In the United States Court of Federal Claims
OFFICE OF SPECIAL MASTERS
********************************
YVONNE HARRIS, as Mother * No. 10-322V
and Natural Guardian of * Special Master Christian J. Moran
KHONSTINCE COUCH, a Minor, *
* Filed: June 10, 2014
Petitioner, *
*
v. *
* Entitlement; human papillomavirus
SECRETARY OF HEALTH * vaccine (“HPV”); lupus.
AND HUMAN SERVICES, *
*
Respondent. *
********************************
Michael A. London, Douglas & London, P.C., New York, NY, for petitioner;
Ann D. Martin, United States Dep’t of Justice, Washington, DC, for respondent.
PUBLISHED DECISION DENYING ENTITLEMENT TO COMPENSATION1
Yvonne Harris alleges that her daughter, Khonstince Couch (“Bre”),
suffered systemic lupus erythematosus (“SLE”) as a result of the human
papillomavirus (“HPV”) vaccinations that she received on May 30, 2007, and
August 1, 2007. Petition at 3-5. Ms. Harris seeks compensation pursuant to the
National Childhood Vaccine Injury Compensation Program, 42 U.S.C. §§ 300aa-
10 through 34 (2006).
In support of her petition, Ms. Harris relies primarily upon the testimony of
Dr. Yehuda Shoenfeld, a specialist in autoimmune disease. Dr. Shoenfeld offered
1
The E-Government Act of 2002, Pub. L. No. 107-347, 116 Stat. 2899, 2913 (Dec. 17,
2002), requires that the Court post this decision on its website. Pursuant to Vaccine Rule 18(b),
the parties have 14 days to file a motion proposing redaction of medical information or other
information described in 42 U.S.C. § 300aa–12(d)(4). Any redactions ordered by the special
master will appear in the document posted on the website.
three theories to explain how the HPV vaccine could have caused Bre’s lupus. Dr.
Shoenfeld’s causation theories were opposed by respondent’s four expert
witnesses: Dr. Carlos D. Rose, a board-certified rheumatologist; Dr. Lawrence D.
Frenkel, a board-certified pediatrician, allergist, and immunologist; Dr. Theodore
C. Eickhoff, an expert in the field of infectious disease and epidemiology; and Dr.
Edward W. Cetaruk, a board-certified medical toxicologist.2 Background
information on each of these testifying experts is discussed below.
This decision is organized into the following sections:
I. Brief Biographies of the Testifying Witnesses
II. Facts
III. Lupus
IV. Procedural History
V. Standards for Adjudication
VI. Althen Prong One – Theory
VII. Althen Prong Three – Timing
VIII. Althen Prong Two – Logical Sequence
IX. Conclusion
As discussed in more detail below, Ms. Harris’s claim lacks persuasiveness
in two respects. First, she did not establish persuasively that the HPV vaccine can
cause lupus. This aspect of her proof is addressed in section VI. below. A second
and independent problem is that the evidence showed that Bre was probably
suffering from lupus before the vaccination. Thus, the vaccine cannot have caused
the disease. The basis for this finding is explained in section VII. below. These
two reasons contribute to the finding, in section VIII., that Ms. Harris did not
establish a logical sequence of cause and effect between the vaccination and Bre’s
lupus.
2
The hearing transcript contains an incorrect spelling (Frankle) of Dr. Frenkel’s name.
2
I. Brief Biographies of the Testifying Witnesses
A. Dr. Shoenfeld
Dr. Shoenfeld graduated from medical school in 1972. In the ensuing 40
years, Dr. Shoenfeld has worked in various capacities, taught at medical schools,
conducted research, and authored (at least in part) more than one thousand articles.
The breadth of his career is reflected in his 118-page curriculum vitae, which was
filed as exhibit 120.
Dr. Shoenfeld’s accomplishments are many. The highlights include being
awarded, in 2005, the EULAR prize for identifying the infectious etiology of the
anti-phospholipid syndrome and being recognized, in 2009, by the Israeli Medical
Association for his lifetime contributions to medicine. Exhibit 120 at 8.
Since 1996 (and perhaps earlier), Dr. Shoenfeld has proposed that vaccines
contribute to autoimmune conditions. See exhibit 120 at 65, item 625. His recent
research has focused on autoimmunity. He founded and still leads the Center for
Autoimmune Diseases located within the Sheba Medical Center. Id. at 2. He
describes himself as an “autoimmunologist.” Tr. 223, 408.
B. Dr. Rose
Dr. Rose graduated from medical school in 1977. He passed his
rheumatology board examination in 1983, his pediatric board examination in 1990,
and his sub-board examination for pediatric rheumatology in 1998. Exhibit B at 3.
He has taught at Thomas Jefferson Medical College since 1991. During his
academic career, he has been promoted from assistant professor to associate
professor to professor. Exhibit B at 6. His recent research work has focused on
arthritis and lupus. Id. at 18-19.
Dr. Rose sees patients as a pediatric rheumatologist at the Alfred I. duPont
Institute of the Nemours Foundation. His patient population is primarily children
with rheumatic disorders such as juvenile idiopathic and rheumatoid arthritis,
Lyme disease, and connective tissue disorders such as lupus. Tr. 549. He has seen
“hundreds” of cases of lupus. Tr. 550.
3
C. Dr. Frenkel
Dr. Frenkel earned his medical degree in 1969. His early career focused on
pediatrics and virology. Exhibit D at 1. In 1983, he became the director of the
Division of Immunology, Allergy and Infectious Diseases in the pediatric
department of the Robert Wood Johnson Medical School. He held that position for
13 years. Id. He then became a professor in the pediatric department of the
University of Illinois, College of Medicine at Rockford. Id. at 2.
Dr. Frenkel is board-certified in pediatrics as well as allergy and
immunology. He has a sub-specialty in pediatric infectious diseases. Id.
In 2000 and 2001, he worked on immunization projects in India. Starting in
2008, he has served as co-chair of the New Jersey Immunization Network. Id. at 4.
D. Dr. Eickhoff
When he testified, Dr. Eickhoff held the position of professor emeritus at the
University of Colorado, School of Medicine. He attained this position in 2003,
which was more than 40 years after he graduated from Western Reserve University
School of Medicine. Exhibit O at 1.
Dr. Eickhoff’s professional career has centered on infectious diseases and
epidemiology. He has served on various committees exploring the safety of
vaccines through the Department of Health and Human Services. Id. at 4. For the
Institute of Medicine, he participated on a similar committee involving the anthrax
vaccine. Id. at 5.
E. Dr. Cetaruk
Dr. Cetaruk graduated from the School of Medicine at New York University
in 1991. He received advanced training in emergency medicine. From 1994 to
1996, he had a fellowship in medical toxicology. The American Board of
Emergency Medicine recognized him as having special qualifications in medical
toxicology in 2000. He became a fellow in the American College of Medical
Toxicology in 2009. Exhibit Q at 1-2.
Each expert was provided with Bre’s medical history for review. A
summary of the relevant medical records is addressed next, followed by a general
overview of lupus.
4
II. Facts
Bre was born in 1998. Bre’s mother has a history of atopic dermatitis and
asthma, a first-generation cousin suffers from lupus, and her great-grandfather had
rheumatoid arthritis. Exhibit 4 at 12; exhibit 3 at 54. This genetic background
makes Bre more likely (but not necessarily destined) to develop an autoimmune
disease. Tr. 24-26, 192 (Dr. Shoenfeld).
The first filed medical record about Bre was created when she was nine
years old. On March 19, 2007, she was seen for a swollen thumb. Exhibit 2 at 1-
56; exhibit 26 at 1. Her doctors eventually determined that she was suffering from
a methicillin resistant staphylococcus aureas (“MRSA”) infection. Id.; see also Tr.
188-89 (Dr. Shoenfeld’s discussion of MRSA). In conjunction with this infection,
doctors ordered blood tests. Exhibit 2 at 50. Dr. Frenkel cited the results as
supporting his opining that Bre was suffering from lupus before vaccination. See
section VII., below.
On April 17, 2007, Bre saw Edward J. Vanderburg, who became her primary
care doctor. Dr. Vanderburg’s examination showed that Bre had a “rash over
complete body.” Exhibit 26 at 1, 3. Dr. Vanderburg’s history of present illness
indicates that the rash “has been going off and on for several years. She will get a
macular, raised, itchy rash.” According to this history, the “[m]ost recent flare up
is 2 weeks out.” Id. at 3.3 Dr. Vanderburg assessed Bre as having “[p]robable
pityriasis rosea.” He prescribed two medications, Bactrim and Keflex, and referred
her to a dermatologist. Id. at 1, 3. In testimony, the expert witnesses disputed the
significance of the rash. Dr. Rose and Dr. Frenkel linked the rash to Bre’s lupus.
Tr. 568-70, 616-17, 694-98. Dr. Shoenfeld disagreed. Tr. 31.
Although Bre’s mother or cousin had requested a referral to a dermatologist,
no record from any dermatologist was filed. Instead, Bre’s next encounter with a
medical professional was on May 30, 2007, when she received her first dose of the
HPV vaccine. The administering entity was the health unit in her local county.
Exhibit 1 at 1. There are no records showing Bre’s state of health on this date.
The same agency administered the second dose of HPV vaccine on August 1,
2007. Id.
3
The source of information about Bre’s history is not entirely clear. On this page of Dr.
Vanderburg’s note, he states that “Mother wants next treatment plan to come from a
dermatologist.” Exhibit 26 at 3. However, on a different page, Dr. Vanderburg created an
addendum, stating “I was informed later that the woman with the child was the cousin.” Id. at 1.
5
On August 23, 2007, Bre was seen because her “index finger swelling
started yesterday.” She also had “bright spots all over [her] body.” Exhibit 26 at
4. An advance practice nurse saw her and recorded that the rash was on her “face
[and] upper extremities,” and “spreading.” The rash was also “itchy.” The nurse
assessed her as having “cellulitis and abscess of finger, unspecified” and “allergy,
unspecified.” The nurse recommended follow up in two weeks. Id.; see also Tr.
571.
Before this follow up appointment took place, Bre developed a fever and
headache. Exhibit 25 at 4. On September 9, 2007, Ms. Harris took her to the
pediatric emergency department of Arkansas Children’s Hospital. Id. at 1-8. The
doctor’s review of systems indicated that except for Bre’s fever, her systems,
including her skin, were normal. The doctor’s impression was that she had a viral
upper respiratory infection and recommended that Bre see her primary care
physician in the next two or three days. Id. at 1-4.
On September 11, 2007, Bre was still running a fever. She also had a rash.
Therefore, Ms. Harris brought Bre to see Dr. Vanderburg. He found that she had
atopic eczema and dry skin on her arms and back. He also diagnosed her with an
upper respiratory infection and prescribed an antibiotic and antihistamine. Exhibit
26 at 6-7.
