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© 2022 College of American Pathologists


Autopsy Histopathologic Cardiac Findings in Two Adolescents Following the Second

COVID-19 Vaccine Dose

James R. Gill, MD; Randy Tashjian, MD; Emily Duncanson, MD

Connecticut Office of the Chief Medical Examiner, Farmington, Connecticut, (Gill); Department

of Pathology, Yale School of Medicine, New Haven, Connecticut (Gill); Wayne County Medical

Examiners’ Office, Detroit, Michigan (Tashijan); Department of Pathology, University of

Michigan, Ann Arbor, Michigan (Tashijan); Jesse E. Edwards Registry of Cardiovascular

Disease, St. Paul, MN (Duncanson)

Corresponding author:

James Gill, MD

OCME

11 Shuttle Rd

Farmington, CT 06032

jgill@ocme.org

Supplemental digital content can be found at the end of article.

The authors have no relevant financial interest in the products or companies described in this article.

Running title: COVID-19 Heart Vaccine

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ABSTRACT

Context.– Myocarditis in adolescents has been diagnosed clinically following the administration

of the second dose of an mRNA vaccine for coronavirus disease 2019 (COVID-19).

Objective.– To examine the autopsy microscopic cardiac findings in adolescent deaths that

occurred shortly following administration of the second Pfizer-BioNTech COVID-19 dose to

determine if the "myocarditis" described in these instances has the typical histopathology of

myocarditis.

Design.– Clinical and autopsy investigation of two teenage boys who died shortly following

administration of the second Pfizer-BioNTech COVID-19 dose.

Results.– The microscopic examination revealed features resembling a catecholamine-induced

injury, not typical myocarditis pathology.

Conclusions.– The myocardial injury seen in these post-vaccine hearts is different from typical

myocarditis and has an appearance most closely resembling a catecholamine-mediated stress

(toxic) cardiomyopathy. Understanding that these instances are different from typical

myocarditis and that cytokine storm has a known feedback loop with catecholamines may help

guide screening and therapy.

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Myocarditis in adolescents (particularly teenage boys) has been reported following the

second dose of the Pfizer-BioNTech COVID-19 vaccine.1-7 Since cardiac biopsies are rarely

performed in these instances with clinically stable patients, the myocardial pathology has not

been clearly elucidated.8 Myocarditis is rarely diagnosed at autopsy in deaths due to severe acute

respiratory syndrome coronavirus 2 (SARS‑CoV‑2) infection.9,10 The incidence of myocarditis,

although low, has been shown to increase after the receipt of the BNT162b2 vaccine, particularly

after the second dose among young male recipients.11 In addition, the first week after the second

vaccine dose was found to be the main risk window.11 The clinical presentation of myocarditis

after vaccination was usually mild.11

We report the autopsy results including microscopic myocardial findings of two teenage

boys who died within the first week after receiving the second Pfizer-BioNTech COVID-19

dose. The microscopic findings are not the alterations seen with typical myocarditis. This

suggest a role for cytokine storm which may occur with an excessive inflammatory response, as

there also is a feedback loop between catecholamines and cytokines.12

MATERIALS AND METHODS

The Connecticut Office of the Chief Medical Examiner (OCME) and the Michigan

Institute of Forensic Science and Medicine investigate all unexpected and unnatural deaths in

their respective jurisdictions: Connecticut and the Michigan counties of Alcona, Gladwin, Huron,

Lapeer, Ogemaw, and Saginaw.

Standard medicolegal autopsies were performed including gross, microscopic, and

toxicological testing. SARS-COV-2 nasal swab testing was performed by reverse transcriptase-

polymerase chain reaction (RT-PCR) assay. Tissues were sent to the National Center for

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Emerging and Zoonotic Infectious Disease Branch of the Centers for Disease Control and

Prevention (CDC) for molecular studies.

Cardiac molecular testing with sequence analysis and deletion/duplication testing of the

100 genes listed in Invitae's arrhythmia and cardiomyopathy comprehensive panel was

performed.

RESULTS

The results of autopsies for two teenage boys who were found dead in bed 3 and 4 days

after receiving the second dose of the Pfizer-BioNTech COVID-19 vaccine are presented (Table

1). Both boys were pronounced dead at home without attempted resuscitation.

Boy A complained of a headache and gastric upset but felt better by post-vaccine day 3.

