated type II collagen and
autoantibodies were formed and deposited in the inflamed articular synovium of RA patients.”
Id. at 4. Whether these immunocomplexes played a role in RA disease pathogenesis was not
determined. Id. at 4-5.
Employing the UniProtKB database,51 Dr. Axelrod compared protein sequence alignment
between HA from two flu strains in the vaccine administered to Petitioner52 with peptides from
human synovial membrane (Trefoil factor family peptide or TFF3)53 and peptides from rabbit
synovial membranes (using “human equivalents”).54 Pet. Ex. 22 at 14-16, apps. A1-A7; Pet.
Exs. 43-44. He identified seven examples of amino acid alignment between the flu B strain of
the flu vaccine and peptides from human equivalents (of peptides from the synovial membranes
of rabbits). Pet. Ex. 22 at 15-16, apps. A1-A7. The amino acid sequences varied in length (from
3 to 13 consecutive amino acids). Id. Based on his research, Dr. Axelrod concluded that the flu
50 Immunocomplexes, also known as antigen-antibody complexes, are “formed by the
noncovalent binding of an antibody and an antigen. Complexes of antibodies belonging to
certain immunoglobulin classes may activate complement. Antigen-antibody complexes are
mediators of type III immune responses (Arthus reactions, serum sickness, and immune complex
diseases).” Antigen-Antibody Complex, Dorland’s Med. Dictionary Online,
https://www.dorlandsonline.com/dorland/definition?id=66292 (last visited Mar. 12, 2026).
51 “The UniProt Knowledgebase (UniProtKB) is the central hub for the collection of functional
information on proteins, with accurate, consistent[,] and rich annotation. In addition to capturing
the core data mandatory for each UniProtKB entry (mainly, the amino acid sequence, protein
name or description, taxonomic data[,] and citation information), as much annotation information
as possible is added.” UniProtKB, https://www.uniprot.org/help/uniprotkb (last modified Nov.
25, 2025).
52 Dr. Axelrod provided the following chart for reference.
Hemagglutinin from Influenza strain UniProtKB Entry ID
A/Brisbane/02/2018 (H1N1)pdm09-like
A/Kansas/14/2017 (H3N2)-like
B/Colorado/06/2017-like (Victoria lineage) A0A1X9RX59
B/Phuket/3073/2013-like (Yamagata lineage) A4D5Q0
Pet. Ex. 22 at 14. For more information on UniProtKB and entry identifiers, see UniProtKB,
https://www.uniprot.org/help/uniprotkb (last modified Nov. 25, 2025).
53 See Pet. Ex. 43 (Judith Popp et al., Human Synovia Contains Trefoil Factor Family (TFF)
Peptides 1–3 Although Synovial Membrane Only Produces TFF3: Implications in Osteoarthritis
and Rheumatoid Arthritis, 20 Int’l J Mol. Scis. 1 (2019)).
54 See Pet. Ex. 44 (Weilin Liu et al., Differential Proteomics of the Synovial Membrane Between
Bilateral and Unilateral Knee Osteoarthritis in Surgery-Induced Rabbit Models, 14 Mol. Med.
Reps. 2243 (2016)).
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vaccine shared “similar consecutive amino acid sequences with synovial antigens.” Id. at 16.
Dr. Axelrod opined this data provided “scientific evidence to link the [flu] vaccination received
by [Petitioner] and an immune reaction to synovial autoantigens, including Type II Collagen that
is considered an autoantigen for [RA].” Pet. Ex. 53 at 4.
Regarding molecular mimicry, Dr. Axelrod did not state that he held his opinions to a
preponderant or more likely than not standard.
In his second report, Dr. Axelrod responded to Dr. Matloubian’s critique of his opinions.
Regarding Dr. Axelrod’s cytokine theory, Dr. Matloubian’s primary criticism was that the flu
vaccine here (inactivated and non-adjuvanted) does not cause “persistent or high level[s] of
cytokine production,” and therefore, it would be unlikely for it to cause joint damage. Resp. Ex.
A at 12. In response, Dr. Axelrod cited Christian et al., which he asserted showed that the flu
vaccine did cause elevated cytokine levels. Pet. Ex. 53 at 6 (citing Pet. Ex. 26). Dr. Axelrod
opined that “it is possible that the elevated cytokine levels cause[s] damage to the synovia.” Id.
Dr. Axelrod also offered rebuttal opinions to Dr. Matloubian’s criticisms of his molecular
mimicry theory. One criticism by Dr. Matloubian was that of the seven peptides proposed, “only
vimentin and collagen have been identified as targets of autoreactive T-cells in [RA].” Pet. Ex.
53 at 8; Resp. Ex. A at 15. Even so, Dr. Axelrod opined “[i]f attacked by the adaptive immune
response, damage with inflammation to the synovium would be an outcome.” Pet. Ex. 53 at 8.
Another concern by Dr. Matloubian about Dr. Axelrod’s sequence research was that
TFF3 has not been identified an antigen that causes disease in RA. Resp. Ex. A at 15. Further,
Dr. Axelrod failed to indicate the beginning and ending point of his proposed peptides. Dr.
Matloubian also took issue with Dr. Axelrod’s failure to account for how “peptides are generated
and presented to T cells,” which renders “comparing simple sequence homology
immunologically meaningless.” Id. While the undersigned does not summarize the details of the
experts’ discussions on the details of these immunological points, the following quote by Dr.
Axelrod is notable. Dr. Axelrod stated, “[p]erhaps the limited probability that similar sequences
will align with the central position of autoreactive T-cell receptors contributes to the safety of the
vaccines.” Pet. Ex. 53 at 10.
In response to Dr. Matloubian’s opinion that there was “no evidence of an association”
between the flu vaccine and RA, Dr. Axelrod did not identify case reports or other articles that
discussed any such association. Instead, he identified exhibits that he referenced in his first
report that discussed cytokines and molecular mimicry. Pet. Ex. 53 at 3 (citing Pet. Ex. 22 at 11
(relative to cytokines), 12-14 (relative to molecular mimicry)). Dr. Axelrod reiterated that he
provided evidence of the “molecular basis for associating the sequences of [HA]” based on his
research of similar amino acid sequences. Id.
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In response to Dr. Matloubian’s opinion that infections have not been shown to induce
RA, Dr. Axelrod cited Mankia et al.,55 who reported an association between P. gingivalis
bacterial infection periodontal disease and RA. Pet. Ex. 53 at 5 (citing Pet. Ex. 54 at 1). Dr.
Axelrod did not explain, however, how P. gingivalis infection and periodontal disease and the
association between this condition and RA provides evidence in support of an association
between the flu vaccine and RA.
Next, regarding the studies cited by Dr. Matloubian supporting the safety profile of the
flu vaccine, Dr. Axelrod agreed that the inactivated flu vaccination “appears to be safe,” but
explained this finding does not “preclude an individual from developing [RA] as a result of [the]
[] vaccine.” Pet. Ex. 53 at 4. He discussed the limitations of epidemiology studies, bias, sample
size, and Type I and Type II errors, concluding that the “absence of evidence, [is] not evidence
of absence.” Id. (emphasis omitted).
Specifically related to the study by Ray et al.,56 Dr. Axelrod stated that the authors
“found that [flu] vaccination measurably increased the risk of developing [RA].” Pet. Ex. 53 at 6
(citing Pet. Ex. 61). However, this statement appears to be inaccurate. Ray et al. reported that
“[i]n [their] initial cohort analysis, [they] found a possible association between RA and [the] [flu]
vaccine in the previous 180 or 365 days, but the extended case-control analysis, bringing in more
data, did not demonstrate this increase.” Pet. Ex. 61 at 5.
Dr. Axelrod also quoted Ray et al. stating “[i]ndividual cases of RA and other
autoimmune disease occurring after vaccination have been reported for years.” Pet. Ex. 53 at 6
(quoting Pet. Ex. 61 at 4). The quote is accurate, but the references cited and examples
following the quote do not describe the flu vaccine and RA; instead, the references describe the
flu vaccine and Guillain-Barré Syndrome (“GBS”), the live virus rubella vaccine and arthritis,
hepatitis vaccination and RA, and hepatitis B vaccination and Sjogren’s syndrome. See Pet. Ex.
61 at 4-5. Ray et al. did not find or report that the flu vaccine was causally associated with RA.
Dr. Matloubian asserted that “RA-related autoimmunity and inflammation are present
long before [disease] onset,” referencing a 2019 review from Deane and Holers.57 Resp. Ex. A
at 9 (citing Resp. Ex. A-6) (emphasis omitted). Dr. Axelrod disagreed, characterizing these
“immunological changes” as “susceptibility factors” that occur in individuals who “may or may
not develop [RA].” Pet. Ex. 53 at 4-5. Dr. Axelrod cited a 2021 paper by Deane and Holers that
stated most people who develop seropositive RA have elevated RA-related antibodies for a
55 Kulveer Mankia et al., Prevalence of Periodontal Disease and Periodontopathic Bacteria in
Anti-Cyclic Citrullinated Protein Antibody-Positive At-Risk Adults Without Arthritis, 2 JAMA
Network Open 1 (2019).
56 Paula Ray et al., Risk of Rheumatoid Arthritis Following Vaccination with Tetanus, Influenza
and Hepatitis B Vaccines Among Persons 15–59 Years of Age, 29 Vaccine 6592 (2011). This
study was also cited as Resp. Ex. A-9.
57 Kevin D. Deane & V. Michael Holers, The Natural History of Rheumatoid Arthritis, 41 Clin.
Ther. 1256 (2019).
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period prior to the clinical manifestation of symptoms, suggesting not all people with RA-related
antibodies develop RA. Id. at 5 (citing Pet. Ex. 58). Here, it seems both experts agree, although
Dr. Axelrod referenced this “pre-RA” phase as a susceptibility, whereas Dr. Matloubian viewed
it as a pre-clinical phase of the illness.