Throughout that night, Bre vomited. She also had a fever, sore throat, and
bleeding in her gums. Id. at 8. On September 12, 2007, Ms. Harris returned with
Bre for a follow up with Dr. Vanderburg. Dr. Vanderburg treated Bre with an
antibiotic administered by intramuscular injection and recommended a follow up
appointment in three months. Id. at 8-9.
On September 16, 2007, shortly after 11:00 P.M., Ms. Harris brought Bre to
Arkansas Children’s Hospital because she had fever, vomiting and dehydration.
Exhibit 3 at 44. Ms. Harris also reported that she had lost weight. Id. at 57. Bre
remained in the hospital until September 21, 2009, during which time many
doctors examined her and conducted many tests. At discharge, the doctors listed
several problems including “recurring fever, fatigue, anorexia, dehydration,
macular rash, conjunctiva injection.” Id. at 142.
On September 28, 2007, Ms. Harris took Bre to Le Bonheur Children’s
Medical Center, where she remained until October 5, 2007. Exhibit 132. For
purposes of this case, the most significant event was a rheumatology evaluation by
6
Dr. Monica Brown and Dr. Linda K. Meyers. They suggested that Bre may have
lupus and ordered tests informative for lupus. Id. at 343-45.
These tests did in fact confirm lupus. The doctors testifying also agreed
with the diagnosis of lupus, see Tr. 17 (Dr. Shoenfeld), 565 (Dr. Rose). Thus, an
extensive recitation of the signs and symptoms that Bre experienced is not needed.
So, too, a discourse about Bre’s multi-year history of lupus is also not
needed to address the issue in this case, which is whether the HPV vaccine caused
Bre to suffer lupus. For purposes of making this finding, it is sufficient to note that
Bre’s course of lupus has been extremely severe. Sadly, Bre has suffered from
many lupus complications, including damage to her kidneys and brain. Exhibit 4
at 84-87; see also Pet’r’s Prehr’g Br., filed Sept. 25, 2012, at 7-8 (summarizing
Bre’s medical history after 2007), Resp’t’s Rep’t, filed Jan. 27, 2012, at 3 (stating
“[t]he subsequent clinical course of [Bre]’s SLE has been quite severe, and central
nervous system involvement has been a major component of [Bre]’s disease” and
citing records).
While Bre’s ultimate diagnosis of lupus is not disputed, determining the
onset of lupus is generally not straightforward. See Tr. 17, 556, 930-34, 1109-12.
For background, a general discussion of the symptoms, diagnosis, and incidence of
lupus is included below.
III. Lupus
Lupus is an autoimmune disease. In autoimmune diseases, “the immune
system is reacting aberrantly in a very strong way against our own constituents.”
Tr. 27. In lupus, many organs, including skin, joints, lungs, heart, central nervous
system, and hematologic system, may be affected. Tr. 551; accord Tr. 554-55.
Hence, it is classified as a “systemic” disease. Tr. 16-17. In Dr. Rose’s view,
lupus may be “the most complex” autoimmune disease that he treats. Tr. 557.
Such complexity derives, in part, from the presentation. Lupus can appear in
a variety of ways. Tr. 223-24. Dr. Shoenfeld stated: “Every lupus differs from the
other. I have not seen two patients with lupus [who] are identical to each other…
This is one of the most diverse diseases, and therefore, it was named the disease of
1,000 faces.” Tr. 194.
The first sign or symptom of lupus “depends on who is asking and who is
looking.” Tr. 562 (Dr. Rose); accord Tr. 195-96 (Dr. Shoenfeld: “at the first
presentation [diagnosis] will be difficult”). The initial symptom is often an
7
“unspecific inflammation,” which may be manifest as “low-grade fever, weight
loss, aches and pains, sometimes nephropathy, sometimes sore throats and rashes
of all sorts.” Tr. 562. According to Dr. Rose, “it has been said that almost any
skin rash can be seen in lupus, from the typical one described in the criteria, also
known as the butterfly rash, to all sorts of macular, circular, purpuric, [and]
necrotic rashes.” Tr. 554.
Researchers have identified 11 criteria for classifying lupus. Although some
physicians require a patient to satisfy at least four of the criteria to diagnose lupus,
Dr. Rose does not. Tr. 563-64, 1109-12. Sometimes, lupus can be diagnosed
based upon fewer than four criteria, especially when the sign or symptom is closely
associated with lupus. In the absence of a particular sign or symptom associated
with lupus, determining when the person first began suffering from the disease is
challenging. See Tr. 930-34 (Dr. Shoenfeld), 1109-12 (Dr. Rose).
The incidence of lupus varies. In the United States, there are 8-10 cases per
100,000. Tr. 917. But, in the African-American female population, the incidence
is one case per 700 African-American females. Tr. 651. The incidence of lupus in
identical (monozygotic) twins is higher than the incidence in fraternal twins. Tr.
919. The concordance rate means that genetics contributes to the cause of lupus.
Tr. 192, 552, 652, 918-19.
Although genes are involved in developing lupus, lupus is not inherited by
the simple rules of Mendelian genetics. For most cases of lupus, a single gene
does not determine that the person will developed lupus. Tr. 193 (Dr. Shoenfeld:
the genetics “is not one to one”), 919-20.4 Dr. Shoenfeld stated that researchers
have “found so far 33 different genes which make you more prone” to develop
lupus. Tr. 920. In Dr. Rose’s view, at least four genetic mutations may need to
occur in combination for a person to develop lupus. Tr. 552-53. Because genetic
mutations do not account for all cases of lupus, environmental factors may also
contribute to its development. Tr. 192, 558-60, 652.
What environmental factors cause lupus is not established. Dr. Rose stated
“the bottom line is that we don’t know what causes lupus to start with.” Tr. 558.
Exposure to the sun may increase the likelihood of developing lupus. Tr. 190-91.
Dr. Shoenfeld stated that infections may lead to the onset of autoimmune diseases
4
Dr. Rose mentioned that a mutation in a particular gene, known as the C1q gene, causes
a deficiency that develops into lupus. This particular form of lupus is almost entirely genetic.
Tr. 553.
8
generally. See Tr. 49, 85, 90-97, 119-20, 140-41, 156, 188-91, 474-75, 480-81.
The Epstein-Barr virus has particularly been associated with the development of
lupus. Tr. 90, 141, 560, 638, 654-55, 673-79, 921-22.
On the other hand, the human papillomavirus has not been associated with
autoimmune diseases. A potential effect of an infection with human
papillomavirus is cervical cancer, but not lupus. Tr. 141.
Ms. Harris claims that the vaccine against the human papillomavirus caused
her daughter to suffer lupus. The events associated with the prosecution of this
claim are set forth in the next section.
IV. Procedural History
Ms. Harris filed her petition on May 26, 2010. She submitted Bre’s medical
records on June 11, 2010 (exhibits 1-14) and a set of affidavits (exhibits 15-22) on
August 12 and 13, 2010. More medical records were filed on September 13, 2010
(exhibits 23-28). None of this material contained a report from an expert
supporting Ms. Harris’s claim that the HPV vaccine caused Bre’s lupus.
The presiding special master granted a series of motions seeking additional
time to file an expert report, totaling approximately one year. On September 11,
2011, Ms. Harris presented the report of Dr. Shoenfeld, exhibit 32.
Dr. Shoenfeld’s report began with a recitation of his background in
immunology and a review of Bre’s medical history. Exhibit 32 at 1-2. He
indicated that the aluminum adjuvant can cause lupus, and that the aluminum
adjuvant in the HPV vaccine caused Bre’s lupus. Id. at 5-6. Dr. Shoenfeld’s report
cited 85 articles (exhibits 33-117) in support of his conclusions, although some
were duplicates. The presiding special master ordered that Ms. Harris file the
articles that Dr. Shoenfeld cited and identify the relevant portions of the article
with highlighting. Order, filed Nov. 1, 2011.
The Secretary responded to this material on January 27, 2012. The
Secretary maintained that the record, including Dr. Shoenfeld’s report, did not
establish that Ms. Harris was entitled to compensation. Resp’t’s Rep’t at 6.
In response to Dr. Shoenfeld’s opinion, the Secretary presented the reports
from Dr. Rose and Dr. Frenkel. Although Dr. Rose agreed that Bre suffered from
lupus, he suggested that she may have developed lupus before she received the
HPV vaccine. Exhibit A at 3-4.
9
Dr. Rose more broadly argued that the evidence does not support a finding
that the HPV vaccine can cause lupus. Dr. Rose relied upon a study by Thomas
Verstraeten, which a manufacturer of an HPV vaccine sponsored. Exhibit M
(Thomas Verstraeten et al., Analysis of adverse events of potential autoimmune
aetiology in a large integrated safety database of AS04 adjuvanted vaccines, 26
Vaccine 6630 (2008)).5 The Verstraeten study integrated an analysis of many
smaller studies, totaling over 68,000 participants. The authors did not find that the
incidence of lupus increased among people who received an HPV vaccine. Id. Dr.
Rose stated that: “The epidemiological data offered is overwhelmingly against a
relationship with SLE.” Exhibit A at 16.
Dr. Rose also reviewed each of the 85 articles Dr. Shoenfeld cited. Dr. Rose
maintained that the cited articles did not support a causal relationship between the
HPV vaccine and lupus. He wrote:
The overwhelming majority of them were editorials and
opinion papers most of them written by Dr. Shoenfeld[;]
as such the arguments and ideas tended to overlap and
are mostly redundant. Without exception all the reports
that involve some level of systematic approach showed
negative results for vaccines in relationship to SLE.
Id. at 16.
The second report filed by the Secretary came from Dr. Frenkel, who
specializes in pediatric infectious diseases and immunology. Like Dr. Rose, Dr.
Frenkel raised the possibility that Bre was suffering from undiagnosed lupus before
she was vaccinated. Exhibit C at 3. Dr. Frenkel’s report further discussed ongoing
work being done to monitor HPV vaccine safety including a study by Chun Chao
et al. that “failed to verify a causal relationship between HPV vaccine and
autoimmune disease including SLE.” Id. (citing exhibit F (Chun Chao et al.,
Surveillance of autoimmune conditions following routine use of quadrivalent
human papillomavirus vaccine, 271(2) J. Internal Medicine 193 (2012)). With
regard to Dr. Shoenfeld’s theory that vaccine adjuvants can cause lupus, Dr.
Frenkel stated Dr. Shoenfeld “fails to offer any specifics regarding the basis of his
causation opinion. He also fails to provide any relevant and reliable peer-reviewed
references in support of his opinion regarding the specific role of the adjuvants in
this case.” Id. at 4.
5
A duplicate of the Verstraeten study appears as exhibit 146.
