First Identified Case of Fatal Fulminant Necrotizing Eosinophilic Myocarditis Following the Initial Dose of the Pfizer-BioNTech mRNA COVID-19 Vaccine (BNT162b2, Comirnaty): an Extremely Rare Idiosyncratic Hypersensitivity Reaction.

RATIONALE: Transient myopericarditis has been recognised as an uncommon and usually mild adverse event predominantly linked to mRNA-based COVID-19 vaccines. These have mostly occurred in young males after the second dose of mRNA COVID-19 vaccines.
OBJECTIVES: Fulminant necrotising eosinophilic myocarditis triggered by a variety of drugs or vaccines is an extremely rare hypersensitivity reaction carrying a substantial mortality risk. Early recognition of this medical emergency may facilitate urgent hospital admission for investigation and treatment. Timely intervention can lead to complete cardiac recovery, but the non-specific clinical features and rarity make early diagnosis challenging.
FINDINGS: The clinical and pathological observations from a case of fatal fulminant necrotising myocarditis in a 57-year-old woman, following the first dose of the Pfizer-BioNTech vaccine, are described. Other causes have been discounted with reasonable certainty.
CONCLUSION: These extremely rare vaccine-related adverse events are much less common than the risk of myocarditis and other lethal complications from COVID-19 infection. The benefits of vaccination far exceed the risks of COVID-19 infection.

Introduction

SARS-CoV-2, the agent responsible for COVID-19, has had a calamitous effect on the world. Recently, several COVID-19 vaccines have received emergency use authorisation. The Pfizer-BioNTech vaccine has now received full FDA approval for individuals over 12 years of age.

COVID-19 vaccines have been well tolerated apart from the expected local reactions at the injection site and mild transient constitutional symptoms, typical of vaccine systemic immune responses. Post-marketing surveillance has identified rare serious adverse events including vaccine-induced thrombosis and thrombocytopenia (VITT) with some adenovirus vaccines including the Astra-Zeneca (ChAdOx1-S) vaccine [1]. In addition to a small risk of VITT, the Janssen/Johnson and Johnson (Ad26.COV2.S) vaccine has also been associated with Guillain–Barre syndrome.

A small risk of anaphylaxis and mild transient myopericarditis, mostly in young males, has been observed predominantly with mRNA vaccines [2, 3]. Life-threatening fulminant necrotising eosinophilic myocarditis, an extremely rare idiosyncratic reaction, has been described with drugs and other vaccines. [4] The clinical features and immunopathology of a case of fatal fulminant necrotizing eosinophilic myocarditis, following the first dose of the Pfizer-BioNTech COVID-19 vaccine, are described in this report. This rarer, much more severe hypersensitivity reaction is fundamentally different from the mild self-limited myopericarditis seen usually after the second dose of mRNA COVID-19 vaccines [2, 5]. These exceptionally rare events must be seen in the context of COVID-19 infection, which carries a far higher risk of myocarditis and other potentially lethal complications. [6]

Case Description

A previously well 57-year-old woman received the first Pfizer-BioNTech vaccine in July 2021. The following day she experienced increasing lethargy and had to leave work early because of worsening fatigue. She had one episode of breathlessness and complained of a stiff neck as well as upper limb pain. She had a sore throat but pointed to her sternum. During the remainder of the day, she became increasingly unwell. The following day she consulted her primary care physician with a sore throat, back pain, fatigue and an episode of haematuria, which had occurred the previous night. She had difficulty getting out of the car and experienced a fall at the family physician’s surgery. She did not complain of palpitations.

On day 2, a complete blood count (CBC) was normal but she was noted to have an increased C-reactive protein (CRP) (Table 1). She had a raised ferritin and alanine transaminase (ALT) but the aspartate aminotransferase (AST) was not undertaken, although the other liver enzymes were normal. There was no eosinophilia. On the third day, she was diagnosed with an Escherichia coli urinary tract infection, which was treated with trimethoprim. During that night, she was found deceased in bed. Apart from long-term omeprazole and the recently commenced trimethoprim, she was on no other treatment. There was no history of autoimmunity or allergic disease.