Relative to molecular mimicry, Dr. Matloubian cited Rose,58 who stated that although
there are examples of molecular mimicry triggering “a defined model of autoimmune disease in
experimental animals,” these occurrences are “still relatively rare in humans.” Pet. Ex. 53 at 7
(quoting Resp. Ex. A-19 at 1); see also Resp. Ex. A at 14. Examples of molecular mimicry in
humans include rheumatic fever and Streptococcus pyogenes, GBS and Campylobacter jejuni,
and possibly narcolepsy and the flu vaccine. Id. at 3. Dr. Axelrod does not take issue with Dr.
Rose’s conclusion that these are rare events or the fact that evidence of homology supporting
molecular mimicry is often lacking. See id. at 4.
Dr. Matloubian cited a paper authored by Malmström et al., who reported that T-cell
activation by an antigen from the flu virus was similarly activated in both normal patients and
RA patients (seropositive). Resp. Ex. A at 14-15; Pet. Ex. 53 at 7 (citing Resp. Ex. A-20 at 7).
This finding weighs against Dr. Axelrod’s theory of molecular mimicry, and in response, Dr.
Axelrod cited Xia et al. for the suggestion that there is a “possible” role of flu virus HA “in the
activation of autoreactive T-cells” in RA because Xia et al. showed flu HA could inhibit binding
of Type II collagen to the T-cell receptor. Pet. Ex. 53 at 7 (citing Pet. Ex. 34). Dr. Axelrod also
cited Yoshida et al., who “found evidence to suggested human Type II Collagen acts as an
autoantigen in [RA].” Id. (citing Pet. Ex. 41). Dr. Axelrod stated, “[t]hese studies suggest that
peptides derived from [flu] [HA] can activate autoreactive T-cells to participate in the
development of [RA].” Id.
ii. Althen Prong Two
Dr. Axelrod opined that Petitioner has RA, and thus, he had the “susceptibilities
required” to develop RA including “the presence of synovial autoreactive T-cells [in] his
peripheral immune system.” Pet. Ex. 22 at 16; see also Pet. Ex. 53 at 5. According to Dr.
Axelrod, Petitioner received the flu vaccine which contained flu HA that “share[d] similar
consecutive amino acid sequences with synovial antigens.” Pet. Ex. 22 at 16. “The [flu] [HA]
activated [Petitioner’s] autoreactive T-cells, allowing those cells to escape his tolerance
mechanisms and attack his synovial cells, resulting in synovitis, with the clinical picture of
[RA].” Id.
As it relates to molecular mimicry, Dr. Axelrod asserted that “Type II Collagen acts as an
autoantigen” in RA, and that both “citrullinated and non-citrullinated type antibodies” have been
found in “serum and synovium” of RA patients. Pet. Ex. 22 at 14. Thus, “[i]t is not
inconceivable that [Petitioner] has these antibodies in his synovial tissue, without being able to
detect them in his serum.” Id.
58 Noel R. Rose, Negative Selection, Epitope Mimicry and Autoimmunity, 49 Curr. Op.
Immunol. 51 (2017).
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Regarding the cytokine theory, Dr. Axelrod opined that the flu vaccine increased
Petitioner’s cytokine levels, which “may have caused his pain symptoms in the hours and days”
following vaccination. Pet. Ex. 22 at 16. The increased cytokine levels caused “some damage to
his synovium, with release of synovial antigens, which activated his autoreactive T-cells to his
synovium,” resulting in synovitis and RA. Id. Although the sequences identified by Dr. Axelrod
(in his searches for homology between HA and human proteins) cannot be tested to determine
whether they would result in T-cell activation, Dr. Axelrod opined that Petitioner “did develop
[RA] following his November 11, 2019 [flu] vaccination. Therefore, he must have presented
[flu] [HA] peptides to autoreactive T-cells, if his [RA] was induced by the [flu] vaccination.”59
Pet. Ex. 53 at 10.
Dr. Axelrod opined that, other than vaccination, Petitioner did not have an alternate cause
for his RA. Pet. Ex. 22 at 17. While Dr. Chimata documented on December 10, 2019, that
Petitioner had a sore throat about the time of vaccination (November 11, 2019), the more
contemporaneous records (December 3, 2019 and December 5, 2019) do not reference
complaints of a sore throat. Id.; Pet. Ex. 53 at 2. Records from December 3 and December 5 do
not document complaints of a sore throat or reveal a physical examination consistent with a sore
throat. Pet. Ex. 22 at 17. The records also do not show that Petitioner had inflammation,
lymphadenopathy, or receive diagnostic testing or treatment for a sore throat or infection. Id.
Thus, Dr. Axelrod concluded Petitioner did not have an alternative cause for his synovitis or RA.
Id.; Pet. Ex. 53 at 2, 12-15.
Dr. Axelrod disagreed with Dr. Matloubian’s opinion that Petitioner had a viral infection
which led to transient inflammatory arthritis. Pet. Ex. 53 at 2. Further, Dr. Axelrod stated there
was no evidence that Petitioner had an infection until November 2, 2020, almost one year after
vaccination, when he had streptococcal tonsillitis. Id.
Relevant to Althen prong two, Dr. Axelrod did not state that he held his opinions to a
preponderant standard. See Pet. Exs. 22, 53.
iii. Althen Prong Three
Dr. Axelrod opined that Petitioner developed RA “abruptly, without laboratory evidence
of inflammation prior to the onset of his clinical disorder.” Pet. Ex. 53 at 5, 15. Whatever
caused Petitioner’s RA “likely [occurred] in proximity to the time” that he first developed
symptoms of RA. Id. at 15. Dr. Axelrod opined that if Petitioner’s onset of RA was one or two
days after vaccination, it was consistent with “cytokine release following vaccination.” Id. If,
however, onset was four or eight days after vaccination, onset was “consistent with a secondary
adaptive immune response.” Id. He agreed that the notes regarding time intervals in Petitioner’s
records closer in time to vaccination are “consistent with a secondary adaptive immune
response” (molecular mimicry). Id. at 6.
59 Dr. Axelrod and Dr. Matloubian engaged in a significant colloquy about what is required for
molecular mimicry and T-cell activation. See Pet. Ex. 53 at 10-11; Resp. Ex. A at 14-21. A
summary of that discussion is omitted for the sake of brevity.
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Petitioner had pain in his spine, shoulders, hips, knees and hands eight days after
vaccination, on November 19, 2019, according to Petitioner’s affidavit. Pet. Ex. 22 at 21 (citing
Pet. Ex. 1). Dr. Axelrod opined “[t]his time interval [was] a bit short for a primary adaptive
immune response,” but “consistent with a secondary adaptive immune response” to the flu
vaccine administered November 11, 2019. Id.
On December 5, 2019, Petitioner reported he had experienced widespread pain for the
past few weeks, which would place onset approximately November 15, four days post-
vaccination. Pet. Ex. 22 at 21. Dr. Axelrod opined that a time interval of four days is also
“consistent with a secondary adaptive immune response” to his flu vaccination. Id.
Related to the adaptive immune response and molecular mimicry, Dr. Axelrod referenced
several papers60 showing that after a “booster” vaccination,61 the secondary adaptive immune
response, characterized by increased antibody levels (of a “greater magnitude than the primary
adaptive immune response”), begins at two to four days post-vaccination, increasing through
eight days, and remaining elevated from 14 to 22 days. Pet. Ex. 22 at 18-20.
In the alternative, using Dr. Chimata’s note on December 10, 2019, Dr. Axelrod opined
that Petitioner had experienced pain for four weeks, which would place onset one or two days
after vaccination. Pet. Ex. 22 at 21. This time frame, according to Dr. Axelrod, “is too short for
a secondary adaptive immune response,” but consistent with an innate immune response and
“symptoms expected from the elevated cytokines.” Id. Dr. Axelrod concluded that Petitioner
developed an “innate immune response with elevated cytokines that caused his early symptoms
and activated his autoreactive T-cells (to the synovia), driving them out of the control of his
immune tolerance mechanisms, allowing him to cause immune damage to his synovia, with
resultant synovitis and a clinical picture of [RA].” Id. at 22.
60 See Pet. Ex. 36; Pet. Ex. 45 (John J. Miller et al, The Speed of the Secondary Immune
Response to Tetanus Toxoid with a Review of War Reports and Observations on Simultaneous
Injection of Toxoid and Antitoxin, 3 Pediatrics 64 (1949)); Pet. Ex. 46 (Asia Wyatt & Doron
Levy, Modeling the Effect of Memory in the Adaptive Immune Response, 82 Bull. Math. Biol.
124 (2020)).
61 A booster response, or a secondary immune response, refers to “the immune response
occurring on the second and subsequent exposures to an antigen; compared to a primary immune
response, the lag period is shorter, the peak antibody titer is higher and lasts longer, IgG
production predominates, the antibodies produced have a higher affinity for the antigen, and a
much smaller dose of the antigen is required to initiate the response.” Immune Response,
Secondary, Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/dorland/
definition?id=103686 (last visited Mar. 12, 2026). Dr. Axelrod did not provide evidence that the
flu vaccine at issue here was a “booster vaccination.” He did not explain how or why his
discussion of a booster vaccination and/or secondary adaptive immune response was relevant
here.
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Dr. Axelrod cited a paper about cytokines produced in the context of flu infection, not
vaccination. See Pet. Ex. 25.62 Hayden et al. showed that when humans are infected with the flu
A virus, they release cytokines IL-6 and TNF-α (found in serum) in the first three days, which
“correlate[] directly with viral titers, temperature, mucus production, and symptoms scores”
during this timeframe. Id. at 1.