10
The presiding special master ordered a response from Dr. Shoenfeld and
repeated the requirement that Ms. Harris highlight the pertinent portions of the
medical literature. Order, filed Feb. 1, 2012. On March 12, 2012, Ms. Harris filed
two reports from Dr. Shoenfeld. The first, exhibit 118, responded to Dr. Rose’s
report. The second, exhibit 119, addressed the opinions of Dr. Frenkel. Dr.
Shoenfeld cited a total of 13 (non-duplicate) articles (exhibits 121-32).
In these reports, Dr. Shoenfeld introduced a new syndrome that Dr.
Shoenfeld’s colleagues and he had recently “crystallized” --- the autoimmune
syndrome induced by adjuvant (“ASIA”). Proponents of this syndrome maintain
that an adverse effect of one type of vaccine, such as the hepatitis B vaccine,
usually portends the adverse effect of another type of vaccine, such as the HPV
vaccine, because the vaccines share a common denominator, the adjuvant. Exhibit
118 at 1. Dr. Shoenfeld noted that a special issue of the journal Lupus was devoted
to ASIA and he cited the articles contained in that issue.
Dr. Shoenfeld responded to Dr. Frenkel’s citation to the Chao article by
saying that “each one of the authors was a private consultant to Merck & Co.,”
which manufactured the vaccine. Exhibit 118 at 2. He also stated that the editor of
the Journal of the American Medical Association criticized the way that “the
Gardasil vaccine was ‘pushed’ to the market.” Id.
Dr. Shoenfeld incorporated these comments into his separate response to Dr.
Frenkel. Here, Dr. Shoenfeld stated that the rash that Bre experienced before the
HPV vaccination “was non-specific,” in contrast to the “specific, identifiable
rashes” that are associated with lupus. Exhibit 119.
The presiding special master ordered that Ms. Harris provide a list of
causation theories advanced by Dr. Shoenfeld. Order, filed Mar. 20, 2012.
Another order, filed April 4, 2012, scheduled a hearing for October 16, 2012.
Ms. Harris filed another report from Dr. Shoenfeld as exhibit 133 on May 7,
2012. In response to the March 20, 2012 order, Dr. Shoenfeld identified three
theories: (1) adjuvant-induced autoimmunity, (2) molecular mimicry, and (3)
bystander activation. Dr. Shoenfeld again cited various medical articles to support
these three theories.
On May 7, 2012, the case was reassigned to the undersigned. A status
conference was held on May 23, 2012, to discuss the plan to have a hearing on
October 16, 2012.
11
The Secretary stated that she intended to respond to the recent opinions
offered by Dr. Shoenfeld. She also planned to retain additional experts to address
the theory based on adjuvants. The ensuing order permitted the Secretary to
submit these reports by July 30, 2012. A subsequent order extended the duration
of the hearing from one day (October 16, 2012) to three days (October 15-17,
2012).
After receiving an enlargement of time, the Secretary presented reports from
two more experts. One of the reports was written by Theodore C. Eickhoff, a
specialist in adult infectious diseases and epidemiology with experience in
studying vaccines. Dr. Eickhoff described the process “by which the adverse
events caused by vaccines are actually attributed to a specific vaccine.” Exhibit N
at 4. He cited three studies (one by Chao, the second by Slade, and the third by
Mok). Id. at 4-5. Dr. Eickhoff interpreted “these epidemiological studies [as]
provid[ing] no basis to believe, as Dr. Shoenfeld has suggested, that HPV vaccine
has in any way caused or facilitated the development of SLE.” Id. at 5.
The Secretary’s last report came from Edward Cetaruk, a medical
toxicologist. He “applied the principles of both experimental and clinical
toxicology in conjunction with scientifically sound causation analysis
methodology” to investigate “aluminum and aluminum-containing adjuvants and
their potential health effects on humans.” Exhibit P at 4. Dr. Cetaruk’s ultimate
conclusion was that “Dr. Shoenfeld fails to present a scientifically sound (i.e.
supported by the medical literature – including those publications he cites in his
report) case for either a general or specific causal relationship between Gardasil or
its aluminum adjuvant and the development of SLE.” Id. at 9.
On September 25 and 27, 2012, the parties filed additional materials before
the hearing. Each party filed a brief. Both parties filed more medical articles. An
extensive and digitally recorded pre-trial conference was held on October 2, 2012.
The hearing was held, as scheduled, for three days, starting on October 15,
2012, in Washington, DC. The five doctors who had submitted reports testified.
Following the hearing, the parties opted to file briefs. Ms. Harris has filed
the final brief, making the case ready for adjudication.
V. Standard for Adjudication
With respect to her burden of proof, Ms. Harris argues for a standard that is
less than a preponderance of the evidence. She stated “medical and scientific
12
certainty is not required for causation to be found pursuant to the Vaccine Act….
Rather, all that is required is a plausible theory of causation consistent with current
body of scientific and medical knowledge that exists today.” Pet’r’s Posthr’g Br.
at 7 (citing Althen v. Sec'y of Health & Human Servs., 418 F.3d 1274, 1278 (Fed.
Cir. 2005)). Consistent with this view, Ms. Harris frequently solicited testimony
about whether particular medical theories were “plausible.” Tr. 21-22, 51, 65, 94-
95, 130, 220-21, 625, 633-34, 636-39, 684-85, 690-93, 712, 1083-84, 1086-88,
1094-95.
Ms. Harris’s argument does not accord with controlling precedent. The
Federal Circuit has consistently rejected attempts to set petitioners’ burden of proof
at the plausibility level. “[P]roof of a ‘plausible’ or ‘possible’ causal link between
the vaccine and the injury… is not the statutory standard.” Moberly v. Sec'y of
Health & Human Servs., 592 F.3d 1315, 1322 (Fed. Cir. 2010). A “petitioner must
do more than demonstrate a ‘plausible’ or ‘possible’ causal link between the
vaccination and the injury; he must prove his case by preponderance of the
evidence.” W.C. v. Sec'y of Health & Human Servs., 704 F.3d 1352, 1356 (Fed.
Cir. 2013) (citing Moberly, 592 F.3d at 1322).
Consequently, the evidence in this case will be examined to determine
whether Ms. Harris has established the elements of her case on a more likely than
not basis. The elements of Ms. Harris’s case are set forth in the often cited passage
from Althen: “(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.
VI. Althen Prong One – A Medical Theory
The first prong of the Althen analysis has been described as a “can it?”
question which asks whether the vaccine could cause the alleged injury. See
Pafford v. Sec'y of Health & Human Servs., 451 F.3d 1352, 1356 (Fed. Cir. 2006)
(affirming special master’s use of “can cause” and “did cause” as consistent with
the Althen test); Veryzer v. Sec'y of Health & Human Servs., 100 Fed. Cl. 344, 352
(2011) (describing the first prong of Althen as presenting the question of general
causation). The Federal Circuit has characterized this aspect as “a frequently more
difficult” inquiry compared to the sometimes more straightforward question of
whether a petitioner suffered from a particular disease. Hibbard v. Sec’y of Health
and Human Servs., 698 F.3d 1355, 1365 (Fed. Cir. 2012).
13
An important aspect to evaluating whether petitioners have established the
persuasiveness of a theory proposed by their expert is to consider what information
is relevant to assessing the reliability of a theory. As discussed in section VI.A,
there is a consensus that some types of studies provide more meaningful
information than other types of studies.
In trying to determine whether there is a reliable basis for a petitioner’s
theory that a vaccine can cause a particular disease (the first prong of Althen), a
potentially useful study is an epidemiological one. Here, the parties submitted four
epidemiologic studies involving vaccinations against the human papillomavirus.
These are discussed in section B. They are discussed before a more in-depth
evaluation of Dr. Shoenfeld’s theories because the epidemiological studies provide
some information about the reliability of all Dr. Shoenfeld’s theories. Because
epidemiological studies cannot definitively resolve whether an HPV vaccine can
cause lupus, Dr. Shoenfeld’s theories are separately addressed in section C.
A. Value of Scientific Studies
While opining on whether an HPV vaccine can cause lupus, the parties’
experts have cited various scientific studies. A discussion of the expert opinions
about a selection of the cited scientific studies appears below. The experts’
opinions differed at several points, offering conflicting interpretations on the value
and relevance of the studies discussed. When the evidence is in conflict, the
special master may determine what evidence is more persuasive. Broekelschen v.
Sec'y of Health & Human Servs., 618 F.3d 1339, 1346-49 (Fed. Cir. 2010); see
also Whitecotton v. Sec'y of Health & Human Servs., 81 F.3d 1099, 1108 (Fed.
Cir. 1996).
The expert witnesses explained the process that doctors use in reaching
conclusions about causation. There was general agreement that the first step is an
observation that two events occur in sequence. See Tr. 26, 509, 593. As Dr.
Shoenfeld stated: “[E]very disease, like Mao Tse-Tung says, every long march
start[s] with one step[;] every new syndrome start[s] with [a] case report.” Tr. 197.
The Secretary’s experts emphasized that case reports usually do not contain
sufficient evidence to establish causation. Tr. 509-10 (Dr. Eickhoff), 579-80 (Dr.
Rose), 1087-88 (Dr. Cetaruk).6 After several separately presented case reports,
6
The opinions from the government’s experts about the relative usefulness of different
types of evidence that might support an opinion regarding causation is quite similar to a view
expressed in a publication from the Federal Judicial Center. The Federal Judicial Center has
(continued…)
14
they might be collected into a “case series.” Tr. 197-98 (Dr. Shoenfeld). A case
series, like a case report, “cannot in and of itself show a causal effect.” Tr. 510
(Dr. Eickhoff).
These groups of observations “might lead to other studies that will prove a
[causal] relationship.” Tr. 1087. Examples of these other more probative studies
include experimental animal models and reports of rechallenge. Tr. 69, 132, 408-
10 (Dr. Shoenfeld). To Dr. Shoenfeld, “the experimental models are much more
scientifically [informative], scientific as in evidence, than just the case report.” Tr.
197.
Another potentially useful type of study is an epidemiological study.
“Epidemiology is the study of disease or some aspect of disease in a population.”
Tr. 508. Epidemiology can show an increased incidence of disease in particular
populations. This increased incidence, in turn, may support an inference that an
exposure to a substance caused the disease. See Tr. 59, 73, 519. Epidemiological
studies, however, are limited in their ability to detect increased incidences of
diseases that are rare. Tr. 579-80, 1091.
B. Epidemiological Studies
In a single person, determining whether an outside factor (such as a vaccine)
caused a disease (such as lupus) may be difficult. It may be that the foreign
substance did cause the disease. However, it may also be true that the introduction
of the outside agent did not cause the illness. In other words, the exposure to the
outside agent was coincident to the onset of the disease.