There was no history of prior medical problems (he took prescribed

amphetamine/dextroamphetamine during the school year for attention deficit hyperactivity

disorder but was not currently receiving it) or prior SARS-COV-2 infection. Boy B had no

complaints, prior health issues, or prior SARS-COV-2 infection. Neither boy complained of

fever, chest pain, palpitations, or dyspnea. The autopsies were unremarkable except for obesity

in one boy and the cardiac findings (Figures 1-7 and Supplemental Figures 1-4 [Supplemental

digital content can be found at the end of article]). Unique cardiac findings in Boy A included

myocardial fibrosis and in Boy B cardiac hypertrophy. There were no rashes or

lymphadenopathy.

Expanded forensic toxicological testing was negative for medications and drugs of abuse.

SARS-COV-2 was not detected by postmortem swab (RT-PCR assay) in either boy. Cardiac

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sections were submitted from the right and left ventricles (12 sections in Boy A and 29 sections

in Boy B). The cardiac conduction systems were not examined.

DISCUSSION

Myocarditis is an inflammatory disease of the myocardium, which may occur in isolation

or as part of multiorgan/systemic immune-mediated disorders or reactions to exogenous/

endogenous substances.13 The etiologies are varied and include infectious and non-infectious

causes. Non-infectious causes include immune/autoimmune (autoantigens, association with

immune-mediated diseases, alloantigens, and allergens), drugs/toxic substances (e.g.,

hypersensitivity or direct toxic effects), and other causes (e.g., radiation, and insect stings, snake

bites).13 Lymphocytic myocarditis is the commonest histological subtype, characterized by an

inflammatory myocardial infiltrate typically comprising mononuclear cells. In the acute/active

phases, it is usually accompanied by myocyte damage/necrosis.13 Although criteria are evolving,

the Dallas Criteria requires "inflammatory infiltrates of the myocardium with necrosis and/or

degeneration of adjacent myocytes, not typical of ischemic damage associated with coronary

artery disease."14-16

Toxic myocarditis is an etiological classification involving direct myocardial injury by

various drugs or substances.13,17,18 Although variable, the histologic features consist of two main

patterns: an early stage with foci of solely necrotic/damaged myocytes and the later phase of

"myocarditis." Toxic myocarditis usually indicates inflammatory stages of catecholamine-

induced myocardial injury. Catecholamine toxicity on the heart was first described in patients

with pheochromocytoma.19-21 These lesions have been described in patients with subarachnoid

hemorrhages and, more recently, in donor hearts rejected for transplantation in deaths declared

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dead by neurological criteria, secondary to catecholamine-release during the ‘sympathetic storm’

following "brain-death" or administered as pharmacologic support (see supplemental

images).22,23 The wide spectrum of these lesions has been studied in detail in routine pathology

examination of donor hearts unsuitable for transplantation.22

Both teenage boys had similar clinical presentations with no obvious cardiac symptoms.

Their histopathology does not demonstrate a typical myocarditis. In those instances, one sees

lymphocytic (or giant cell) infiltrates with adjacent myocyte necrosis; changes such as

hypereosinophilic myocytes and contraction bands are absent. In these two post-vaccination

instances, there are areas of contraction bands and hypereosinophilic myocytes distinct from the

inflammation. This injury pattern is instead similar to what is seen in the myocardium of patients

who are clinically diagnosed with Takotsubo, toxic, or “stress” cardiomyopathy, which is a

temporary myocardial injury that can develop in patients with extreme physical, chemical, or

sometimes emotional stressors.24-31

Stress cardiomyopathy is a catecholamine-mediated ischemic process seen in high

catecholamine states in the absence of coronary artery disease or spasm.17,31 It has also been

called “neurogenic myocardial injury” and “broken heart syndrome.”18,24-36 Surges in

catecholamines may have several triggers (fight/flight response, adrenal pathology, etc.).