Dr. Axelrod also cited studies showing that cytokines IL-6 and TNF-α peak one day after
vaccination and up to seven days when there is a “shift from an acute inflammatory response to a
more generalized function of the immune system.” Pet. Ex. 22 at 18 (citing Pet. Exs. 26, 28)
(emphasis omitted). He also cited Yamaguchi et al. for the proposition that IL-6 induced other
proinflammatory cytokines (IL-1 β and TNF-α), “with increased proliferation of synovial cells at
24 and 48 hours.” Id. (citing Pet. Ex. 29). Based on these studies, Dr. Axelrod further opined
that it was “possible” that “elevated cytokine levels caused damage to the synovia.” Pet. Ex. 53
at 6 (citing Pet. Ex. 22 at 11).
In summary, Dr. Axelrod opined that the onset of Petitioner’s symptoms was consistent
with an innate response and a secondary adaptive immune response to the flu vaccination. Pet.
Ex. 22 at 22. Dr. Axelrod further opined that “[Petitioner] developed [RA] following his [flu]
vaccination of November 11, 2019. Therefore, whatever caused his [RA] was likely in
proximity to the time that he developed the first symptoms of [RA]” and “[t]he only new
environmental exposure prior to the onset of [RA] was the [flu] vaccination.” Pet. Ex. 53 at 15.
Regarding causation, Dr. Axelrod did not state in either of his expert reports that he held
his opinions to a preponderant evidence or “more likely than not” standard. See Pet. Exs. 22, 53.
2. Respondent’s Expert, Dr. Mehrdad Matloubian63
a. Background and Qualifications
Dr. Matloubian is a “physician-scientist with basic science training in virology and
immunology and clinical training in adult rheumatology.” Resp. Ex. A at 1. He is board
certified in rheumatology and internal medicine. Resp. Ex. B at 1-2. He received his M.D. as
well as a Ph.D. in virology/immunology from University of California, Los Angeles. Resp. Ex.
A at 1; Resp. Ex. B at 1. Since 2001, he has taught at the University of California, San Francisco
where he is now a Professor. Resp. Ex. B at 2. Dr. Matloubian’s research for the past 20 years
has been focused on “innate and adaptive immune responses, including those of T and B cells, to
acute and chronic viral infections.” Resp. Ex. A at 1. “[His] areas of expertise include T and B
cell responses, especially to viruses as well as factors that regulate lymphocyte circulation and
trafficking.” Id. He has published numerous peer-reviewed articles in these areas. Id.; see Resp.
Ex. B at 10-17. “As an immunologist and board-certified rheumatologist who actively evaluates
62 Frederick G. Hayden et al., Local and Systemic Cytokine Responses During Experimental
Human Influenza A Virus Infection, 101 J. Clin. Invest. 643 (1998).
63 Dr. Matloubian submitted one expert report. Resp. Ex. A.
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and treats patients with complex autoimmune diseases[,] . . . [Dr. Matloubian] [is] qualified to
address both diagnostic and immunological issues regarding these diseases.” Resp. Ex. A at 1.
b. Diagnosis
Before offering an opinion about diagnosis, Dr. Matloubian summarized Petitioner’s pre-
vaccination history. Resp. Ex. A at 1-2, 6. Before vaccination, based on available records from
Saudi Arabia, Petitioner took “multiple rounds” of antibiotics from 2016 through 2018. Id. at 2,
6. He also had abnormalities in his lungs seen on chest X-rays in 2017. Id.
Petitioner received the flu vaccine at issue on November 11, 2019. Resp. Ex. A at 2, 6.
He had documented swelling and tenderness in his thumbs and DIP joints of his index fingers
within three weeks of his flu vaccination, and steroids were prescribed. Id. at 6 (citing Pet. Ex.
19 at 270). Petitioner also had elevated inflammatory markers (ESR and CRP). Id. (citing Pet.
Ex. 19 at 272-77). Subsequently, Petitioner was seen by rheumatologist Dr. Chimata, who noted
joint tenderness in the hands and a swollen joint in the foot. Id. (citing Pet. Ex. 4 at 24). Dr.
Chimata diagnosed Petitioner with seronegative RA and prescribed treatment with methotrexate
followed by Arava, resulting in a favorable result. Id.
Dr. Matloubian questioned Petitioner’s diagnosis of seronegative RA. Resp. Ex. A at 6-
9. When seen by Dr. Nolan on December 3, 2019, Petitioner’s physical examination did not
reveal swollen joints. Id. at 7 (citing Pet. Ex. 3 at 8). Two days later, on December 5, Petitioner
was seen by Dr. Hodges who noted that Petitioner had swelling and tenderness in the small joints
of his hands. Id. (citing Pet. Ex. 19 at 270). Petitioner had elevated inflammatory markers, but
these were “nonspecific.” Id. Dr. Matloubian explained that because the lab results were non-
specific, the results “do not distinguish between inflammation due to a recent infection or an
autoimmune inflammatory process.” Id. On December 10, 2019, while Petitioner was taking
steroids, Petitioner was seen by Dr. Chimata who documented “only one swollen small joint of
the foot” and a small knee effusion. Id. (citing Pet. Ex. 4 at 24). Dr. Matloubian also noted
these findings were non-specific, though he agreed they “could be consistent with an
inflammatory arthritis, such as RA.” Id.
In addition to findings that were non-specific, Dr. Matloubian believed that Petitioner’s
presentation was “atypical” of RA. Resp. Ex. A at 7. Petitioner reported severe muscle pain,
which Dr. Matloubian opined is not typical in RA since RA primarily affects joints and not
muscles. Id. Another unusual feature of Petitioner’s presentation was that his pain began in his
neck, shoulders, and hips, before it moved to his hands, knees, and feet. Id. According to Dr.
Matloubian, most patients report symptoms in the small joints before larger joints. Id. (citing
Resp. Ex. A-3 at 2, 4, 9).64 Next, Dr. Matloubian noted that when seen by Dr. Hodges on
December 5, 2019, Petitioner had tenderness in the DIP joints of the index fingers. Id. at 8. Dr.
Matloubian opined this is not characteristic of RA, since it “rarely, if ever, involves the [DIP]
joints.” Id. (citing Resp. Ex. A-3 at 4-5).
64 James R. O’Dell et al., Rheumatoid Arthritis, in Current Diagnosis & Treatment in
Rheumatology (John Imboden et al. eds., 3d ed. 2013).
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Due to Petitioner’s “atypical presentation,” and because he had an antecedent sore throat,
Dr. Matloubian suggested Petitioner “possibly had a virus associated transient arthritis that was
labeled as seronegative RA.” Resp. Ex. A at 8. Dr. Matloubian opined that Petitioner responded
well to Arava and did well when he discontinued Arava, suggesting his condition was transient.
Id. Moreover, Petitioner was prescribed 10 mg per day, and Dr. Matloubian opined that the
“typical dose” for RA is 20 mg per day. Id. at 23. As to whether Petitioner was able to
discontinue Arava, Dr. Matloubian noted he only reviewed Petitioner’s medical records through
June 2021 and had not reviewed updated records, and thus, he acknowledged his opinions were
limited in time to events occurring up until June 2021.65 Id. at 8. He issued a caveat and noted
that if updated records showed that Petitioner developed a recurrence of symptoms after
discontinuing immunosuppressive theory, this would support a diagnosis of chronic
inflammatory arthritis (RA). Id.
Dr. Matloubian did not dispute Dr. Axelrod’s opinion that Petitioner satisfied the
ACR/EULAR 2010 criteria for the diagnosis of RA, “especially since he was observed to have at
least one swollen joint on physical examination.” Resp. Ex. A at 9. However, Dr. Matloubian
opined that the diagnosis of seronegative RA is “challenging” and “requires careful longitudinal
observation for confirmation.” Id. While he believed it was “possible” that Petitioner was
correctly diagnosed, Petitioner’s atypical presentation combined with the lack of recurrence of
symptoms when Arava was discontinued, “suggest[ed] a more likely transient inflammatory
arthritis.” Id.
c. Causation
i. Athen Prong One
Dr. Matloubian disagreed that the flu vaccine is “associated with the development [] of
RA.” Resp. Ex. A at 10. He explained that the causes of RA are not known; however,
“established and evolving research” suggests there is a “pre-RA” phase and that “RA-related
autoimmunity and inflammation are present long before” onset of symptoms. Id. at 9 (quoting
Resp. Ex. A-6 at 2) (emphasis omitted). Thus, there is a “breakdown of tolerance and []
autoimmunity” years before swollen joints develop. Id. (emphasis omitted).
In support, Dr. Matloubian cited studies showing that “RA-related autoantibodies are
detectable . . . 3-5 years before” symptoms are “clinically detectable.” Resp. Ex. A at 9 (quoting
Resp. Ex. A-6 at 2) (emphasis omitted); see also Pet. Ex. 31 at 1 (“[S]ignificant recent data from
longitudinal studies have demonstrated that the onset of autoimmune responses and the
development of clinical symptoms are separated in time.”). Deane and Holers wrote that “[i]t is
now well established that RA develops in a series of phases.” Resp. Ex. A-6 at 1. The first
phase is characterized by genetic and/or environmental risk factors, “in the absence of detectable
systemic autoimmunity” such as autoantibodies or inflammatory markers. Id. The second phase,
65 No additional medical records were filed documenting treatment related to RA after June
2021. Records from Houston Methodist Oncology Group after June 2021 were filed, but do not
speak to the issue of whether Petitioner continued to take Arava or have a recurrence of
symptoms if he discontinued Arava. See generally Pet. Ex. 21.
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or propagation phase, is notable for “autoimmunity, inflammation, and symptoms.” Id. This
leads to “clinically detectable inflammatory arthritis . . . classified as RA.” Id. Studies have
shown that ‘”RA-related autoantibodies are detectable in the circulation a mean of 3-5 years”
before symptoms of inflammatory arthritis occur. Id. at 2. Based on this current knowledge, Dr.
Matloubian opined “it is [] highly likely that factors that trigger and propagate RA-related
autoimmunity [and] drive the transition from pre-RA to [RA] are acting years before diagnosis.”
Resp. Ex. A at 10 (emphasis omitted). Smoking has been identified as a major risk factor,
“which is thought to act years before transition to clinical RA.” Id.