Separating out these coincidences from causal events is difficult, but
epidemiological studies are a useful part of the process. An advantage to
epidemiological studies is that they can account for the background incidence of a
disease -- the number of cases that are expected to occur in the population without
any effect from the putative causative factor. Michael D. Green et al., Reference
published a series of guides designed “to assist judges . . . in reaching an informed and reasoned
assessment concerning the basis of expert evidence.” Jerome P. Kassirer & Gladys Kessler,
Preface, in Reference Manual on Scientific Evidence (Federal Judicial Center, 3d ed. 2011). A
pertinent guide contained therein states that “Anecdotal evidence usually amounts to reports that
events of one kind are followed by events of another kind. Typically, the reports are not even
sufficient to show association, because there is no comparison group.” David H. Kaye & David
A. Freedman, Reference Guide on Statistics, in Reference Manual on Scientific Evidence 211,
218 (Federal Judicial Center, 3d ed. 2011).
15
Guide on Epidemiology, in Reference Manual on Scientific Evidence 549, 570
(Federal Judicial Center, 3d ed. 2011) (calculating attributable risk using
epidemiological incidence data from cohort studies). The Verstraeten study
commented upon how the background rate can help distinguish a coincidence from
an actual increase in disease:
Bearing in mind the background incidence of
autoimmune disorders in the adolescent and young adult
population, it seems likely that, with broader use of HPV
vaccines or other vaccines targeting this age group,
autoimmune disorders will be reported in temporal
association with vaccine administration even in the
absence of a causal relationship.
Exhibit M (Verstraeten) at 6633.
As a co-author, Dr. Shoenfeld has recommended additional studies of the
HPV vaccine with a longer follow-up period that would take into account “the
expected rate of [autoimmunity] in young girls.” Exhibit 145 (Ari Balofsky et al.,
The new H1N1 and HPV vaccines and old fears, 22 Current Op. in Rheumatology
431 (2010)) at 433. Dr. Shoenfeld’s testimony about the background rate was
similar. Tr. 426-32.
Epidemiological studies can detect when the incidence of disease exceeds
the background rate. For example, in the 1970s, epidemiological studies
discovered an increased incidence of Guillain-Barré syndrome among people
receiving the swine flu vaccine. Tr. 539-40. Dr. Shoenfeld stated that more
recently, large studies demonstrated an increased number of cases of narcolepsy in
Finland among people who received a type of flu vaccine. Tr. 59-60.7
While epidemiological studies can establish an increased incidence, and this
increased incidence can support an inference of causation, epidemiological studies
cannot absolutely refute a causal connection. Epidemiological studies cannot
prove a negative. It is always possible that another epidemiological study
involving a bigger population will detect an increased risk not otherwise apparent
7
Although Dr. Shoenfeld testified about this study, Dr. Shoenfeld did not cite the study
in his report and the petitioner did not file the relevant article. Consequently, the Secretary
objected to Dr. Shoenfeld's testimony about an article not included in the record. Tr. 58-61.
16
in smaller studies.8 Nevertheless, epidemiological studies have been considered
relevant and meaningful evidence in determining causation. See Holmes v. Sec'y
of Health & Human Servs., 115 Fed. Cl. 469, 485 (2014) (“causation can without
question be based on epidemiological evidence”) (citing Knudsen v. Sec'y of
Health & Human Servs., 35 F.3d 543, 549 (Fed. Cir.1994)); see also Andreu v.
Sec'y of Dep't of Health & Human Servs., 569 F.3d 1367, 1379 (Fed. Cir. 2009)
(“the special master can consider [epidemiological evidence] in reaching an
informed judgment as to whether a particular vaccination likely caused a particular
injury”); Koehn v. Sec'y of Health & Human Servs., 11-355V, 2013 WL 3214877,
at *20 (Fed. Cl. May 30, 2013) (discussing epidemiology articles as additional
reason for finding petitioner’s causation theory unlikely and citing Andreu), mot.
for review denied sub nom. C.K. v. Sec'y of Health & Human Servs., 113 Fed. Cl.
757 (2013), appeal docketed, No. 14-5054 (Fed. Cir. Feb. 18, 2014).
Consideration of epidemiological studies is not unique to the Vaccine
Program and courts, in the context of evaluating whether plaintiffs established an
exposure caused them to suffer a personal injury, have looked at epidemiological
studies. For example, when a plaintiff alleged silicone breast implants caused her
to develop an autoimmune disease, she advanced reports from two doctors,
attempting to establish that silicone breast implants can cause disease in people.
The defendant submitted at least 17 epidemiological studies to support its
argument that silicone breast implants do not cause disease. The district court
excluded the plaintiff’s evidence and granted summary judgment. Norris v. Baxter
Healthcare Corp., 397 F.3d 878, 880-81, 887 n.5 (10th Cir. 2005). On appeal, the
Tenth Circuit affirmed, holding that while “the presence of epidemiology does not
necessarily end the inquiry, where epidemiology is available, it cannot be ignored.
As the best evidence of general causation, it must be addressed.” Id. at 882. The
court clarified: “We are not holding that epidemiological studies are always
necessary in a toxic tort case. We are simply holding that where there is a large
body of contrary epidemiological evidence, it is necessary to at least address it
with evidence that is based on medically reliable and scientifically valid
methodology.” Id.
8
For example, Dr. Shoenfeld stated that a study has found an increased risk of multiple
sclerosis among people who received the hepatitis B vaccine. But, this risk was not apparent
until more than two years later. Tr. 115, 156, 183-86, 427-28. Again, Dr. Shoenfeld did not cite
this study and it does not appear in the record.
17
Here, the record includes epidemiological studies by Chao, Slade, Mok, and
Verstraeten. These articles and the experts’ commentary on them are discussed
below.
1. Chao
When the manufacturer of an HPV vaccine, Merck, was obtaining regulatory
approval for Gardasil from the FDA, Merck committed to funding post-licensure
studies about the safety of Gardasil. One such study was conducted by 13
employees of two large health maintenance organizations in California. Tr. 124,
526, 537-38, 544. The lead author of the ensuing article is Chun Chao, PhD.
Through computerized medical records, Chao and colleagues identified
more than 180,000 women who received at least one dose of the HPV vaccine.
The researchers followed these women for 180 days, looking to see if they
developed any autoimmune diseases. Lupus was one of the autoimmune diseases
for which the researchers searched. Exhibit F (Chao) at 193-94; see also Tr. 438,
512-13, 520-21.
The incidence of lupus among women who received the HPV vaccine was
not statistically increased compared to women who did not receive the HPV
vaccine. Exhibit F (Chao) at 199 (table 3); see also Tr. 523-24, 543. Dr. Frenkel
interpreted this finding as “fail[ing] to verify a causal relationship between HPV
vaccine and autoimmune disease including SLE.” Exhibit C at 3. Dr. Eickhoff
opined that this study showed the HPV vaccine “did not result in an increased
incidence of lupus.” Tr. 524.
Dr. Shoenfeld rejected the data Chao presented. He stated flatly that “this is
a fraud in medicine.” Tr. 438; accord Tr. 423. In his testimony, Dr. Shoenfeld
proposed that the payments from Merck influenced the outcome of the study. He
went so far as to say that Merck employees may have ghostwritten the article. Dr.
Shoenfeld acknowledged that he did not have any direct knowledge about Dr.
Chao or ghostwriting. Tr. 423, 436-39, 491-96. Dr. Shoenfeld made a similar,
although less bombastic, criticism in a letter addressed to the editors of the journal
that published the Chao article. Exhibit 126.9
9
Exhibit 126 is the manuscript version of Dr. Shoenfeld's letter. The published version
appears in 272 J. Internal Medicine 98 (2012).
18
In her reply brief, Ms. Harris repeats Dr. Shoenfeld’s accusation. She thus
argues “the Chao study is tainted because it was funded by Merck.” Pet’r’s
Posthr’g Reply, filed Aug. 26, 2013, at 13 (citing Exxon Shipping Co. v. Baker,
554 U.S. 471, 501 n.17 (2008); UFCW Local 1776 v. Eli Lilly and Co. (In re
Zyprexa Prods. Liab. Litig.), 253 F.R.D. 69, 107 (E.D.N.Y. 2008), rev’d on other
grounds, 620 F.3d 121 (2d Cir. 2010)), Ms. Harris contends that “given that
funding bias is a true concept,… [t]he reliability of the results of the Chao study
must be questioned.” Pet’r’s Posthr’g Reply, filed Aug. 26, 2013, at 14.10
2. Slade
Another post-licensure study of the safety of Gardasil was led by Barbara
Slade. The funding for this study came from the Centers for Disease Control and
Prevention and the Food and Drug Administration. An external source did not
sponsor this investigation. Exhibit K (Slade) at 757.
Dr. Slade and her team searched for health problems reported to the Vaccine
Adverse Event Reporting System (VAERS). They determined the frequency of
reports of different health problems per 100,000 doses of vaccine distributed. The
researchers compared reporting rates for Gardasil and reporting rates for other
vaccines. Exhibit K at 750-51; see also Tr. 441, 511-15. The authors grouped the
adverse events following immunizations into 15 categories, including dizziness,
hypersensitivity reaction, Guillain-Barré syndrome, death, and autoimmune
disorder. Exhibit K at 753 (table 2). The group of autoimmune disorders included
18 reports of lupus. Exhibit K at 755.
Dr. Slade and colleagues identified an increased reporting ratio for syncope
and venous thromboembolic events. They did not otherwise detect an increased
rate of reports for any of the other conditions. Exhibit K at 755; Tr. 516-17.11
Dr. Shoenfeld questioned the methodology Dr. Slade used. In his opinion,
the different diseases listed in table 2 should not have been analyzed separately.
Dr. Shoenfeld stated that the reports of Guillain-Barré syndrome, the reports of
thromboembolic phenomena, and the reports of transverse myelitis should have
10
Because it was evident that the Secretary intended to rely upon the Chao study, the
better practice would have been for Ms. Harris to present these cases in her initial posthearing
brief.
11
Dr. Slade and colleagues noted some of the limitations of their analysis, including
problems associated with the underlying VAERS reports. Exhibit K (Slade) at 756-57.
19
been grouped into one large category. Tr. 212-13. This approach is consistent
with Dr. Shoenfeld’s overall view that all autoimmune diseases are the same. Dr.
Shoenfeld asserted that “if we will combine[] [the reports from all categories] and I
will use the proper statistical analysis, I will find that it is statistically significant.”
Tr. 213. Dr. Shoenfeld did not actually perform this analysis, but he averred, “I
can assure you that as somebody can find that it’s not [statistically significant], I
can find that it is.” Tr. 929.
3. Mok
A third epidemiological study involving Gardasil was conducted by
researchers from Hong Kong. Merck funded the study and provided some
assistance. However, the primary investigator retained independence and did not
have any financial interest in Merck. Exhibit R (Chi Chiu Mok et al.,
Immunogenicity and safety of a quadrivalent human papillomavirus vaccine in
patients with systemic lupus erythematosus: a case-control study, Annals of the
Rheumatic Diseases (electronically published May 15, 2012)) at 6.