Table 1

Day 2 ante-mortem blood results. ALT alanine transaminase, CRP C-reactive protein, GGT gamma glutamyl transferase

	Result	Reference interval
Haemoglobin (g/L)	126	115–155
Neutrophils 10(9)/L	6.7	1.9–7.5
Platelets 10(9)/L	239	150–400
Lymphocytes 10(9)/L	1.2	1–4
Monocytes 10(9)/L	0.6	0.2–1
Eosinophils 10(9)/L	0.1	< 0.6
Basophils 10(9)/L	0	< 0.2
CRP mg/L	42	< 5
Total bilirubin (µmol/L)	14	< 25
Alkaline phosphatase (U/L)	89	40–120
GGT (U/L)	49	< 50
ALT (U/L)	397	< 45
Albumin (g/L)	30	32–48
Globulin (g/L)	23	25–41
Total protein (g/L)	53	66–84
Ferritin (µg/L)	846	20–380

Autopsy Findings

The body was that of a small-built adult female of Chinese descent, consistent with the stated age of 57 years (height 155 cm; weight 40 kg). External examination was unremarkable. On internal examination, the most striking finding was a tan, solid lobulated mass originating from the mediastinum and situated in the left pleural cavity (Fig. 1, top left and top right). This mass was 130 × 120 × 90 mm and weighed 710 g. Mild splenomegaly (240 g) was noted. There was no pericardial effusion and there was no intracardiac thrombosis. The remainder of the autopsy examination was unremarkable. There were no abnormalities of other organs.

Fig. 1

Top left: Left pleural mass originating from the mediastinum. Top right: Cut section of thymoma. Bottom left: × 20 magnification showing multifocal inflammatory cell infiltration in the myocardium; asterisk (*) showing areas of eosinophil-rich inflammatory aggregates with myococyte necrosis. Bottom right: × 40 magnification showing an abundant eosinophilic infiltrate with myocyte necrosis. Arrow shows an eosinophil, asterisk (*) showing myocyte necrosis

Histology and Ancillary Tests

Histological examination of the heart sections showed fulminant necrotizing eosinophilic myocarditis (Fig. 1, bottom left and bottom right). There were multifocal aggregates of lymphoid cells, histiocytes and abundant eosinophils with focal myocyte necrosis in the free walls of both ventricles, inter-ventricular septum and around the conduction system (sino-atrial and atrio-ventricular nodes). No parasitic organisms or giant cells were identified. The eosinophilic infiltrate would make autoimmune myocarditis less likely. There was no evidence of eosinophils in other organs or eosinophilic vasculitis. Histological examination of the left pleural space mass showed a thymoma, WHO subtype AB.

There was a limited amount of post mortem serum for diagnostic studies. Antibodies to SARS-CoV-2 were negative on histological paraffin blocks and she had a mild reduction in IgG 4.54 (7–14 g/L), IgA 0.72 (0.8–4.0 g/L) and IgM 0.26 (0.4–2.5 g/L) levels, post mortem. T cell receptor excision circle numbers from peripheral blood DNA were normal, as was a tryptase level. She had a borderline parvovirus PCR test from the myocardium, below quantifiable levels. Other viral PCR tests including enterovirus, metapneumovirus, parainfluenza (1–4), rhinovirus, adenovirus, respiratory syncytial virus, SARS-CoV-2, parechovirus and influenza A and B were negative. A toxicology screen was negative. Complement studies and cytokine studies were not undertaken as there was no ante-mortem blood available.

Discussion

Fulminant necrotizing eosinophilic myocarditis is an extremely rare hypersensitivity syndrome caused by a variety of drugs and vaccines [4]. This life-threatening idiosyncratic reaction specifically targets the myocardium. The cardiac injury is likely to be mediated by the highly toxic contents of granules including eosinophilic cationic protein, eosinophil major basic protein, eosinophil peroxidase and eosinophil-derived neurotoxin. In mice, eosinophil-derived IL4 plays a critical role in cardiac damage. [7]

The immunopathology of this extremely rare disorder remains to be defined but is likely to be mediated by cytotoxic T cells producing IL5. In the future, staining for IL5-producing T cells may be helpful in confirming this hypothesis. It is also possible these T cells have specific homing receptors for the heart. Single-cell RNA profiling may also help identify such cells but was not possible in this case because of post mortem RNA degradation. Cardiac myocytes express ACE2 receptors, which could bind the spike glycoprotein, translated from the mRNA vaccine. A specific ACE2-induced hypersensitivity reaction would not explain the pathogenesis of this disorder, given it can be triggered by other drugs and vaccines. In contrast to most other immune-mediated hypersensitivity disorders, a priming exposure may not be required since fulminant necrotising eosinophilic myocarditis can occur after the first exposure to a drug or vaccine. [4]

There was no family history of premature cardiac disease. Other first-degree family members have tolerated the Pfizer-BioNTech vaccine without any significant adverse events. This would make a genetic drug hypersensitivity disorder to the Pfizer-BioNTech vaccine less likely.