Further, Dr. Matloubian stated that acute infections have not been shown to induce RA.
Resp. Ex. A at 10. He acknowledged that there are references to acute infections in the
literature, but opined there is no conclusive evidence that they trigger RA. Id. Dr. Matloubian
further opined that based on currently available literature, the flu virus has not been shown to
cause RA. Id. (citing Resp. Ex. A-4 (listing viruses that cause arthritis and not listing the flu
virus);66 Resp. Ex. A-8 (same)).67 For these reasons, “RA is not a post-infectious disease.” Id.
After opining that infections are not thought to cause RA, Dr. Matloubian opined there is
no association between vaccines and RA, specifically the flu vaccine and RA, and discussed
studies in support. Resp. Ex. A at 10-11. Ray et al. conducted a large study of one million
Kaiser Permanente Northern California patients and found no association between hepatitis B,
tetanus, and flu vaccinations and RA. Pet. Ex. 61 at 1, 4. The study employed a retrospective
chart review with cohort and case-control analysis (of ages 15 to 59) from 1997 to 1999. Id. at 1.
A “possible association” between the flu vaccination and RA was seen in the range of 180 and
365 days after vaccination in the cohort analysis, but in the larger case-control analysis, this
association was not seen. Id.
Fomin et al.,68 a small study with case controls, studied the efficacy of the flu vaccine
given to patients with RA being treated with disease modifying drugs. Resp. Ex. A-10 at 1.
Vaccination did not cause significant worsening of symptoms or adversely affect inflammatory
markers. Id. at 4.
66 Terry L. Moore & Reema Syed, Viruses That Cause Arthritis, UpToDate,
https://www.uptodate.com/contents/viruses-that-cause-arthritis?search=viral+arthritis&topic
Ref=5614&source=see_link (last updated Nov. 27, 2018).
67 Terry L. Moore, Viral Arthritis: Approach to Evaluation and Management, UpToDate,
https://www.uptodate.com/contents/viral-arthritis-approach-to-evaluation-and-management?
search=viral+arthritis&topicRef=5584&source=see_link (last updated Feb. 11, 2019).
68 I. Fomin et al., Vaccination Against Influenza in Rheumatoid Arthritis: The Effect of Disease
Modifying Drugs, Including TNFα Blockers, 65 Ann. Rheum. Dis. 191 (2006).
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Bengtsson et al.69 conducted a larger study of 1,998 Swedish RA patients with matched
controls (2,252) and found no increased risk of RA after vaccinations, including the flu, tetanus,
diphtheria, and hepatitis vaccinations. Resp. Ex. A-11 at 1-2. The study group included patients
with and without ACPAs. Id. Vaccinations did not increase the risk of RA in a control group or
in patients with a history of smoking who are at higher risk of developing RA. Id. at 2.
And Westra et al.70 showed that vaccination is effective and safe in patients with
autoimmune inflammatory rheumatic diseases to prevent vaccine preventable diseases, even in
patients being treated with immunomodulatory drugs. Resp. Ex. A-14 at 8.
Based on these studies and others, the ACR in 2015 issued guidelines for patients with
RA who were beginning or receiving disease modifying treatment or biologic agents,
recommending use of killed vaccines (like the flu vaccine) and live attenuated vaccines (herpes
zoster vaccine). Resp. Ex. A-15 at 17 fig.8, 18.71
In summary, based on multiple studies, Dr. Matloubian concluded that “no association
has been found” between vaccinations, including the flu vaccination, and RA. Resp. Ex. A at 11.
Next, Dr. Matloubian addressed Dr. Axelrod’s theories based on cytokines and molecular
mimicry. Starting with the cytokine theory, especially IL-6 and TNF-α, Dr. Matloubian opined
that the literature does not support such a theory. Resp. Ex. A at 12. Christian et al. showed that
while there were post-vaccination elevations of cytokines IL-6 and TNF-α, the peak occurred
one day after vaccination and was transient. Id. (citing Pet. Ex. 26 at 5). No safety issues were
associated with the increased cytokines. See id. (citing Pet. Ex. 26 at 6). Thus, Dr. Matloubian
opined the findings by Christian et al. do not support the idea that an inactivated non-adjuvanted
flu vaccine causes levels of cytokines that lead to joint damage. Id.
Dr. Matloubian also commented on Papoudas et al., who studied TNF-α effects on mouse
synovial cells and showed that it changed expression of proteins in these cells. Resp. Ex. A at 12
(citing Pet. Ex. 28 at 2). However, Dr. Matloubian explained the study did not show that low or
transient levels of TNF-α can cause joint injury. Id.
Dr. Matloubian disagreed that Yamaguchi et al. supported Petitioner’s cytokine theory.
Resp. Ex. A at 13. Yamaguchi et al. studied the role of IL-6 in synovial fluid in children with
ischemic osteonecrosis of the femoral head. Pet. Ex. 29 at 1, 8. Hip MRIs revealed the presence
of synovitis and additional studies showed elevated IL-6 in synovial fluid. Id. at 8. The study
69 Camilla Bengtsson et al., Common Vaccinations Among Adults Do Not Increase the Risk of
Developing Rheumatoid Arthritis: Results from the Swedish EIRA Study, 69 Ann. Rheum. Dis.
1831 (2010).
70 Johanna Westra et al., Vaccination of Patients with Autoimmune Inflammatory Rheumatic
Diseases, 11 Nat. Rev. Rheumatol. 135 (2015).
71 Jasvinder A. Singh et al., 2015 American College of Rheumatology Guideline for the
Treatment of Rheumatoid Arthritis, 68 Arthritis Care & Rsch. 1 (2016).
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suggested a “link between the induction of femoral head ischemia and the production of IL-6
from articular chondrocytes.” Id. Dr. Matloubian opined that the study does not support vaccine
causation due to cytokine effects but instead shows that surgically induced injury that causes
joint damage can lead to inflammation that involves the production of IL-6. Resp. Ex. A at 13.
Hayden et al. studied cytokine responses to flu A virus infection and showed that IL-6
peaked at two days and returned to baseline between four to eight days after infection. Resp. Ex.
A at 12 (citing Pet. Ex. 25 at 4). TNF-α peaked three days after infection and returned to
baseline between days four to eight. Id. (citing Pet. Ex. 25 at 4). If Petitioner’s cytokine theory
was likely, Dr. Matloubian opined that RA would be commonly associated with flu infections,
but it is not. Id.
While Dr. Matloubian agreed that IL-6 and other proinflammatory cytokines may be
elevated during infections, after surgery, and in patients with certain autoimmune illnesses, these
instances or illnesses “differ in their pathogenic mechanism.” Resp. Ex. A at 13. Further, he
opined that elevated IL-6 levels “seem[] to be a consequence of multiple disease processes,” and
“not the triggering cause.” Id.
Moreover, Dr. Matloubian explained that if Dr. Axelrod’s cytokine hypothesis—that
vaccinations (including the flu vaccine) increase IL-6 leading to disease or worsening of
symptoms—was well founded, then ACR and others in the medical community would not
recommend vaccinations (including the flu vaccine) to patients with RA and other autoimmune
diseases. Resp. Ex. A at 13. For support, Dr. Matloubian cited Westra et al., who showed that
vaccination is effective and safe in patients with autoimmune inflammatory rheumatic diseases to
prevent vaccine preventable diseases, even in patients being treatment with immunomodulatory
drugs. Resp. Ex. A-14 at 8. Dr. Matloubian also cited to 2015 ACR guidelines recommending
vaccinations, including inactivated killed vaccines (flu) and live attenuated vaccines (herpes
zoster), to RA patients following review of numerous studies. Resp. Ex. A-15 at 17 fig.8, 18.
Regarding Dr. Axelrod’s molecular mimicry theory, Dr. Matloubian summarized
Petitioner’s theory: RA was caused by activation of flu specific T cells, which through the
mechanism of molecular mimicry, “recognized joint associated self-antigens” and induced
seronegative RA. Resp. Ex. A at 14 (citing Pet. Ex. 22 at 16, 22). More specifically, Dr.
Axelrod suggested that the flu vaccine “share[d] similar consecutive amino acid sequences with
synovial antigens. The [flu vaccine] [HA] activated [] autoreactive T cells, allowing those cells
to escape [] tolerance mechanisms and attack [] synovial cells,” causing synovitis and resulting
in RA. Id. (citing Pet. Ex. 22 at 16). Dr. Matloubian disagreed with this theory.
First, although natural infections have been shown to cause autoimmune illness via
molecular mimicry, the natural flu virus infection has not been demonstrated to cause RA. Resp.
Ex. A at 14. Since there is no cause-and-effect link between the flu infection and RA, Dr.
Matloubian argued it is not probable (“exceedingly improbable”) that antigens from the natural
infection contained in the flu vaccine could cause RA via molecular mimicry. Id. (emphasis
omitted). He explained that flu antigens are not thought to be associated with RA. Id. In fact,
this is why research studies about autoreactive T cells in RA patients use antigens derived from
the flu virus as a control. Id. (citing Resp. Ex. A-20 at 7 (noting studies have shown “reactivity
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to an unrelated antigen (from [flu] virus) was similar between healthy controls and patients with
RA”)).
Second, Dr. Matloubian noted he is not aware of any reliable evidence in medical
literature or from his experience caring for RA patients, suggesting that RA occurs after flu
infections or flu vaccination. Resp. Ex. A at 10, 14. As described above, based on his review of
the relevant studies, Dr. Matloubian concluded that “multiple controlled studies have shown that
immunizations do not lead to development of RA . . . [or] lead to exacerbation of symptoms in
those who already suffer from this disease.” Id. at 11.
Moving to Dr. Axelrod’s sequence homology research, Dr. Matloubian raised several
concerns. Of the peptide sequences identified, Dr. Matloubian stated that “only vimentin and
collagen have been identified as targets of autoreactive T cells in RA.” Resp. Ex. A at 15. There
was no evidence provided by Dr. Axelrod to show that the other proteins identified are
“biologically relevant to the pathogenesis of RA.” Id.