Dr. Mok and colleagues investigated Gardasil’s safety by giving the vaccine
to 50 women who suffered from stable lupus. They identified the number of flares
in these women and compared the number of flares to a control group of 50 women
with lupus who did not receive Gardasil. Exhibit R (Mok) at 1; Tr. 513-14, 528-
31.
The incidence of lupus worsening were similar. Exhibit R at 3; Tr. 530. Dr.
Eickhoff described this study as “reassuring,” although it was “small.” Tr. 531,
537.
Dr. Shoenfeld questioned the usefulness of this study. He asserted that all
the subjects in this experiment had a suppressed immune system from receiving
medication for their lupus. This suppressed immune system mitigated the effect of
the vaccine including any harmful consequences. Tr. 445-50, 940-44. Dr. Rose
countered that whether an anti-inflammatory medication would prevent recipients
of a vaccine from flaring is “an extremely complicated matter.” Tr. 659.
4. Verstraeten
Researchers at GlaxoSmithKline Biologics (“GSK”), led by Thomas
Verstraeten, conducted an integrated analysis of data from over 68,000 participants
in GSK-funded vaccine trials. Exhibit M (Verstraeten) at 6630. The objective of
the GSK analysis was to assess the occurrence of autoimmune-type adverse events
20
following aluminum-adjuvanted vaccination. Id. at 6631. The analysis included
GSK trials of AS04 adjuvanted HPV-16/18 (Ceravix), HSV and HBV (Fendrix)
vaccines. Id. The adjuvant AS04 is a combination of aluminum salt with a
lipopolysaccharide derivative called “MPL.” Id.
Verstraeten et al. found no increased risk of autoimmune disorders
associated with the aluminum-adjuvanted vaccines. Id. at 6637 (“results… do not
suggest any causal association between AS04 adjuvanted vaccines and
development of autoimmune disorders”). Dr. Rose referred to the Verstraeten
findings as an “encouraging” indication that future epidemiologic evidence
associating the HPV vaccine with lupus should not be anticipated. Exhibit A at 3-
4.
Dr. Shoenfeld interpreted the Verstraeten article very differently, relying on
it as evidence of hyperstimulation of the immune system following vaccination.
Tr. 75-76, 926-927. Dr. Shoenfeld emphasized the objective of the paper --
assessing the risks of adjuvanted vaccines -- rather than the findings. While
Verstraeten et al. provide a background of the immune-stimulating role of
adjuvants in vaccines, they found no increased incidence of lupus following
vaccination with an aluminum-adjuvanted HPV vaccine. Exhibit M (Verstraeten)
at 6631-34.
5. Conclusion regarding Epidemiological Studies
Collectively, these epidemiological studies weigh against finding that an
HPV vaccine contributes to an increased risk of lupus. Each of these studies has
some strength and some weaknesses. For example, the source for Dr. Chao’s
funding opens a potential (if ultimately unresolvable) argument that her
conclusions are not valid. But, funding as a potential source of bias or interest in
outcome is not an issue for Dr. Slade. Similarly, some studies have many
thousands of participants, but the Mok study involved fewer than 100. In short,
none of the epidemiological studies are perfect. But, a perfect scientific study is
not required by the relevant legal standards applying to Ms. Harris’s claim.
The overall effect of the epidemiological studies casts some doubt about the
persuasiveness and plausibility of Dr. Shoenfeld’s theories. If it were likely that
the HPV vaccine were causing lupus (regardless of the precise mechanism), then
there should be some evidence of an increased incidence of lupus. The studies
have not detected an increased incidence.
21
Even a very large epidemiological study cannot rule out conclusively the
possibility that the vaccine may cause lupus. Thus, the following section discusses
whether any of Dr. Shoenfeld’s theories proposing to explain a causal connection
between vaccination and lupus are persuasive. See Holmes, 115 Fed.Cl. at 486
(“Absent epidemiological evidence to support causation, it remained the job of
petitioner, not respondent, to supply a reputable medical or scientific explanation
of causation.”).
C. Dr. Shoenfeld’s Theories
Dr. Shoenfeld holds the broad opinion that “any vaccine can cause any
autoimmune disease at any time.” Tr. 406. As to the specific method for how a
vaccine can cause an autoimmune disease, Dr. Shoenfeld presented three theories
in a supplemental report that he prepared in response to an order. Exhibit 133.
The three theories are: (1) adjuvant-induced autoimmunity, (2) molecular mimicry,
and (3) bystander activation. Dr. Shoenfeld ranked the adjuvant theory as “the
most important.” Molecular mimicry was next, followed by bystander activation.
Tr. 156; see also Tr. 964 (indicating that the adjuvant part of a vaccine is probably
stronger than the viral part of a vaccine). These theories will be evaluated in the
sequence that Dr. Shoenfeld listed them, beginning with the most important, the
adjuvant theory.
1. Adjuvant
Adjuvants are substances that “enhance the immune system.” Tr. 38. They
are often incorporated into a vaccine because the vaccine contains a less potent
form of the substance (bacterium or virus) that causes the infection naturally. Tr.
37-38, 989-90.
Different compounds act as adjuvants. Common examples include
aluminum, pristane, squalene, and Freund’s adjuvant. Scientists have not
determined how any adjuvant stimulates the immune system, although they have
proposed various hypotheses. Tr. 38-41.
Dr. Shoenfeld has advanced the theory that the adjuvant in the HPV vaccine
can cause lupus. An important aspect of Dr. Shoenfeld’s theory is that he
considers all adjuvants to be the same. All adjuvants cause stimulation of the
immune system normally and in Dr. Shoenfeld’s theory the adjuvant causes an
22
abnormally hyperstimulated immune system. Tr. 167-68, 172-73; see also Tr. 669-
70 (Dr. Frenkel’s explanation of hyperstimulation).12
The Secretary’s experts disagreed with Dr. Shoenfeld’s assertion that all
adjuvants are the same. Tr. 687 (Dr. Rose: it is “crucially important to note that
[pristane and aluminum are] very different adjuvants and it is likely that they
worked in different fashions and that they have different immunologic
consequences”), 735-36 (Dr. Frenkel: “I think there's animal data that suggests that
pristane can cause autoimmune phenomenon. I don't think there's animal data that
is convincing… that aluminum can cause autoimmune phenomenon.”), 1001-02
(Dr. Cetaruk interpreting exhibit Y: “different adjuvants will elicit different
responses and, for that matter, a given adjuvant might elicit a different response at
a different dose.”). On this point, the Government’s experts were more persuasive
partly because the literature supported their view. A prominent support for treating
different adjuvants differently was the article by Michael Potter and Judith S. Wax.
Exhibit Y (Michael Potter & Judith S. Wax, Peritoneal Plasmacytomagenesis in
Mice: Comparison of Different Pristane Dose Regimens, 71(2) J. Nat’l Cancer
Inst. 391 (1983)). This study showed that different adjuvants (and the same
adjuvant in different doses) caused different immunological effects. Id.; Tr. 1001-
02. Dr. Shoenfeld, on the other hand, did not present any persuasive reason for
treating aluminum the same as pristane.
Because preponderant evidence suggests that pristane may stimulate the
immune system in a way that aluminum does not, Dr. Shoenfeld’s extensive
discussion of studies involving pristane is not relevant. Thus, the Wesley Reeves
studies (Tr. 486) are not discussed, although they were considered. Instead of
analyzing evidence involving an adjuvant that Bre did not receive, it is more useful
to focus on the adjuvant present in the HPV vaccine that Bre received, aluminum.
Bre’s exposures to aluminum through the two doses of the HPV vaccine
were not her only exposures to aluminum. Aluminum is present in most drinking
water and in many foods. Tr. 180. Dr. Cetaruk, the toxicologist, explained that the
method of exposure (for example, ingestion or intramuscular injection) affects how
much of the substance remains available to the body. Tr. 1104-08. In the normal
course of digestion, the body largely eliminates aluminum. Tr. 1107.
12
Dr. Shoenfeld's presentation emphasized the effect of the adjuvant on the immune
system. However, he did also mention that the adjuvant could also have a toxic effect. Tr. 175-
76.
23
Additionally, there is some evidence that the body also eliminates aluminum
that is injected as part of a vaccine. “Preliminary animal experiments have shown
that the aluminum adjuvants are dissolved by citrate in the interstitial fluid, leaving
the body rapidly. The ability of the body to eliminate aluminum-containing
adjuvants may be partly responsible for the excellent safety record of these
adjuvants.” Exhibit BB (Thomas C. Eickhoff & Martin Myers, Workshop
summary: aluminum in vaccines, 20 Vaccine S1 (2002)) at S2.13
Considering if aluminum could cause lupus initially raises the question of
whether the persistence of aluminum in the body could explain why lupus is a
chronic disease. See Tr. 956-57. Dr. Shoenfeld did not state whether he expected
aluminum would persist in the body long enough to cause a chronic disease like
lupus. However, Dr. Shoenfeld also answered “absolutely” to the question “if the
aluminum is excreted from the body quickly[,] it still can cause lupus?” Tr. 957.
To support the proposition that aluminum from a vaccine may remain in the
body, Dr. Shoenfeld cited the work led by Romain Gherardi. Tr. 69-72, 173-74,
957-59. Dr. Gherardi’s work was one of two sets of studies investigating
aluminum’s effect on living beings. Dr. Gherardi showed that aluminum may
remain at the site of an injected vaccine for years. Exhibit 137 (Romain K.
Gherardi & François-Jérȏme Authier, Aluminum inclusion macrophagic
myofasciitis: a recently identified condition, 23(4) Immunology Allergy Clinics N.
Am. 699 (2003)) at 703. Many people suffered from chronic fatigue as well as
muscle pain, and Dr. Gherardi coined the phrase macrophagic myofasciitis,
frequently abbreviated as MMF, to describe this condition.14 Id. at 702-03.
The World Health Organization (“WHO”) acted in response to Dr.
Gherardi’s findings. The WHO investigated whether people whose vaccination
sites contained a persistent amount of aluminum suffered any multi-system
disorder. The WHO concluded that “MMF represent[s] a simple marker of
vaccination with long-term persistence of aluminum at the injection site and local
inflammatory response to it, without other symptoms or consequences.” Exhibit Z
13
At first, Dr. Shoenfeld agreed with this assessment. But, he also added that the
reference to S in the pagination meant that this article came from a supplemental issue of the
journal and supplements are not peer-reviewed. Tr. 462-65.
14
Although Dr. Gherardi uses the term MMF to describe a group of symptoms, others
have associated the term with the histologic lesion described by Dr. Gherardi in 1998. Exhibit
BB (Eickhoff) at S3.