Proposed mechanisms for catecholamine-mediated stunning in stress cardiomyopathy include

epicardial spasm, microvascular dysfunction, hyperdynamic contractility with midventricular or

outflow tract obstruction, and direct effects of catecholamines on cardiomyocytes.33

Catecholamine-mediated myocardial stunning may be due to direct myocyte injury as

elevated catecholamines decrease the viability of myocytes through cyclic adenosine

monophosphate (AMP)–mediated calcium overload. Catecholamines also are a potential source

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of oxygen-derived free radicals which can interfere with sodium and calcium transporters,

possibly resulting in myocyte dysfunction through increased transsarcolemmal calcium influx

and cellular calcium overload.37

Histologically, catecholamine effects have been associated with contraction band necrosis,

characterized by hypercontracted sarcomeres, dense eosinophilic transverse bands, and an

interstitial mononuclear inflammatory response that is distinct from the polymorphonuclear

inflammation seen with infarction. In addition, the mononuclear cells are not causing the

myocyte necrosis; there is a distinct, separate distribution.37

We suspect that the acute cardiac changes seen in these two boys are the result of

epinephrine-mediated effects on cardiomyocytes. These occurrences generally have a favorable

prognosis, however, some patients may die from the underlying (non-cardiac) cause of the

myocardial findings (e.g., such as with subarachnoid hemorrhage). Histologically, diffuse

hypereosinophilic myocytes, contraction bands, and coagulative myocytolysis are seen, with a

patchy and random pattern and a neutrophilic/mononuclear cell infiltrate. With longer survival,

global myocardial ischemia may develop.37

This post-vaccine reaction may represent an overly exuberant immune response and the

myocardial injury is mediated by similar immune mechanisms as described with SARS-COV-2

and multisystem inflammatory syndrome (MIS-C) cytokine storms.38 MIS-C is a rare systemic

illness presenting with persistent fever and extreme inflammation following exposure to SARS-

CoV-2. Affected children have persistent fever and may have acute abdominal pain with

diarrhea or vomiting, muscle pain/malaise, and hypotension. Other reported symptoms include

rashes, enlarged lymph nodes, and swelling.

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A hypersensitivity reaction is in the differential diagnosis, however, infrequency/lack of

eosinophils would be unusual. The common denominator of a hypersensitivity reaction is the

eosinophilic infiltrate, which may be the major inflammatory component or be part of a complex

picture of mixed inflammation with lymphocytes, macrophages, plasma cells, poorly formed

microgranulomas, and giant cells.39 An autopsy study of 69 cases of hypersensitivity

myocarditis examined the spectrum of histologic findings including the distribution of infiltrates

and the extent and composition of the infiltrates.40 They reported that hypersensitivity

myocarditis was "defined by the presence of eosinophils, a mixed lymphohistiocytic infiltrate

along natural planes of separation, and an absence of fibrosis or granulation tissue in areas of

infiltrate."40

Despite a molecular investigation, the etiology of the fibrosis in case A is unclear. It is

conceivable that this process first started with the first vaccination dose and the initial

myocardial effects resolved and healed over time. The second dose may have restarted the

process. One might expect some scarring/repair after a few weeks, although the scarring in Case

A appears more organized than the three-week interval between the vaccine doses. Also, it is

only in one of the cases. It remains possible that the fibrosis represents arrhythmogenic

cardiomyopathy. Unfortunately, cardiac molecular testing was equivocal.

Regardless of the etiology of the fibrosis, the extent of scarring by itself is potentially

arrhythmogenic and may be a contributing factor with the acute post-vaccine myocardial injury.

Similarly, the cardiac hypertrophy in Case B may have made the heart more susceptible to an

arrhythmia. The key point is that since these boys had died suddenly and unexpectedly in their

sleep without resuscitation, if the arrhythmia had been due to the myocardial scar (Boy A) or

cardiomegaly (Boy B), then the fulminant, global myocardial injury would not be an expected

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finding. These two clinical histories support the etiology of the acute myocardial injury as a

primary factor not a secondary agonal or post-resuscitative artefact.

Two adults (ages 42 and 45 years) with "myocarditis" diagnosed histologically (one at

autopsy and one by biopsy) following SARS-COV-2 mRNA vaccinations were recently

reported.41 One occurred 10 days after receiving the first Pfizer-BioNTech COVID-19 vaccine

dose and the other occurred 14 days after receiving the second mRNA-1273 (Moderna) dose.

Histologically, both were described as "fulminant" myocarditis with "multifocal cardiomyocyte

damage associated with mixed inflammatory infiltration." In addition to areas of myocyte

necrosis associated with the inflammatory infiltrate, the photomicrographs demonstrate ischemic

changes distinct from the inflammation similar to our findings.