Next, Dr. Matloubian opined that simply having homologous protein sequences between
pathogen and host is not sufficient to achieve molecular mimicry. Resp. Ex. A at 15 (citing Pet.
Ex. 35 at 5). Without information about “how peptides are generated and presented to T cells,” it
is not meaningful to simply compare sequence homology.72 Id. Therefore, showing that the flu
vaccine shares short sequences of amino acids with the synovium “does not constitute evidence
for molecular mimicry.” Id. at 16, 18-20.
Further, Dr. Matloubian takes issue with Dr. Axelrod’s suggestion that molecular
mimicry can occur with similarity as opposed to complete identity. Resp. Ex. A at 18.
According to Dr. Matloubian, even one amino acid difference in a peptide sequence can
significantly affect the ability of the peptide to activate T cells. Id. Thus, he disagreed that
similar but not identical sequences support molecular mimicry for T cells.73 Id. at 18-19.
Moreover, the critical and identical amino acids must be “at a specific position within a peptide.”
Id. at 19-20.
72 For Dr. Matloubian’s discussion of how peptides are presented to T cells and what is required
for molecular mimicry to occur, see Resp. Ex. A at 15-22.
73 For support of this aspect of Dr. Matloubian’s opinion, see Resp. Ex. A-23 (Mark A. Daniels
et al., Thymic Selection Threshold Defined by Compartmentalization of Ras/MAPK Signalling,
444 Nature 724 (2006)); Resp. Ex. A-24 (Amitabh Gaur et al., Amelioration of Relapsing
Experimental Autoimmune Encephalomyelitis with Altered Myelin Basic Protein Peptides
Involves Different Cellular Mechanisms, 74 J. Neuroimmunol. 149 (1997)); Resp. Ex. A-25
(Nathan Karin et al., Reversal of Experimental Autoimmune Encephalomyelitis by a Soluble
Peptide Variant of a Myelin Basic Protein Epitope: T Cell Receptor Antagonism and Reduction
of Interferon γ and Tumor Necrosis Factor α Production, 180 J. Exp. Med. 2227 (1994)); Resp.
Ex. A-26 (Vijay K. Kuchroo et al., A Single TCR Antagonist Peptide Inhibits Experimental
Allergic Encephalomyelitis Mediated by a Diverse T Cell Repertoire, 153 J. Immunol. 3326
(1994)).
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Dr. Axelrod cited Xia et al., stating they showed “a possible role of [flu] [HA] in the
activation of autoreactive T-cells[] in RA.” Resp. Ex. A at 21 (quoting Pet. Ex. 22 at 12, 14)
(citing Pet. Ex. 34); see also Pet. Ex. 53 at 7. Dr. Matloubian opined Dr. Axelrod’s interpretation
of Xia et al. as a “misinterpretation of the findings” for several reasons. Resp. Ex. A at 21. First,
the study did not suggest molecular mimicry between flu HA and collagen peptides. Id. at 22.
Second, “[t]he residues of a peptide that bind to MHC molecules are distinct from those that are
recognized by T cells.” Id. (quoting Pet. Ex. 36 at 25). Dr. Matloubian explained that “just
because two peptides bind to the same MHC/HLA molecule, does not mean that they are going
to be recognized by the same T cell” or constitute a molecular mimic of each other. Id.
According to Dr. Matloubian, Xia et al. “took advantage of this fact and altered the [flu] HA
peptide so that it [could] bind to HLA-DR1/4 but not be recognized by T cells.” Id. The altered
peptide ligand74 binds to “a specific MHC/HLA molecule with high affinity,” thus preventing the
binding by a pathogenic self-peptide, like collagen, to prevent T cells that recognize the
autoantigens from being activated. Id. at 22, 23, fig. 6.
Dr. Matloubian summarized that
Dr. Axelrod opine[d] that Petitioner “developed RA due to vaccine induced
cytokine damage to joints leading to activation of autoreactive T cells as well as
through molecular mimicry between [flu] HA and components of the joint.
However, natural infection with [flu] virus induces higher and more prolonged
levels of cytokines . . . than vaccination, yet, it has not been established to cause
RA. Since [flu] vaccines contain the same antigens as the wild-type [flu] virus, it
is unlikely that [the flu] vaccination would induce RA through molecular mimicry
when the [flu] virus itself does not. Moreover, . . . peptide sequence homologies
and even extensive identities do not reliably demonstrate molecular mimicry even
under a more likely than not standard.
Resp. Ex. A at 25.
ii. Althen Prong Two
Dr. Matloubian opined that Petitioner’s inflammatory arthritis diagnosed as seronegative
RA was not caused by his flu vaccination. Resp. Ex. A at 25. He further opined that “[t]he
cause of RA is not known and [he] [did] not know what caused [P]etitioner’s inflammatory
arthritis.” Id. at 23.
While Dr. Matloubian does not know the cause of Petitioner’s RA, he discussed a
possible alternate cause for his illness: a viral infection that led to a “transient virus associated
74 A ligand is “a molecule that binds to another molecule, used especially to refer to a small
molecule that binds specifically to a larger molecule, e.g., an antigen binding to an antibody, a
hormone or neurotransmitter binding to a receptor, or a substrate or allosteric effector binding to
an enzyme.” Ligand, Dorland’s Med. Dictionary Online, https://www.dorlandsonline.com/
dorland/definition?id=28261 (last visited Mar. 12, 2026).
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inflammatory arthritis” instead of seronegative RA. Resp. Ex. A at 23. This opinion, however,
was not stated as more likely than not, but as a “possibility.” Id.
Dr. Matloubian referenced medical records documenting that Petitioner had a sore throat
prior to his vaccination. Resp. Ex. A at 22. Although he discussed the possibility of a viral
infection, Dr. Matloubian was careful to explain that Petitioner’s RA was not caused by
infection. See id. at 22-24. However, Dr. Matloubian described a growing body of evidence
suggesting that the gut microbiome75 may be involved in the development of RA. Id. at 24.
Antibiotics can disrupt the “equilibrium of the gut microbiome, which can then indirectly affect
the immune system.” Id. Petitioner’s medical records show that he was treated with “multiple
courses of antibiotics,” presumably for infections prior to the onset of his RA. Id. And
“alteration of the gut microbiome by repeated antibiotic usage” may affect self-tolerance in
susceptible people. Id. Resulting imbalance of “intestinal flora composition of patients with
preclinical and diagnosed RA indicate that the imbalance of intestinal flora may have an
important impact on the induction and persistence of RA.” Id. (quoting Resp. Ex. A-30 at 2).76
Regardless, Dr. Matloubian opined there is no reliable evidence to suggest that either the flu
vaccine or an acute flu infection can cause RA. Id.
Dr. Matloubian concluded that Petitioner’s illness “more likely than not was not a
consequence of his [flu vaccine].” Resp. Ex. A at 25.
iii. Althen Prong Three
Dr. Matloubian opined that “RA develops for several years before symptoms manifest.”
Resp. Ex. A at 25. Therefore, he opined that, more likely than not, Petitioner developed RA
before his flu vaccination on November 11, 2019. Id.
Regarding clinical symptom manifestation, Dr. Matloubian cited Petitioner’s affidavit
and excerpts from the medical records which provide inconsistent references to symptom onset.
Resp. Ex. A at 24-25. Beginning with his affidavit, Petitioner averred he developed muscle and
joint pain approximately eight days after his flu vaccination. Id. at 24 (citing Pet. Ex. 1 at 1).
Then, the medical records show Petitioner called Dr. Nolan requesting a prescription for
Motrin on November 25, 2019, approximately 14 days post-vaccination. Resp. Ex. A at 24
(citing Pet. Ex. 15 at 6).
75 Dr. Matloubian defined the microbiome as “the collection of all microbes, especially bacteria
that constantly live on our external and internal body surfaces that are open to the environment.”
Resp. Ex. A at 24.
76 Yanhui Peng et al., Associations Between Rheumatoid Arthritis and Intestinal Flora, with
Special Emphasis on RA Pathologic Mechanisms to Treatment Strategies, 188 Microb. Pathog. 1
(2024).
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On December 5, 2019, Dr. Hodges took a history that noted Petitioner had joint pain for
the “past few weeks,” which would place onset approximately November 19, or eight days post-
vaccination. Resp. Ex. A at 24 (quoting Pet. Ex. 19 at 266).
However, on December 10, Dr. Chimata’s history referenced symptoms for the “last 4
weeks” and “for the past 1-2 months.” Resp. Ex. A at 24 (quoting Pet. Ex. 4 at 23). This would
place onset in a range from approximately October 10, 2019 (two month) to November 12, 2019
(four weeks). Id. This range begins pre-vaccination and ends one day after vaccination. Id.
In summary, Dr. Matloubian opined that Petitioner’s onset is not clear. Resp. Ex. A at
25. However, based on the current understanding of the illness, “more likely than not,”
Petitioner’s RA onset predated his flu vaccination. Id.
III. DISCUSSION
A. Standards for Adjudication
The Vaccine Act was established to compensate vaccine-related injuries and deaths. §
10(a). “Congress designed the Vaccine Program to supplement the state law civil tort system as
a simple, fair and expeditious means for compensating vaccine-related injured persons. The
Program was established to award ‘vaccine-injured persons quickly, easily, and with certainty
and generosity.’” Rooks v. Sec’y of Health & Hum. Servs., 35 Fed. Cl. 1, 7 (1996) (quoting
H.R. Rep. No. 908 at 3, reprinted in 1986 U.S.C.C.A.N. at 6287, 6344).