24
(Statement from the Global Advisory Committee on Vaccine Safety on aluminum-
containing vaccines, World Health Organization (last reviewed Dec. 3, 2008)); see
also exhibit BB (Eickhoff) at S4 (“Causality has not been established for Dr.
Gherardi’s claim that MMF, the histologic entity, is associated with a ‘symptom
complex’ of fatigue and ascending myalgias”); but see Tr. 462-65 (Dr. Shoenfeld:
“Supplements are not peer reviewed.”). The WHO reached this conclusion based
on, among other work, an experiment that scientists from Aventis Pasteur
performed on monkeys. This study found that monkeys who received an injection
of aluminum, which persisted at the injection site, did not have any abnormal
clinical signs. See exhibit CC (François Verdier et al., Aluminum assay and
evaluation of the local reaction at several time points after intramuscular
administration of aluminum containing vaccines in the Cynomolgus monkey, 23
Vaccine 1359 (2005)); see also Tr. 1021-23.
Another set of studies involving aluminum and living beings was conducted
by a group of researchers led by Dr. Christopher Shaw. Dr. Shaw explored
whether vaccines given to military personnel contributed to their development of
Gulf War syndrome. Tr. 1036-37; see also Tr. 73-75. Dr. Shaw and colleagues
gave mice the amount of aluminum equivalent to the amount of aluminum
contained in the anthrax vaccine. These mice displayed some cognitive problems
and were found to have fewer neurons in their spinal cord. Exhibit 143 (Michael
S. Petrik et al., Aluminum Adjuvant Linked to Gulf War Illness Induces Motor
Neuron Death in Mice, 9 NeuroMolecular Med. 83 (2007)); Tr. 1039-42.
Dr. Shoenfeld interpreted the Petrik study as showing “an adjuvant [can]
cause a strenuous effect on different systems in our body, and specifically, the
immune system.” Tr. 75. In Dr. Shoenfeld’s opinion, the mice’s “cognitive
impairment is [evidence of] autoimmunity and it is believed that the deaths of the
neurons is also autoimmune in nature.” Tr. 172. However, Dr. Cetaruk asserted
that the only immunologic test on these mice showed an increased number of
antibodies to squalene. Tr. 1039. Consequently, Dr. Cetaruk stated that the Petrik
study was useful for looking at motor neuron diseases, such as amyotrophic lateral
sclerosis, and cognitive diseases only. Tr. 1043.
Without citing any specific articles, some experts discussed how an
unusually high exposure to aluminum affects people. For example, years ago, the
dialysis solution used for people with impaired kidneys contained aluminum
creating an exposure to aluminum. Dr. Cetaruk said that dialysis patients receiving
this formulation of solution often accumulated aluminum in their kidneys as they
are unable to excrete it normally. Tr. 1011, 1025, 1078. In addition, welders have
25
higher than normal exposure to aluminum. Tr. 1101. Dr. Cetaruk asserted that
neither group had an increased incidence of lupus. Tr. 1101-02.
In sum, Ms. Harris has not established the persuasiveness of Dr. Shoenfeld’s
theory that the aluminum adjuvant in the HPV vaccine can cause lupus. The
evidence surrounding this theory suggests that the theory is not reliable. In the
mice model involving aluminum from Dr. Petrik’s group, the mice exposed to
aluminum developed some cognitive impairment and, more drastically, lost
neurons in their spinal cord. These symptoms are not characteristic of lupus, even
though cases of lupus may involve cognitive problems. The monkeys in Dr.
Verdier’s experiment did not development any systemic disease after they were
injected with aluminum. Similarly, the people with MMF were not reported to
have developed any autoimmune disease like lupus. Finally, the anecdotal
information about dialysis patients and welders was that they, too, did not develop
lupus. In short, while a dose of aluminum in an amount exceeding the normal
exposure could, as a purely theoretical matter, cause some disease, there is no
persuasive evidence that an aluminum-caused disease would look anything like
lupus.
A specific finding that an aluminum adjuvant is not likely to cause lupus is
in accord with the general information about aluminum adjuvants. Aluminum has
been included as an adjuvant in vaccines since the 1920’s. During this time,
billions of doses of vaccines with aluminum adjuvants have been administered and
the adjuvant in the vaccine has been considered safe. Exhibit M (Verstraeten) at
6637. Ms. Harris has not presented any persuasive evidence to create an exception
for lupus.
2. Molecular Mimicry
In a single paragraph, Dr. Shoenfeld’s May 6, 2012 report presented
molecular mimicry as another theory to explain how the HPV vaccine can cause
lupus. He stated: “an infectious antigen incorporated in vaccines . . . may resemble
host antigens.” Exhibit 133 at 3. The vaccinee may develop an autoimmune
condition when “the autoantibodies against the infectious agent or the vaccine
ingredients, ‘home’ to tissue antigens which have a similar (molecular mimicry)
structure.” Id.
In his testimony, Dr. Shoenfeld attempted to establish the foundation for this
theory. He stated that the medical community understands that an infection with
the streptococcus bacteria can cause rheumatic fever because the streptococcus
26
bacteria contain a substance, known as an M protein, that is also present in the
heart. Tr. 84-86.
Dr. Shoenfeld also cited a paper in which he, as a co-author, identified how
other combinations of pathogens and host antigens could cause a disease. Exhibit
138 (Miri Blank et al., Molecular Mimicry and Auto-Immunity, 32 Clinical Rev. in
Allergy & Immunology 111 (2007)) at 113; Tr. 89-90.15 The Blank authors used a
computer to screen antibodies to find evidence of similarities with organs. In this
paper, Dr. Shoenfeld stated “not every crossreaction or homology in amino acid
sequences between a self-infecting and infecting agent has a biological function.”
Exhibit 138 at 112; Tr. 470. The Blank researchers did not disclose the minimum
number of amino acids that is needed to establish homology but, in his testimony,
Dr. Shoenfeld asserted that as few as four amino acids could be sufficient. Tr. 146.
The Secretary’s experts questioned the reliability of using molecular
mimicry to explain how the HPV vaccine can cause lupus. Preliminarily, Dr. Rose
and Dr. Frenkel agreed that molecular mimicry was a biologically plausible
explanation for why rheumatic fever sometimes follows an infection with
streptococcus bacteria. Tr. 625-29, 672, 692-93. But, neither Dr. Rose nor Dr.
Frenkel saw any evidence that components of the HPV vaccine shared homology
with the parts of the body involved in lupus. Tr. 638 (Dr. Rose: “I did not see
homology data between any of Bre’s human tissue . . . with the L1 component of
the vaccine”), 673 (Dr. Frenkel).
Dr. Shoenfeld agreed that homology has not been established. When asked
about this topic, he stated “We don’t know yet. . . . Nobody so far [has] tested for
molecular mimicry except of the measles [vaccine]. . . . I believe that in the future
it will be found by having what we call genomic analysis.” Tr. 147. Later, Dr.
Shoenfeld asserted that if his laboratory received Gardasil from the manufacturer,
he could conduct the relevant study “in two weeks’ time.” Tr. 473.
The lack of established homology is an impediment to accepting as
persuasive Dr. Shoenfeld’s theory that the HPV vaccine can cause lupus via
molecular mimicry. Dr. Shoenfeld’s assertion of the theory, by itself, does not
carry the petitioner’s burden of presenting a persuasive and reliable theory. See
Moberly, 592 F.3d at 1325. One criterion that a special master may use in
15
Dr. Shoenfeld also referred to a paper by Dimitri Bogdanos. However, the Secretary
objected to testimony on this paper because Dr. Shoenfeld did not cite the paper and the
petitioner did not file it. Tr. 87-90.
27
evaluating the reliability of a theory is whether the theory can be tested and
whether it has been tested. See Terran v. Sec'y of Health & Human Servs., 195
F.3d 1302, 1316 (Fed. Cir. 1999) (citing Daubert v. Merrell Dow Pharm., Inc., 509
U.S. 579 (1993)). Here, the Blank paper demonstrates that homology can be
established and Dr. Shoenfeld acknowledged that his colleagues and he could
perform the necessary test. However, this testing has not been done and this lack
of testing for homology undercuts the persuasiveness of the theory. 16
3. Bystander Activation
The third theory proposed in Dr. Shoenfeld’s May 6, 2012 report was
bystander activation. Under this theory, the exposure to an infectious antigen (or
vaccine) prompts lymphocytes to go to the area of infection and inflammation
develops. The inflammation, in turn, damages or destroys tissue and the damage
exposes other host parts to the immune system. The immune system sends
additional lymphocytes to attack the host tissue. Exhibit 133 at 4. Dr. Shoenfeld’s
testimony was similar. Tr. 476-81; see also Tr. 93-95, 147-51. In support of the
bystander activation theory, Dr. Shoenfeld cited two articles, one published in
1989 and the other published in 1998. Exhibit 133 at 4.
Dr. Shoenfeld stated that bystander activation was his least preferred theory,
falling after adjuvant induced autoimmunity and molecular mimicry. Tr. 156. In
Dr. Shoenfeld’s view, bystander activation was relatively weaker than the other
two theories, although still biologically plausible, because there are no
experimental models for bystander activation. Id. He also described bystander
activation as “one of the first theories for autoimmunity.” Tr. 129. But, “[t]oday,
people believe more in the molecular mimicry, and the toll-like receptor activity
and so forth.” Id.
The Secretary’s experts did not discuss bystander activation extensively. On
cross-examination, Dr. Frenkel indicated that bystander activation might be a
plausible explanation for some autoimmune diseases but not necessarily an
16
Identifying some homology between the HPV vaccine and host tissue would simply be
one step to establishing that the vaccine can cause a disease via molecular mimicry. Homology
is a necessary step, but not a sufficient step, along this pathway because, as Dr. Shoenfeld stated,
“not every . . . homology in amino acid sequences . . . has a biological function.” Exhibit 138 at
112. Because there is no evidence of homology in this case, it is not necessary to resolve
whether evidence of homology is a persuasive basis for inferring causation in the Vaccine
Program.
28
explanation for lupus. Tr. 693. Dr. Rose did not see any persuasive evidence
regarding bystander activation and could not say that bystander activation was a
biologically plausible theory. Tr. 638-39.
Overall, the evidence surrounding bystander activation was not persuasive.
The theory appears to be an older theory now supplanted by other ideas such as
molecular mimicry. When Dr. Shoenfeld was asked whether he believed that
bystander activation was a more-likely-than-not explanation, he responded
“Absolutely no.” Tr. 157.
D. Conclusion regarding Althen Prong One
Ms. Harris’s claim that the HPV vaccine can cause lupus falls short in
several respects. She has advocated that the appropriate benchmark is a plausible
medical theory, but the Federal Circuit has consistently and explicitly rejected that
standard. Under the statutory standard, which is preponderance of evidence, Ms.