It is very unlikely the trimethoprim, begun a few hours before death, was responsible for the disorder as the patient was already acutely unwell for over 48 h prior to commencing treatment. Trimethoprim has not been associated with fulminant eosinophilic myocarditis. Given the benign CBC and modestly elevated CRP, it is unlikely sepsis that caused cardiovascular collapse. The urine infection contributed to the diagnostic confusion but is also unlikely to have been a factor in the fulminant necrotizing eosinophilic myocarditis. The elevated ALT, ferritin and splenomegaly and reduced protein parameters were likely part of the acute inflammatory reaction. The brief haematuria is likely to have been a result of the UTI. The borderline parvovirus PCR is unlikely to be of significance as no giant cells or inclusion bodies were noted at autopsy. Only a high copy number (> 500) in myocardial tissues are considered causal. [8] COVID-19 serology and RT-qPCR tests from the myocardium were negative. NZ had been completely free from COVID-19 for many months at the time of her death.

The patient was noted to have an incidental thymoma at autopsy. Myocarditis has been described in patients suffering from WHO type B thymomas [9]. Ryanodine receptor antibodies may have a pathogenic role in such patients. [10] These patients however have lymphocytic or giant cell myocarditis, not seen in this case. It was also unlikely this patient had Good’s syndrome (thymoma associated with immunodeficiency). In contrast to this patient, the great majority of patients with Good’s syndrome are symptomatic, with recurrent infections or autoimmunity [11]. Most patients with Good’s syndrome have markedly reduced immunoglobulin levels [12]. The mild reduction in the post mortem IgG, IgA and IgM is likely to be an artefact [13]. In contrast to this patient, the majority of patients with Good’s syndrome have haematological abnormalities (Table 1). [14] Furthermore, the presence of a severe T cell defect in Good’s syndrome would have made an eosinophilic hypersensitivity response less likely, as IL5 plays a critical role in eosinophil biology.

Globally, there are rare case reports of possible fulminant myocarditis, including fatalities, following mRNA vaccines, attesting to the extreme rarity of these reactions [15, 16]. Histological features showed an inflammatory infiltrate composed of T cells and macrophages, eosinophils, B cells and plasma cells. These cases were however not identified as fulminant necrotising eosinophilic myocarditis. The clinical and immunological differences between milder cases and fulminant cases were not explored in detail (Table 2).

Table 2

Comparing the two types of myocarditis associated with mRNA vaccines and risk of myocarditis with COVID-19. Because of the infrequency of endomyocardial biopsy, the histology of the transient myopericarditis is poorly characterised. *From published cases, the risk of fulminant necrotising eosinophilic myocarditis is likely to be considerably lower than 1:10 [8] vaccine doses. Global vaccination data from Bloomberg. **A recent community-based study estimated the risk of COVID-19-induced myocarditis is 110/10 [6] infections over and above those caused by vaccines. [3] The risk of myocarditis from COVID-19 infection far exceeds the risks from vaccines. Furthermore, many COVID-19 survivors experience long-term myocardial dysfunction [17]. MRI magnetic resonance imaging

Demographics and clinical features	Transient myopericarditis following mRNA vaccines	Fulminant necrotising eosinophilic myocarditis	Myocarditis associated with COVID-19 infection
Age group	Younger	May be older	Any age
Gender	Predominantly males	Males or females	Males or females
Frequency/million doses [18] Males < 30 years Males > 30 years Females < 30 years Females > 30 years	40.6 2.4 4.2 1.0	*1 reported case (and possibly 2 others) from over 6.75 billion vaccine doses	**110/million COVID-19 infections (in excess of that from vaccines) [3]
Specificity for COVID-19 vaccine	Relatively specific for mRNA COVID-19 vaccines	Can also occur with other vaccines and drugs	NA
Dose	Usually second dose (unless primed by previous SARS-CoV-2 infection) [19]	May be first dose	NA
Symptoms	Chest pain [20]	May be non-specific	May be non-specific
EKG	Abnormal	Abnormal	Abnormal
Echocardiography	Abnormal	Abnormal	Abnormal
Troponins	Elevated	Elevated	Elevated
Cardiac MRI	Abnormal	Abnormal	Abnormal
Pathology	Myocarditis and pericarditis	Myocarditis	Myocarditis
Histology	Lymphocyte, macrophages [21]	Eosinophilic infiltrates with myocyte necrosis	Lymphocytic infiltrates
Treatment	Conservative	Immunosuppression, IL5 inhibitors	Dexamethasone for severe COVID-19
Prognosis	Excellent	Poor without treatment	Prognosis dependent on age, comorbidities