Petitioner’s burden of proof is by a preponderance of the evidence. § 13(a)(1). The
preponderance standard requires a petitioner to demonstrate that it is more likely than not that the
vaccine at issue caused the injury. Moberly v. Sec’y of Health & Hum. Servs., 592 F.3d 1315,
1322 n.2 (Fed. Cir. 2010). Proof of medical certainty is not required. Bunting v. Sec’y of Health
& Hum. Servs., 931 F.2d 867, 873 (Fed. Cir. 1991). Petitioner need not make a specific type of
evidentiary showing, i.e., “epidemiologic studies, rechallenge, the presence of pathological
markers or genetic predisposition, or general acceptance in the scientific or medical communities
to establish a logical sequence of cause and effect.” Capizzano v. Sec’y of Health & Hum.
Servs., 440 F.3d 1317, 1325 (Fed. Cir. 2006). Instead, Petitioner may satisfy his burden by
presenting circumstantial evidence and reliable medical opinions. Id. at 1325-26.
In particular, Petitioner must prove that the vaccine was “not only [the] but-for cause of
the injury but also a substantial factor in bringing about the injury.” Moberly, 592 F.3d at 1321
(quoting Shyface v. Sec’y of Health & Hum. Servs., 165 F.3d 1344, 1352-53 (Fed. Cir. 1999));
see also Pafford v. Sec’y of Health & Hum. Servs., 451 F.3d 1352, 1355 (Fed. Cir. 2006). The
received vaccine, however, need not be the predominant cause of the injury. Shyface, 165 F.3d
at 1351. A petitioner who satisfies this burden is entitled to compensation unless Respondent
can prove, by a preponderance of the evidence, that the vaccinee’s injury is “due to factors
unrelated to the administration of the vaccine.” § 13(a)(1)(B). However, if a petitioner fails to
establish a prima facie case, the burden does not shift. Bradley v. Sec’y of Health & Hum.
Servs., 991 F.2d 1570, 1575 (Fed. Cir. 1993).
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“Regardless of whether the burden ever shifts to the [R]espondent, the special master
may consider the evidence presented by the [R]espondent in determining whether the [P]etitioner
has established a prima facie case.” Flores v. Sec’y of Health & Hum. Servs., 115 Fed. Cl. 157,
162-63 (2014); see also Stone v. Sec’y of Health & Hum. Servs., 676 F.3d 1373, 1379 (Fed. Cir.
2012) (“[E]vidence of other possible sources of injury can be relevant not only to the ‘factors
unrelated’ defense, but also to whether a prima facie showing has been made that the vaccine
was a substantial factor in causing the injury in question.”); de Bazan v. Sec’y of Health & Hum.
Servs., 539 F.3d 1347, 1353 (Fed. Cir. 2008) (“The government, like any defendant, is permitted
to offer evidence to demonstrate the inadequacy of the [P]etitioner’s evidence on a requisite
element of the [P]etitioner’s case-in-chief.”); Pafford, 451 F.3d at 1358-59 (“[T]he presence of
multiple potential causative agents makes it difficult to attribute ‘but for’ causation to the
vaccination. . . . [T]he Special Master properly introduced the presence of the other unrelated
contemporaneous events as just as likely to have been the triggering event as the vaccinations.”).
B. Factual Issues
A petitioner must prove, by a preponderance of the evidence, the factual circumstances
surrounding his claim. § 13(a)(1)(A). To resolve factual issues, the special master must weigh
the evidence presented, which may include contemporaneous medical records and testimony.
See Burns v. Sec’y of Health & Hum. Servs., 3 F.3d 415, 417 (Fed. Cir. 1993) (explaining that a
special master must decide what weight to give evidence including oral testimony and
contemporaneous medical records). 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.” § 13(b)(1)(A).
Contemporaneous medical records, “in general, warrant consideration as trustworthy
evidence.” Cucuras v. Sec’y of Health & Hum. Servs., 993 F.2d 1525, 1528 (Fed. Cir. 1993).
But see Kirby v. Sec’y of Health & Hum. Servs., 997 F.3d 1378, 1382 (Fed. Cir. 2021) (rejecting
the presumption that “medical records are accurate and complete as to all the patient’s physical
conditions”); Shapiro v. Sec’y of Health & Hum. Servs., 101 Fed. Cl. 532, 538 (2011) (“[T]he
absence of a reference to a condition or circumstance is much less significant than a reference
which negates the existence of the condition or circumstance.” (quoting Murphy v. Sec’y of
Health & Hum. Servs., 23 Cl. Ct. 726, 733 (1991), aff’d per curiam, 968 F.2d 1226 (Fed. Cir.
1992))), recons. den’d after remand, 105 Fed. Cl. 353 (2012), aff’d mem., 503 F. App’x 952
(Fed. Cir. 2013).
However, there are situations in which compelling oral testimony may be more
persuasive than written records, such as where records are deemed to be incomplete or
inaccurate. Campbell v. Sec’y of Health & Hum. Servs., 69 Fed. Cl. 775, 779 (2006) (“[L]ike
any norm based upon common sense and experience, this rule should not be treated as an
absolute and must yield where the factual predicates for its application are weak or lacking.”);
Lowrie v. Sec’y of Health & Hum. Servs., No. 03-1585V, 2005 WL 6117475, at *19 (Fed. Cl.
Spec. Mstr. Dec. 12, 2005) (“Written records which are, themselves, inconsistent, should be
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accorded less deference than those which are internally consistent.” (quoting Murphy, 23 Cl. Ct.
at 733)). Ultimately, a determination regarding a witness’s credibility is needed when
determining the weight that such testimony should be afforded. Andreu v. Sec’y of Health &
Hum. Servs., 569 F.3d 1367, 1379 (Fed. Cir. 2009); Bradley, 991 F.2d at 1575.
Despite the weight afforded to medical records, special masters are not rigidly bound by
those records in determining onset of a petitioner’s symptoms. Valenzuela v. Sec’y of Health &
Hum. Servs., No. 90-1002V, 1991 WL 182241, at *3 (Fed. Cl. Spec. Mstr. Aug. 30, 1991); see
also Eng v. Sec’y of Health & Hum. Servs., No. 90-1754V, 1994 WL 67704, at *3 (Fed. Cl.
Spec. Mstr. Feb. 18, 1994) (noting Section 13(b)(2) “must be construed so as to give effect also
to § 13(b)(1) which directs the special master or court to consider the medical records (reports,
diagnosis, conclusions, medical judgment, test reports, etc.), but does not require the special
master or court to be bound by them”).
C. Causation
To receive compensation through the Program, Petitioner must prove either (1) that he
suffered a “Table Injury”—i.e., an injury listed on the Vaccine Injury Table—corresponding to a
vaccine that he received, or (2) that he suffered an injury that was actually caused by a
vaccination. See §§ 11(c)(1), 13(a)(1)(A); Capizzano, 440 F.3d at 1319-20. Petitioner must
show that the vaccine was “not only a but-for cause of the injury but also a substantial factor in
bringing about the injury.” Moberly, 592 F.3d at 1321 (quoting Shyface, 165 F.3d at 1352-53).
Because Petitioner does not allege he suffered a Table Injury, he must prove a vaccine he
received caused his injury. To do so, Petitioner must establish, by preponderant evidence: “(1) a
medical theory causally connecting the vaccination and the injury; (2) a logical sequence of
cause and effect showing that the vaccination was the reason for the injury; and (3) a showing of
a proximate temporal relationship between vaccination and injury.” Althen, 418 F.3d at 1278.
The causation theory must relate to the injury alleged. Petitioner must provide a sound
and reliable medical or scientific explanation that pertains specifically to this case, although the
explanation need only be “legally probable, not medically or scientifically certain.” Knudsen v.
Sec’y of Health & Hum. Servs., 35 F.3d. 543, 548-49 (Fed. Cir. 1994). Petitioner cannot
establish entitlement to compensation based solely on his assertions; rather, a vaccine claim must
be supported either by medical records or by the opinion of a medical doctor. § 13(a)(1). In
determining whether a petitioner is entitled to compensation, the special master shall consider all
material in the record, including “any . . . conclusion, [or] medical judgment . . . which is
contained in the record regarding . . . causation.” § 13(b)(1)(A). The undersigned must weigh
the submitted evidence and the testimony of the parties’ proffered experts and rule in Petitioner’s
favor when the evidence weighs in his favor. See Moberly, 592 F.3d at 1325-26 (“Finders of
fact are entitled—indeed, expected—to make determinations as to the reliability of the evidence
presented to them and, if appropriate, as to the credibility of the persons presenting that
evidence.”); Althen, 418 F.3d at 1280 (noting that “close calls” are resolved in Petitioner’s
favor).
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Testimony that merely expresses the possibility—not the probability—is insufficient, by
itself, to substantiate a claim that such an injury occurred. See Waterman v. Sec’y of Health &
Hum. Servs., 123 Fed. Cl. 564, 573-74 (2015) (denying Petitioner’s motion for review and
noting that a possible causal link was not sufficient to meet the preponderance standard). The
Federal Circuit has made clear that the mere possibility of a link between a vaccination and a
petitioner’s injury is not sufficient to satisfy the preponderance standard. Moberly, 592 F.3d at
1322 (emphasizing that “proof of a ‘plausible’ or ‘possible’ causal link between the vaccine and
the injury” does not equate to proof of causation by a preponderance of the evidence); Boatmon
v. Sec’y of Health & Hum. Servs., 941 F.3d 1351, 1359-60 (Fed. Cir. 2019). While certainty is
by no means required, a possible mechanism does not rise to the level of preponderance.
Moberly, 592 F.3d at 1322; see also de Bazan, 539 F.3d at 1351.
IV. ANALYSIS
A. Diagnosis
As Federal Circuit precedent establishes, in certain cases it is appropriate to determine the
nature of an injury before engaging in the Althen analysis. Broekelschen v. Sec’y of Health &
Hum. Servs., 618 F.3d 1339, 1346 (Fed. Cir. 2010). Since “each prong of the Althen test is
decided relative to the injury [,]” determining facts relating to the claimed injury can be
significant. Id. Here, the parties disagree as to diagnosis. The undersigned finds that
preponderant evidence supports Petitioner’s diagnosis of seronegative RA. There are several
reasons for this finding.