Harris’s evidence is lacking.
The Secretary has introduced a strong type of evidence, epidemiological
studies, that suggest the HPV vaccine is unlikely to cause lupus. Ms. Harris
countered with the presentation of case reports. But, case reports are generally not
a valuable form of evidence as the Federal Judicial Center has explained. Hence,
although the case reports were considered, they are not discussed.
Through Dr. Shoenfeld, Ms. Harris has proposed three theories to connect
the HPV vaccine to lupus. Ms. Harris has not demonstrated the persuasiveness of
these theories. They are much more like untested hypotheses than valid theories to
explain how HPV vaccine can cause lupus. Although additional study and testing
may ultimately show that sound and reliable science underlies Dr. Shoenfeld’s
theories, the record in this case contains too much extrapolation and conjecture for
the theories to be accepted. See La Londe v. Sec'y of Health & Human Servs., 110
Fed. Cl.184, 201 (2013) (the petitioner’s expert “could not back up his hypothesis
with a reliable medical or scientific explanation. . . . [The special master] quite
properly required petitioner to carry her burden to bring forward a reliable medical
or scientific explanation”), aff’d 746 F.3d 1334, 1340 (Fed. Cir. 2014); Langland
v. Sec'y of Health & Human Servs., 109 Fed. Cl. 421, 441 (2013) (“the Special
Master did not commit a legal error by requiring a sufficiently-detailed explanation
of how” a vaccine can cause a disease); Taylor v. Sec'y of Health & Human Servs.,
108 Fed. Cl. 807, 819 (2013) (“the mere existence” of expert testimony about a
29
theory “is insufficient to satisfy the burden of showing a ‘persuasive’ medical
theory --- this theory must also preponderate”).
VII. Althen Prong Three -- Timing
In addition to presenting a reliable medical theory explaining how the HPV
vaccine can cause lupus, Ms. Harris must also show that Bre’s first manifestation
of lupus occurred in a medically appropriate timeframe to infer causation. Bazan
v. Sec’y of Health & Human Servs., 539 F.3d 1347, 1352 (Fed. Cir. 2008). To
satisfy the third Althen prong, petitioner’s burden is to present “preponderant proof
that the onset of symptoms occurred within a timeframe which, given the medical
understanding of the disorder’s etiology, it is medically acceptable to infer
causation.” Bazan, 539 F.3d at 1352; accord Shapiro v. Sec'y of Health & Human
Servs., 101 Fed. Cl. 532, 542-43 (2011), reconsideration denied after remand, 105
Fed. Cl. 353 (Fed. Cl. 2012), aff’d without opinion, 503 Fed. Appx. 952 (Fed. Cir.
2013).
Dr. Shoenfeld presented two ideas regarding the amount of time that is
expected to pass if a vaccine caused lupus. The first concept was, to use Dr.
Shoenfeld’s word, the “classic” amount of time, three weeks. Tr. 26; accord Tr.
96-97. The second idea can be considered a new understanding of the temporal
relationship, although Dr. Shoenfeld did not use the word “new.” In Dr.
Shoenfeld’s view, because aluminum persists in the body, the interval between
vaccination and the onset of disease can be much longer than previously expected.
Tr. 152, 181-87. Dr. Shoenfeld was willing to accept a seven-year interval as
plausible. Tr. 220.
Although Dr. Shoenfeld’s extended latency has previously been found
problematic, see Hennessey v. Sec'y of Health & Human Servs., No. 01-190, 2009
WL 1709053, at *54-56 (Fed. Cl. Spec. Mstr. May 29, 2009), mot. for rev. den’d,
91 Fed. Cl. 126, 134-35 (2010), an analysis of multi-year interval is not needed
here. Dr. Rose accepted the proposition that an interval of approximately one
month between the vaccination and the onset of symptoms would be an appropriate
interval from which to infer causation. See Tr. 620-22.17
17
Dr. Frenkel did not agree. He stated that there is no classic time between the
introduction of an antigen to the onset of disease. Tr. 735. Similarly, he also opined that if Bre
did not have lupus before the HPV vaccination and if she developed lupus after the HPV
(continued…)
30
Thus, a critical part of the prong-three inquiry is when Bre developed lupus.
The parties’ conflicting positions are set forth below, followed by an analysis.
Parties’ Onset Arguments
Dr. Shoenfeld proposed that Bre fit within the classical amount of time
(three weeks) because she received the second dose of the HPV vaccine on August
1, 2007, and presented with a spreading, itchy rash on her body and face on August
23, 2007. Exhibit 1 at 1; exhibit 26 at 4. The report from August 23, 2007,
describes Bre’s rash as “spreading, itchy….er[y]thematous spots on arms and
trunk.” Exhibit 26 at 4. Dr. Shoenfeld accepted this rash as a manifestation --- the
initial manifestation --- of Bre’s lupus. Exhibit 32 at 2-3. In other words, Dr.
Shoenfeld sees evidence of Bre suffering from lupus before October 1, 2007, when
she was actually diagnosed with the disorder. Exhibit 4 at 13.
The Secretary’s experts shared Dr. Shoenfeld’s perspective in the sense that
Dr. Rose and Dr. Frenkel also viewed Bre’s history as consistent with lupus before
her actual diagnosis. Dr. Rose and Dr. Frenkel part company with Dr. Shoenfeld,
however, because they think Bre could have had lupus even before she was
vaccinated. Consistent with the theory that lupus is based in part on genetic
factors, Dr. Frenkel stated that Bre could have been suffering from lupus for years
before April 2007. Tr. 698-99. The most relevant abnormal health issue was a
recurrent rash. Dr. Frenkel cited a report from Bre’s pediatrician that she had had a
rash for several years. Exhibit C at 2 (citing exhibit 26 at 3 (history of “a macular,
raised, itchy rash”)).
Furthermore, more than four months before her August 23, 2007
vaccination, Bre presented with a “recurrent rash over complete body.” Dr.
Vanderburg’s recitation of Bre’s history was that the recurrent rash was “macular,
raised, [and] itchy.” Exhibit 26 at 3. Following a physical examination, Dr.
Vanderburg stated Bre had “er[y]thematous spots on arms and trunk.” Id. at 4. He
diagnosed her as suffering from pityriasis rosea. Exhibit 26 at 3. In his expert
report, Dr. Rose stated that the treatment record lacks description of a “pattern of
distribution or presence of [a] ‘herald lesion’, two important elements for the
diagnosis of [pityriasis rosea].” Exhibit A at 1. Similarly, in his testimony, he
averred that he was “suspicious of the rash in April” as evidence that Bre’s lupus
pre-dated the vaccinations. Tr. 616.
vaccination, this sequence of events would present a “temporal association,” not a “logical causal
relationship.” Tr. 706.
31
Agreeing with Dr. Rose, Dr. Frenkel also opined that Bre’s April 2007 rash
was a manifestation of her lupus. Dr. Frenkel stated that recognizing whether a
rash is a sign of lupus is challenging for doctors and, sometimes, a doctor’s
diagnosis of pityriasis rosea is mistaken. Tr. 694-98. Thus, he opined that “Bre
had symptoms of a disease that would later manifest itself [as] SLE months to a
couple of years prior to her being diagnosed in September [2007].” Tr. 699-700.
On cross-examination, Dr. Frenkel expanded the basis for his conclusion
that Bre suffered from lupus before April 17, 2007. When Dr. Frenkel was asked
an open-ended question about what “other sign or symptom” supported his
statement that Bre had lupus before vaccination, he referred to laboratory studies of
her erythrocyte sedimentation rate (“sed rate” or “ESR”), C-reactive protein
(“CRP”), and white blood count. Tr. 700. Later, Dr. Frenkel acknowledged that
his report did not mention the results of these tests as a basis for his conclusion
about when Bre began suffering from lupus. Dr. Frenkel justified this addition
because he “did some more thinking” in preparing to testify. Tr. 721.
Introducing a new basis for an opinion during a hearing is hardly an ideal
practice. Dr. Frenkel should have disclosed that the various laboratories studies
contributed to his opinion in his report. This disclosure would have permitted Ms.
Harris’s attorney and Dr. Shoenfeld an opportunity to consider this aspect of Dr.
Frenkel’s opinion before the hearing. Perhaps in recognition of the omission from
Dr. Frenkel’s report, the Secretary has not cited Bre’s sed rate, etc. as evidence that
her lupus existed before the vaccination. See Resp’t’s Br. at 21-23.
On the other hand, the questioning by Ms. Harris’s attorney opened the door
for Dr. Frenkel’s extra opinion. She did not move to strike this testimony on the
ground that it was not contained in his expert report. As such, this testimony
remains in the record and it is incumbent upon the special master to consider it. 42
U.S.C. § 300aa—13(a)(1).
The foundation for Dr. Frenkel’s opinion is a set of results from various
laboratories studies. These are set forth in the following table:
Source Exhibit 2 at 50-51 Exhibit 3 at 158-60,
167
Date March 20, 2007 (before Sept. 16, 2007 (after
vaccination) vaccination)
White Blood Count (K/uL), 6.87 3.88, marked low
Reference 4.5-13.5
32
ESR (MM/HR), Reference 35.0, marked high 49.0, marked high
0.0-20.
CRP (MM/HR), Reference 17.3, marked high < 3.0
0.0-10.
In Dr. Frenkel’s opinion, the elevated scores for the sedimentation rate and
the C-reactive protein in March 2007, indicate that Bre was suffering from lupus at
that time. A commonly used reference guide supports Dr. Frenkel’s opinion that
elevated sedimentation rates and elevated C-reactive proteins are consistent with
lupus. Kathleen Deska Pagana & Timothy J. Pagana, Mosby’s Manual of
Diagnostic Laboratory Tests (4th ed. 2010) at 197-99, 234-36. In addition, Bre’s
white blood count was toward the low end of the normal reference range despite
her having an infection, which normally leads to an elevated white blood count.
Tr. 700; see also Tr. 1113-14 (Dr. Rose’s confirmation that lupus can depress
white blood counts).
During the rebuttal phase of the case, Dr. Shoenfeld had an opportunity to
address the March 2007 laboratories studies. However, his opinion was not clear.
He acknowledged that sedimentation rates between 30 and 50 are “accelerated,”
indicating “mild inflammation.” But, without much elaboration, Dr. Shoenfeld
opined that a severe inflammatory disease, like lupus, is a consideration when the
sedimentation rate exceeds 100. Tr. 937.18
Onset Findings
Determining when Bre began suffering from lupus is difficult for at least
two reasons. First, as a general matter, lupus presents in many ways. Dr.
Shoenfeld stated that lupus is known as the “disease of 1,000 faces.” Tr. 194.
With such variability, different doctors may detect lupus earlier than other doctors.
See Tr. 564 (Dr. Rose).