Cytokine storm has been described with an excessive and uncontrolled inflammatory

response, and there is a feedback loop between catecholamines and cytokines.12 Clinical

complications may include cardiac compromise, respiratory distress, and hypercoagulation.42

The myocardial injury seen in these post-vaccine hearts has a similar histologic appearance as

catecholamine-mediated stress cardiomyopathy and severe SARS-COV-2 infection, including

“myocarditis” which is associated with cytokine release syndrome.38 Recognition that these

instances are different from typical myocarditis and that cytokine storm has a known feedback

loop with catecholamines may help guide screening, diagnosis, and therapy.

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FIGURE LEGENDS

Figure 1: Case A, Heart: Confluent areas of ischemia. Hematoxylin and Eosin stain (H&E),

100X.

Figure 2: Case A, Heart. Coagulative and contraction band necrosis. H&E 200X.

Figure 3: Case A, Heart: Subepicardial fibrosis. This appears older than the timing of the first

vaccine dose. This is a possible arrhythmogenic cardiomyopathy, but its appearance is more

consistent with healed ischemia or inflammation. H&E 40X.

Figure 4: Case A, Heart. Confluent areas of ischemia with contraction bands and coagulative

myocytolysis. 200X.

Figure 5: Case B, Heart: Hypereosinophilic myocytes, contraction band necrosis and coagulative

myocytolysis H&E 100X. Inset: The infiltrate is predominantly neutrophilic. H&E 400X.

Figure 6: Case B, Heart. Subepicardial coagulative myocytolysis/contraction band necrosis.

H&E 100X.

Figures 7: Case B, Heart. Perivascular inflammation. H&E 200X.

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Table 1. Summary of Clinical and Autopsy findings.
Patient Heart Gross Microscopic and Molecular
Teenage Boy A, 280 gms, normal There was global myocardial injury with areas of
BMI=21. History of coagulative myocytolysis and contraction bands,
attention with a perivascular pattern of inflammation
deficit/hyperactivity consisting of predominantly neutrophils with
syndrome. histiocytes, scant lymphocytes, and occasional
eosinophils (Figures 1-4, Supplemental Figures 1-2).
In some sections, the myocardial injury was
predominantly subepicardial, while in other sections
it was patchy and transmural. In the posterior wall,
there was subepicardial/transmural fibrous scar,
without fatty replacement. There were no acute or
organizing thrombi. The overall pattern of injury
was consistent with “stress cardiomyopathy” with
contraction bands and a neutrophilic/histiocytic
infiltrate.
PCR tissue testing performed by the CDC on heart
and lung found no molecular evidence of SARS-
CoV-2 infection.
Molecular testing on postmortem blood detected two
variants of uncertain significance: DOLK
(c.1257C>G (p.Ile419Met) heterozygous) and
MAP2K2 (c.581-3C>T (Intronic) heterozygous).
Teenage Boy B, 520 grams with There was global myocardial injury similar to that
BMI=30 with obesity biventricular seen above, but with more widespread transmural
dilatation and ischemic changes and more interstitial
marked pulmonary inflammation, again with a predominant neutrophil
edema (combined component with histiocytes and scant lymphocytes
lung weight=1481 (Figure 5-7, Supplemental Figures 3-4). Several
grams). sections had transmural, confluent areas of

1
hypereosinophilic myocytes, confluent areas of
contraction bands apart from any inflammation, and
florid neutrophilic inflammation with some
histiocytes. In this case, a subepicardial distribution
of injury was not seen. There were no acute or
organizing thrombi. PCR tissue testing performed
by the CDC on heart and lung found no molecular
evidence of SARS-CoV-2 infection.

Abbreviations: BMI, body mass index; CDC, Centers for Disease Control and Prevention; PCR,
polymerase chain reaction.

2
Supplemental Digital Content. The Supplemental Digital Content was not copyedited by
Archives of Pathology & Laboratory Medicine.

Figure 1: Case A, Heart: Confluent contraction band necrosis/coagulative myocytolysis, with a

predominantly neutrophilic inflammatory infiltrate with histiocytes. Hematoxylin and Eosin stain

(H&E), 100X
Figure 2: Case A, Heart. Interstitial inflammation adjacent to fibrosis. H&E 200X
Figure 3: Case B, Heart. Confluent areas of ischemia with coagulative myocytolysis and
contraction band necrosis. H&E 200X
Figures 4: Case B, Heart. Perivascular inflammation. H&E 200X

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