First, Petitioner’s treating rheumatologist made a diagnosis of seronegative RA.
Petitioner saw his rheumatologist, Dr. Chimata, for an initial evaluation in December 2019. Dr.
Chimata noted that Petitioner’s CRP and ESR were abnormal. Physical examination revealed
wrist tenderness and tenderness of the MCP and PIP joints of the fingers without involvement of
the DIP joints. Petitioner had a small knee effusion. He also had tenderness and swelling of the
MTP joints of both of his feet. Testing for RA-related antibodies was ordered. At a follow-up
visit in January 2020, Dr. Chimata diagnosed Petitioner with seronegative RA. Dr. Chimata
continued to see Petitioner at six months intervals, and the diagnosis of seronegative RA
remained consistent. The latest relevant records show that in June 2021, Petitioner continued to
see Dr. Chimata for his RA and continued to take Arava daily. See Pet. Ex. 19 at 21, 24.
Here, the undersigned gives weight to the statements of Petitioner’s treating physician as
she is “in the best position” to determine Petitioner’s injury. See Andreu, 569 F.3d at 1367;
Capizzano, 440 F.3d at 1326; Cucuras, 993 F.2d at 1528 (noting contemporaneous medical
records, “in general, warrant consideration as trustworthy evidence”).
Second, Dr. Axelrod was persuasive in showing why Petitioner’s diagnosis of
seronegative RA was appropriate under the relevant criteria. Applying Dr. Chimata’s physical
examination findings and Petitioner’s lab results to the 2010 ACR/EULAR criteria, Dr. Axelrod
calculated a score of seven, which was based on swelling of at least one joint, involvement of
more than 10 joints, elevated CRP and ESR, symptoms lasting longer than six weeks, and no
other disease implicated, and he concluded that Petitioner met the requirements for RA.
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Furthermore, Dr. Matloubian did not dispute Dr. Axelrod’s opinion that Petitioner satisfied the
ACR/EULAR 2010 criteria for the diagnosis of RA. See Resp. Ex. A at 9.
Using the Gera and Muley classification criteria for seronegative RA and applying the
physical examination findings and labs for Petitioner also shows that Petitioner’s diagnosis of
seronegative RA was appropriate due to documented swelling of five or more joints, elevated
CRP and ESR, and absence of infection, psoriasis, or other disqualifying conditions.
Further, although Dr. Matloubian questioned the diagnosis of seronegative RA due to
Petitioner’s nonspecific findings and atypical presentation, he agreed that Dr. Chimata’s initial
physical examination findings could be consistent with RA.
Moreover, Dr. Matloubian’s opinion suggesting that Petitioner had a transitory
inflammatory arthritis instead of RA was based on a caveat. Dr. Matloubian’s opinion was based
on the assumption that after June 2021, Petitioner did not continue to require Arava for treatment
of his symptoms. Dr. Matloubian did not review records after that date, and no relevant records
were filed that reflect care after that date. Thus, while there is a question about whether
Petitioner continued to take medication for his RA, this question does not negate the fact that
Petitioner required medication for his illness beginning in December 2019, and that he continued
to take the medication diagnosis for his RA through June 2021.
For the above reasons, the undersigned finds Petitioner has proven by preponderant
evidence that his appropriate diagnosis was seronegative RA.
B. Causation
1. Althen Prong One
Under Althen prong o, Petitioner must set forth a medical theory explaining how the
received vaccine could have caused the sustained injury. Andreu, 569 F.3d at 1375; Pafford, 451
F.3d at 1355-56. Petitioner’s theory of causation need not be medically or scientifically certain,
but it must be informed by a “sound and reliable” medical or scientific explanation. Boatmon,
941 F.3d at 1359; see also Knudsen, 35 F.3d at 548; Veryzer v. Sec’y of Health & Hum. Servs.,
98 Fed. Cl. 214, 223 (2011) (noting that special masters are bound by both § 13(b)(1) and
Vaccine Rule 8(b)(1) to consider only evidence that is both “relevant” and “reliable”). If
Petitioner relies upon a medical opinion to support his theory, the basis for the opinion and the
reliability of that basis must be considered in the determination of how much weight to afford the
offered opinion. See Broekelschen, 618 F.3d at 1347 (“The special master’s decision often times
is based on the credibility of the experts and the relative persuasiveness of their competing
theories.”); Perreira v. Sec’y of Health & Hum. Servs., 33 F.3d 1375, 1377 n.6 (Fed. Cir. 1994)
(stating that an “expert opinion is no better than the soundness of the reasons supporting it”
(citing Fehrs v. United States, 620 F.2d 255, 265 (Ct. Cl. 1980))).
The undersigned finds Petitioner failed to provide preponderant evidence of a sound and
reliable theory to explain how the flu vaccination can cause RA.
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First, the undersigned finds there is not preponderant evidence of a causal association
between the flu vaccine and RA. Petitioner did not file a case report, a case series study, or other
medical literature or evidence showing that the flu vaccine can cause RA. Studies filed and
referenced by Respondent also did not show an association between the flu vaccine and RA. For
example, Ray et al. conducted a study involving medical chart review of approximately one
million patients with RA from 1997 to 1999 and found a “possible association” between flu
vaccination and RA with onset periods between six months and one year (180 days to 365 days)
in their cohort analysis but no association in their larger case-control analysis. Bengtsson et al.,
in a large study of 1,998 Swedish RA patients with matched controls (2,252), found no increased
risk of RA after vaccinations, including the flu vaccination. Fomin et al. conducted a small study
on the efficacy of the flu vaccine in RA patients and noted no significant worsening of symptoms
or adversely affect inflammatory markers were seen. Similarly, Westra et al. showed
vaccinations are effective and safe in patients with autoimmune inflammatory rheumatic
diseases.
Although a petitioner need not make a specific type of evidential showing (i.e.,
epidemiologic studies) to satisfy her burden, special masters shall still consider and weigh the
evidence in the record, including the epidemiological studies filed. See § 13(b)(1) (indicating the
special master shall consider all materials in the record); Capizzano, 440 F.3d at 1325-26; Grant
v. Sec’y of Health & Hum. Servs., 956 F.2d 1144, 1149 (Fed. Cir. 1992) (finding
“epidemiological studies are probative medical evidence relevant to causation” and
“considerable weight [is] due to epidemiological studies in the absence of direct evidence of
actual causation”). And after weighing the submitted evidence, the undersigned finds the
evidence does not preponderate in Petitioner’s favor. See Moberly, 592 F.3d at 1325-26
(“Finders of fact are entitled—indeed, expected—to make determinations as to the reliability of
the evidence presented to them and, if appropriate, as to the credibility of the persons presenting
that evidence.”). The undersigned finds the totality of the medical literature evidence presented
demonstrates no association between the flu vaccine and the development of RA.
Second, Petitioner’s expert did not offer his opinions using the preponderant evidence
standard. That is, Dr. Axelrod did not offer his causation opinions to a more likely than not
standard. The few times that he quantified his opinion, he used words suggesting possibility, not
more likely than not. See Pet. Ex. 22 at 12, 14 (referencing Xia et al. and stating they “showed
that [flu] [HA] could inhibit binding of type II collagen to the T-cell receptor, suggesting a
possible role of [flu] [HA] in the activation of autoreactive T-cells[] in [RA]”); Pet. Ex. 22 at 14
(“It is not inconceivable that [Petitioner] has these antibodies in his synovial tissue, without
being able to detect them in his serum.”); Pet. Ex. 53 at 6 (regarding “damage to the synovia, it is
possible that the elevated cytokine levels caused damage”); Resp. Ex. 53 at 10 (“Perhaps the
limited probability that similar sequences will align with the central position of autoreactive T-
cell receptors contributes to the safety of the vaccines.”). Opinions based on possibilities are
insufficient to prove causation. See Waterman, 123 Fed. Cl. 564, 573-74; Moberly, 592 F.3d at
1322; de Bazan, 539 F.3d at 1351.
Lastly, the undersigned’s finding that Petitioner has failed to provide preponderant
evidence of causation is consistent with case law regarding vaccination (including but not limited
to the flu vaccine) and RA. See, e.g., Hock v. Sec’y of Health & Hum. Servs., No. 17-168V,
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2020 WL 6392770, at *23-25 (Fed. Cl. Spec. Mstr. Sept. 30, 2020) (discussing numerous
reasoned Program decisions that have dismissed petitions alleging the flu vaccine can cause RA);
Aultman v. Sec’y of Health & Hum. Servs., No. 21-1802V, 2025 WL 2401983, at *22 (Fed. Cl.
Spec. Mstr. July 11, 2025) (listing reasoned decisions that have not found any covered vaccine
can cause RA); Maxwell v. Sec’y of Health & Hum. Servs., No. 17-1367V, 2025 WL 1291642,
at *29-30 (Fed. Cl. Spec. Mstr. Mar. 26, 2025) (discussing reasoned decisions that have rejected
petitioners’ theories that a vaccine can cause RA).
In Hock, the Chief Special Master found the petitioner’s theory was not “sufficiently
reliable” to show that the flu vaccine can cause RA. Hock, 2020 WL 6392770, at *1. There,
petitioner’s expert proposed a three-phase theory: an initial innate response with rapid secretion
of cytokines, followed by “bystander activation,” and ending with molecular mimicry. Id. at *5-
7. The special master in Moran rejected the petitioner’s theory that the flu vaccine can cause RA
via molecular mimicry, finding it was not a sound and reliable theory. Moran v. Sec’y of Health
& Hum. Servs., No. 16-538V, 2021 WL 4853544, at *22-30 (Fed. Cl. Spec. Mstr. Oct. 4, 2021).
And the special master in Maxwell found the petitioner did not provide preponderant evidence to
support his theory that the flu vaccine can cause an abnormal innate immune response in the
joints. Maxwell, 2025 WL 1291642, at *23-27.