18
Dr. Shoenfeld also commented upon the difference between the elevated sedimentation
rate and the decreased C-reactive protein in September 2007. In his view and in the opinion of
Dr. Rose, these values do not always move in parallel in lupus. Tr. 938-39, 949-54, 1112-13. A
rheumatology textbook supports these opinions. Irving Kushner & Stanley P. Ballou, Chapter
52: Acute-Phase Reactants and the Concept of Inflammation, Kelley’s Textbook of
Rheumatology 771 (Gary S. Firestein et al. eds., 8th ed. 2009).
33
Second, for Bre specifically, her remote medical history is not as well
documented as it could have been. Although Dr. Vanderburg’s April 17, 2007
record states that Bre has been having a rash “for several years,” there are no
records from physicians describing the rash.19 In addition, there are no
photographs of any of the rashes Bre experienced that could aid the experts in
evaluating her case. Nevertheless, there is sufficient information to evaluate how
the evidence preponderates.
The stronger evidence supports a finding that Bre was suffering from lupus,
albeit undiagnosed, when she received her first HPV vaccination on April 17,
2007. Several reasons support this finding.
First, Bre presented with a rash on this date. Dr. Vanderburg’s description
of the rash --- “macular, raised [and] itchy” --- is similar to the advance practice
nurse’s description of the rash on August 23, 2007 --- “bright spots all over [her]
body,” “spreading,” and “itchy.” Compare exhibit 26 at 3 with exhibit 26 at 4. Dr.
Shoenfeld accepted the latter description as a manifestation of lupus, but he
rejected the former.
Dr. Shoenfeld has a legitimate, yet ultimately unpersuasive, basis for
disregarding the April 17, 2007 rash. Dr. Vanderburg stated that Bre suffered from
pityriasis rosea. However, as Dr. Rose and Dr. Frenkel explained, the words that
Dr. Vanderburg used to describe Bre’s rash do not match a typical description for
pityriasis rosea. Most notably, there is usually a “herald patch.” Exhibit DD
(Sidney Hurwitz, Chapter 5: Papulosquamous and Related Disorders, Clinical
Pediatric Dermatology (2d ed. 1993)) at 122. But, Dr. Vanderburg did not describe
anything like a herald patch. This dissimilarity calls into question the accuracy of
Dr. Vanderburg’s diagnosis. See Tr. 694-98.
Second, Bre has experienced rashes periodically for years. There was no
testimony suggesting that these episodes were also manifestations of pityriasis
rosea. Recurrence would be unlikely for pityriasis rosea, which is “self-limiting”
and is complete by “14 weeks.” See exhibit DD (Hurwitz) at 122-23. However,
lupus waxes and wanes with its sufferers experiencing flares unpredictably.
Third, Dr. Rose’s presentation was impressive. He appeared to be interested
in providing an accurate assessment of Bre’s situation, regardless of how his
19
The Secretary did not specifically request these records and the special master
presiding at the time also did not request these records.
34
testimony would affect the outcome of the case. His opinion that Bre may have
had lupus at the time of her vaccination, therefore, carries a great deal of weight.
His opinion is meaningful, in part, because his expertise in pediatric rheumatology
gives him insights into lupus that other physicians may not have.
A reliance on a specialist’s understanding of a disease has precedential
support. In Locane, the petitioner unquestionably suffered from Crohn’s disease
and she claimed that she started experiencing symptoms of Crohn’s disease shortly
after receiving the hepatitis B vaccine. The Secretary presented the opinion of a
doctor who, among other achievements, wrote a book about Crohn’s disease. His
opinion was that the petitioner was suffering from Crohn’s disease before she was
vaccinated and this opinion was credited. Locane v. Sec'y of Health & Human
Servs., No. 99-589V, 2011 WL 3855486, at *6-8 (Fed. Cl. Spec. Mstr. Feb. 17,
2011). Finding that the special master’s decision to credit the Secretary’s expert
on Crohn’s disease was not arbitrary, the Court of Federal Claims denied
petitioner’s motion for review, 99 Fed. Cl. 715, 726 (2011), and the Federal Circuit
affirmed. 685 F.3d 1375, 1380 (Fed. Cir. 2012).
Fourth, the blood tests from March 20, 2007, are consistent with lupus.
They show that when Bre was suffering from a MRSA infection, her white blood
count, which should have been quite high, was toward the bottom of the normal
range. Exhibit 2 at 50-51. Although, as a matter of procedure, Dr. Frenkel should
have included this information with his report, Ms. Harris and Dr. Shoenfeld had
an opportunity to address it. In his rebuttal testimony, Dr. Shoenfeld
acknowledged that the sedimentation rate was high and consistent with “mild”
inflammation. Tr. 936-37. Dr. Shoenfeld did not persuasively explain why only
mild inflammation was not consistent with someone suffering from lupus.
All these reasons support a finding that Bre had lupus before she was
vaccinated. It is important to emphasize that the standard for adjudication is
merely a preponderance of the evidence. 42 U.S.C. § 300aa—13; cf. Knudsen, 35
F.3d at 549 (discussing the burden of proof when the Secretary attempts to
establish an alternative factor as the cause for a presumed Table injury). If the
standard for adjudication were more taxing, then this finding might not be made
because much about Bre’s condition before vaccination is not known.
Nevertheless, there is some evidence about Bre’s health before vaccination and this
evidence preponderates in favor of finding that Bre was already suffering from
lupus before vaccination.
35
When a disease affects a vaccinee before vaccination, that person may not
receive compensation based upon a theory that the vaccine caused the illness. See
Locane, 685 F.3d at 1381 (logical to conclude vaccine did not cause the alleged
disease when finding that petitioner suffered from the alleged disease prior to
vaccination). However, the person may proceed on a theory that the vaccine
worsened the pre-existing condition. W.C., 704 F.3d at 1358.
Here, Ms. Harris has not presented any argument based upon a theory of
significant aggravation. Although Dr. Rose and Dr. Frenkel expressed the opinion
that Bre suffered from lupus before vaccination, exhibit A at 2, exhibit C at 3-4,
Dr. Shoenfeld did not present an alternative theory involving significant
aggravation in his supplemental reports. See exhibit 118; see also exhibit 119.
Similarly, Ms. Harris did not argue for significant aggravation. See Pet’r’s
Posthr’g Br.
Consequently, the finding that Bre suffered from lupus before receiving the
HPV vaccination is another flaw in her case. Even if, contrary to the finding made
in section VI. above, she had established that the HPV vaccine can cause lupus,
Ms. Harris would be required to establish the appropriate temporal interval. She
cannot make this showing and this failure is another reason to deny Bre
compensation.
VIII. Althen Prong Two -- Logical Sequence
The final aspect of Ms. Harris’s causation claim is to establish by
preponderant evidence “a logical sequence of cause and effect” showing that the
HPV vaccine caused Bre’s lupus. Althen, 418 F.3d at 1274. Because Ms. Harris
has failed to demonstrate that the HPV vaccine can cause lupus generally, see
section VI., above, she cannot be found to have established that the HPV vaccine
did cause her lupus specifically. See Caves v. Sec'y of Health & Human Servs.,
07-443V, 2010 WL 5557542, at *9-*19 (Fed. Cl. Spec. Mstr. Nov. 29, 2010), mot.
for rev. den’d, 100 Fed. Cl. 119, 145 (2011), aff'd per curiam without opinion, 463
F. App'x 932 (Fed. Cir. 2012). Moreover, as explained in the preceding section,
the sequence of events (development of lupus followed by vaccination) prevents a
finding in Ms. Harris’s favor on this prong. See Locane, 685 F.3d at 1381.
Nevertheless, for sake of judicial efficiency, the evidence Ms. Harris cited
regarding this remaining prong will be discussed.
36
Ms. Harris relies upon two sources of information to establish this element.
First, she cites Dr. Shoenfeld’s opinion. Second, she cites a medical record from
her treating pediatrician, Dr. Vanderburg. See Pet’r’s Posthr’g Br. at 27, 37.
Dr. Shoenfeld’s reasoning was that: (1) the HPV vaccine can cause lupus,
(2) there is an appropriate and classical temporal association between the second
dose of the vaccine and the onset of lupus, and (3) the lack of alternative cause for
the lupus. To these factors, Dr. Shoenfeld also added that Bre was genetically
predisposed to suffer an autoimmune disease. See Pet’r’s Posthr’g Br. at 27.
However, the Federal Circuit has rejected this logic as sufficient to meet
petitioner’s burden of proof under Althen prong two. See Hibbard, 698 F.3d at
1365-66.20
Besides Dr. Shoenfeld’s opinion, Ms. Harris cites to a record from Dr.
Vanderburg, who saw Bre about one year after her diagnosis. In the “history of
present illness” portion of the report, Dr. Vanderburg states, “[I]mmun.[ ]reactions
she continues to deal with her lupus. [R]heumatology feels that this was brought
on by her [G]ard[a]sil shot.” Exhibit 26 at 32. The parties have not located any
report from a rheumatologist who purportedly stated that the HPV vaccine had
caused Bre’s lupus. Tr. 663. During the hearing, Ms. Harris elicited testimony
from the experts about their understanding of Dr. Vandenberg’s note. Tr. 106,
643-44.
In contrast to this unidentified rheumatologist, the Secretary identifies other
doctors who treated Bre, were aware that Bre had received the HPV vaccine, but,
nonetheless, did not associate Bre’s lupus with her previous vaccination. See
Resp’t’s Posthr’g Br. at 23. Significantly, the Secretary also relies upon one doctor
who indicated that the HPV vaccine did not cause Bre’s lupus. On August 11,
2008, over a year since Bre received her HPV vaccines, Ms. Harris called Bre’s
neurologist to report a possible seizure and her concern “that symptoms began
shortly after having Gard[a]sil injection.” Dr. Fulton requested that his nurse “let
Mom know that the Gard[a]sil injection/reaction would have taken place 24 to 36
hours after injection.” Exhibit 4 at 165-66.
20
In Hibbard, the petitioner's argument was based upon only the first three points and did
not include a reference to "genetic predisposition." However, Bre's genetic predisposition to
develop an autoimmune disease also suggests that she was disposed to developing an
autoimmune disease without receiving a vaccination.
37
Taken as a whole, the records of Bre’s treating doctors do not persuasively
show that they believed the HPV vaccine caused Bre’s lupus. Consequently, Ms.
Harris has failed to meet her burden of proof for the second Althen prong.
IX. Conclusion
Although Bre’s severe disease is regrettable, Congress limited the
compensation available from the Vaccine Program to only those people who have
demonstrated that a vaccine caused or significantly aggravated an illness. Ms.
Harris has not made this showing. Consequently, she is not entitled to
compensation.
The Clerk’s Office is instructed to issue judgment in accord with this
decision.
IT IS SO ORDERED.
s/ Christian J. Moran
Christian J. Moran
Special Master
38