Milder cases have occurred mostly in adolescent males usually after the second dose of an mRNA vaccine and have resolved spontaneously [22, 23]. Transient myopericarditis has less commonly occurred after the first dose, often in patients who have previously suffered COVID-19 infection, indicating the need for immunological priming [19, 21]. Although rarely biopsied, it appears these patients have lymphocyte predominant myocarditis [21]. Deaths are exceptionally rare and the histology is distinct from fulminant necrotising eosinophilic myocarditis [24]. Although less frequently described with the Janssen/Johnson and Johnson vaccine, these milder cases appear to be a specific hypersensitivity reaction to mRNA COVID-19 vaccines (Table 2). [25].

Fulminant necrotizing eosinophilic myocarditis progresses in three clinical stages. Many cases are fatal in the acute stage. A review of fulminant necrotizing eosinophilic myocarditis showed cardiac arrest in almost one-half of patients and high in-hospital mortality with rates of 36.1%. [4] In addition to systemic steroids, many patients have required mechanical cardiac assistance in the acute phase. Early diagnosis and treatment with systemic steroids has however resulted in complete cardiac recovery in the majority of individuals. [4]

Untreated survivors may progress to a second clinical stage where there is increased risk of cardiac thromboembolic events. A third clinical stage comprises endomyocardial fibrosis leading to a chronic restrictive cardiomyopathy.

In up to 25% of fulminant necrotizing eosinophilic myocarditis cases, there is no eosinophilia in the blood or in other organs. [4] This distinguishes the condition from other causes of eosinophilic myocarditis such as Loeffler’s syndrome or eosinophilic granulomatosis and polyangiitis (EGPA). There was no evidence of eosinophilic vasculitis at autopsy.

Diagnosing fulminant necrotising eosinophilic myocarditis is challenging given its rarity and non-specific presentation. Most patients experiencing mild constitutional symptoms following COVID-19 vaccines improve by 48 h. If patients become progressively unwell beyond this time, following the Pfizer-BioNTech vaccine, they should be carefully reviewed for vaccine complications as well as other co-incidental disorders. Severe chest pain may be less common in cases of fulminant necrotising eosinophilic myocarditis compared to the transient myopericarditis occurring in young males (Table 2) [4, 19]. The characteristic chest pain in younger males may reflect high rates of concomitant pericarditis. [20].

In cases of fulminant necrotising eosinophilic myocarditis, there may be electrocardiographic changes and an increase in troponin levels and echocardiography studies may show systolic and diastolic myocardial dysfunction [4]. Cardiac magnetic resonance imaging may show late gadolinium enhancement but this is not specific for fulminant necrotizing eosinophilic myocarditis. A diagnosis of fulminant necrotizing eosinophilic myocarditis requires an endomyocardial biopsy, acknowledging the disease process may be uneven. [4]

Early admission to an intensive care or coronary care unit may facilitate diagnosis and treatment. If there are delays in obtaining an endomyocardial biopsy, or if negative despite high clinical suspicion, consideration should be given to pulse intravenous methylprednisolone treatment as well as mechanical cardiac assistance, if required. Apart from high-dose systemic corticosteroids, IL5 inhibitors such mepolizumab may have an important therapeutic role in treating fulminant necrotising eosinophilic myocarditis. [26].

It seems probable the Pfizer-BioNTech vaccine was responsible for the fatal fulminant necrotizing myocarditis in this case. The temporal association is compatible with such a hypersensitivity reaction, other causes have been excluded, and the histomorphology is consistent with the diagnosis. These are extremely rare adverse events and the benefits of COVID-19 vaccination far exceed the risks of COVID-19 infection [18]. COVID-19 infection carries a much higher rate of acute and chronic cardiovascular sequelae including myocarditis, arrhythmias and myocardial infarction and thromboembolic events (Table 2), which can be mitigated by COVID-19 vaccination. [3, 6, 17].