Recently, the undersigned issued a dismissal decision in a flu/RA case. Powell v. Sec’y
of Health & Hum. Servs., No. 20-1726V, 2025 WL 3443590, at *31-34 (Fed. Cl. Spec. Mstr.
Oct. 8, 2025). Petitioner’s expert in Powell described six immunological concepts by which the
flu vaccine can cause RA. Id. The undersigned found that none of the mechanisms reached the
level of preponderant evidence required, and thus, due to the lack of a sound and reliable theory
under Althen prong one, among other reasons, Petitioner’s case was dismissed. Id.
The undersigned acknowledges there is one case where a petitioner was found entitled to
compensation in a flu vaccine/RA case; however, the undersigned finds this case is not
instructive because it applies a different standard (plausibility) and the facts and circumstances
are distinct from this present case. See Campbell v. Sec’y of Health & Hum. Servs., 97 Fed. Cl.
650 (2011).
Although decisions of other special masters are not binding, the undersigned finds the
above cases instructive and follows the reasoning of her colleagues. See Boatmon, 941 F.3d at
1358; Hanlon v. Sec’y of Health & Hum. Servs., 40 Fed. Cl. 625, 630 (1998), aff’d, 191 F.3d
1344 (Fed. Cir. 1999).
Overall, the undersigned finds that here, Petitioner’s proffered concepts do not constitute
sound and reliable causal theories. Thus, the undersigned finds Petitioner has failed to provide
preponderant evidence with respect to the first Althen prong.
2. Althen Prong Two
Under Althen Prong Two, Petitioner must prove by a preponderance of the evidence that
there is a “logical sequence of cause and effect showing that the vaccination was the reason for
the injury.” Capizzano, 440 F.3d at 1324 (quoting Althen, 418 F.3d at 1278). “Petitioner must
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show that the vaccine was the ‘but for’ cause of the harm . . . or in other words, that the vaccine
was the ‘reason for the injury.’” Pafford, 451 F.3d at 1356 (internal citations omitted).
In evaluating whether this prong is satisfied, the opinions and views of the vaccinee’s
treating physicians are entitled to some weight. Andreu, 569 F.3d at 1367; Capizzano, 440 F.3d
at 1326 (“[M]edical records and medical opinion testimony are favored in vaccine cases, as
treating physicians are likely to be in the best position to determine whether a ‘logical sequence
of cause and effect show[s] that the vaccination was the reason for the injury.’” (quoting Althen,
418 F.3d at 1280). Medical records are generally viewed as trustworthy evidence, since they are
created contemporaneously with the treatment of the vaccinee. Cucuras, 993 F.2d at 1528.
Petitioner need not make a specific type of evidentiary showing, i.e., “epidemiologic studies,
rechallenge, the presence of pathological markers or genetic predisposition, or general
acceptance in the scientific or medical communities to establish a logical sequence of cause and
effect.” Capizzano, 440 F.3d at 1325. Instead, Petitioner may satisfy his burden by presenting
circumstantial evidence and reliable medical opinions. Id. at 1325-26.
Since Petitioner failed to prove Althen prong one, it follows that he cannot prove Althen
prong two. However, even if Petitioner had proven Althen prong one, the undersigned finds an
additional reason why Petitioner has failed to provide preponderant evidence that there is a
logical sequence of cause and effect showing Petitioner’s flu vaccine caused his RA.
The undersigned bases her finding on the lack of support by Petitioner’s treating
physicians. Petitioner’s treating physicians did not offer opinions in his medical records
associating his RA with his flu vaccination. In cases with such evidence, it can be considered in
an analysis of Althen prong two. See Andreu, 569 F.3d at 1367; Capizzano, 440 F.3d at 1326
(“[M]edical records and medical opinion testimony are favored in vaccine cases, as treating
physicians are likely to be in the best position to determine whether a ‘logical sequence of cause
and effect show[s] that the vaccination was the reason for the injury.’” (quoting Althen, 418 F.3d
at 1280)).
There is one reference where Dr. Chimata noted in the history that Petitioner had
received a flu vaccine before he presented with symptoms of RA. However, this notation
reflects merely a temporal association. Dr. Chimata did not offer any opinion to suggest vaccine
causation. Isaac v. Sec’y of Health & Hum. Servs., No. 08-601V, 2012 WL 3609993, at *26
(Fed. Cl. Spec. Mstr. July 30, 2012) (“A treating physician’s recognition of a temporal
relationship does not advance the analysis of causation.”).
Regarding alternative causes, the undersigned acknowledges that Petitioner is not
required to eliminate other potential causes in order to be entitled to compensation. See Walther
v. Sec’y of Health & Hum. Servs., 485 F.3d 1146, 1149-52 (Fed. Cir. 2007) (finding petitioner
does not bear the burden of eliminating alternative independent potential causes). However, it is
reasonable to consider “evidence of other possible sources of injury” in determining “whether a
prima facie showing has been made that the vaccine was a substantial factor in causing the injury
in question.” Stone, 676 F.3d at 1379; see also Winkler v. Sec’y of Health & Hum. Servs., 88
F.4th 958, 963 (Fed. Cir. 2023) (“Such contemplation of a potential causative agent when
evaluating whether or not a petitioner has established a prima facie case is in accordance with the
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law.”); Flores, 115 Fed. Cl. at 162-63 (“[T]he special master may consider the evidence
presented by the [R]espondent in determining whether the [P]etitioner has established a prima
facie case.”). Here, the record indicates two other possible causes: (1) medical record
documentation of a sore throat prior to his illness and (2) Petitioner’s history of antibiotic use, as
described by Dr. Matloubian. However, the undersigned finds Dr. Matloubian did not opine that
he held either of these opinions to a preponderant evidence standard. Thus, the undersigned does
not find evidence of an alternative cause for Petitioner’s RA.
Regardless, for the reasons stated above, the undersigned finds that Petitioner failed to
satisfy his burden under Althen prong two.
3. Althen Prong Three
Althen prong three requires Petitioner to establish a “proximate temporal relationship”
between the vaccination and the injury alleged. Althen, 418 F.3d at 1281. That term has been
defined as a “medically acceptable temporal relationship.” Id. The Petitioner must offer
“preponderant proof that the onset of symptoms occurred within a time frame for which, given
the medical understanding of the disorder’s etiology, it is medically acceptable to infer
causation-in-fact.” de Bazan, 539 F.3d at 1352. The explanation for what is a medically
acceptable time frame must also coincide with the theory of how the relevant vaccine can cause
the injury alleged (under Althen Prong One). Id.; Koehn v. Sec’y of Health & Hum. Servs., 773
F.3d 1239, 1243 (Fed. Cir. 2014); Shapiro, 101 Fed. Cl. at 542; see also Pafford, 451 F.3d at
1358. A temporal relationship between a vaccine and an injury, standing alone, does not
constitute preponderant evidence of vaccine causation. See, e.g., Veryzer, 100 Fed. Cl. at 356
(explaining that “a temporal relationship alone will not demonstrate the requisite causal link and
that [P]etitioner must posit a medical theory causally connecting the vaccine and injury”).
Since Petitioner failed to prove Althen prong one, it follows that he cannot prove Althen
prong three. In addition, there are independent reasons why the undersigned finds Petitioner
failed to prove Althen prong three.
Petitioner offered two theories of causation, each having a different medically acceptable
time frame within which onset would be expected to occur. In support of his cytokine theory,
Dr. Axelrod cited Hayden et al., who showed that when humans are infected with the flu A virus,
they release cytokines IL-6 and TNF-α in the first three days. He also cited studies showing that
cytokines IL-6 and TNF-α peak a day after vaccination and up to seven days, although
Yamaguchi et al. noted increased proinflammatory cytokines (IL-1 β and TNF-α) within 24 to 48
hours.
Both experts note there are inconsistencies in the record regarding onset of Petitioner’s
symptoms. Petitioner’s affidavit placed onset eight days after vaccination. The medical records
show that Petitioner requested a prescription for Motrin approximately 14 days after vaccination.
Other medical records indicate Petitioner had widespread pain approximately November 15, four
days after vaccination. And Dr. Chimata’s history referenced onset began four weeks prior or
one to two months prior, which would place onset between October 10 and November 12, 2019,
which ranges pre-vaccination to one day after vaccination.
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Dr. Axelrod opined that onset of either four days or eight days is consistent with a
secondary adaptive immune response, but this opinion is premised on research related to booster
vaccinations. There is no foundational evidence that the flu shot administered to Petitioner was a
booster vaccine. Therefore, the undersigned does not find this opinion to be supported by the
evidence.
In the alternative, based on Dr. Chimata’s note on December 10, 2019, Dr. Axelrod
opined that Petitioner had experienced pain for four weeks, which would place onset a day or
two after vaccination. He opined this time frame was consistent with an innate immune response
and “symptoms expected from the elevated cytokines.” Pet. Ex. 22 at 21. However, the
undersigned did not find that Petitioner proved his Althen prong one theories by preponderant
evidence, thus, this opinion, or any other opinion offered by Dr. Axelrod as to Althen prong one
is insufficient to support Althen prong three.
Therefore, the undersigned finds that Petitioner failed to provide preponderant evidence
of Althen prong three.
V. CONCLUSION
The undersigned extends her sympathy to Petitioner for the pain and suffering that he has
experienced due to his illness. The undersigned’s Decision, however, cannot be decided based
upon sympathy, but rather on the evidence and law.
For the reasons discussed above, the undersigned finds that Petitioner has failed to
establish by preponderant evidence that his flu vaccine caused his RA. Therefore, Petitioner is
not entitled to compensation, and the petition must be dismissed.
In the absence of a timely filed motion for review pursuant to Vaccine Rule 23, the Clerk
of Court SHALL ENTER JUDGMENT in accordance with this Decision.
IT IS SO ORDERED.
s/Nora Beth Dorsey
Nora Beth Dorsey
Special Master
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