In December 2019, coronavirus disease 2019 (COVID-19) was first described in Wuhan, China, in patients complaining of flu-like symptoms. The mortality rate of COVID-19 disease, estimated to be <1%, is a result of patients developing severe acute respiratory syndrome (ARDS) and multi-organ dysfunction. A minority of patients develop acute cardiovascular manifestations, including myocardial infarction and myocarditis-like syndrome [1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11]. In this report, a case of a young, healthy Qatari woman who developed COVID-19 myocarditis requiring treatment with venous-arterial extracorporeal membrane oxygenation as a bridge to recovery, is described.
A previously healthy 49-year-old Qatari woman, presented at the Communicable Disease Hospital, Doha, Qatar, with a history of cough and shortness of breath over the preceding week.
She was diagnosed with coronavirus disease 2019 (COVID-19) by real-time reverse transcription-polymerase chain reaction (RT-PCR) test, on the day of admission. Her initial chest x-ray demonstrated bilateral infiltrates (Figure 1a) consistent with COVID-19 pneumonia. Initially, the patient had minimal respiratory symptoms. On the day of admission, after the diagnosis was made, she was prescribed 500 mg azithromycin (Actimycin™, Venus, India) orally once daily, for seven days, two gms ceftriaxone (Rocephin™, Fresenius, Portugal) intravenous once daily, for three days, 400 mg hydroxychloroquine (Paquenil™, Sanofi, India) orally once daily for ten days, and 150 mg oseltamivir (Tamiflue™, Roche, Switzerland) orally twice daily, for five days. This combination of drugs corresponded with the hospital protocol. Also, low molecular weight heparin 40 mg enoxaparin (Clexane™, Sanofi, India) subcutaneous once daily for eight days, was prescribed as a prophylaxis for deep venous thrombosis.
On Day 2, the patient became febrile, tachypneic, and had oxygen desaturation despite the escalation in non-invasive ventilation; arterial blood gas sample was consistent with Type 1 respiratory failure showing a low PaO2/FiO2 ratio (Table 1). Repeat chest X rays demonstrated a worsening of the bilateral lung infiltrates (Figure 1b). A diagnosis of acute respiratory distress syndrome (ARDS) was made, and the patient was transferred to the hospital’s intensive care unit for further management.
Laboratory parameters of the patient throughout hospitalization
Reference | Arrival | Day 2 - Intubation | D5 | D8 | D9 - VA ECMO | D11 | D12 | D14 -VV ECMO | DECMO 16 - decannulation | Discharge | |
---|---|---|---|---|---|---|---|---|---|---|---|
WBC | 4-103 u/L | 7.8 | 11.2 | 14.9 | 33.3 | 32.2 | 26 | 33 | 10 | ||
Absolute Lymphocytes | 1-33 u/L | 0.7 | 0.4 | 0.7 | |||||||
CRP | 0-5 mg/L | 193 | 428 | 23 | 20 | 11 | 8 | 5 | 4 | ||
Procalcitonin | <0.5 ng/mL | 1.38 | 7.14 | 6.27 | 2.89 | 0.94 | 0.25 | ||||
Pro-BNP | <125 pg/mL | 430 | 34.198 | 4.403 | 1.132 | ||||||
Troponin T | 3-10 ng/L | 9 | 146 | 112 | 1.076 | 1.401 | 75 | ||||
Myoglobin | 25-58 ng/mL | 331 | |||||||||
Ferritin | 18-340 ug/L | 628 | 928 | 4.689 | 1,633 | 1.959 | 1.339 | 576 | 457 | 303 | |
LDH | 135-214 U/L | 548 | 835 | 1.239 | 980 | 948 | 1,011 | >1000 | 1249 | ||
AST/ALT | <33 U/L | 23/12 | 35/15 | 49/27 | 251/114 | 118/95 | 82/97 | 70/74 | 131/90 | 137/138 | 23/32 |
Triglycerides | < 1.7 mmol/L | 1.4 | 2.7 | 3.1 | 1.8 | 1.1 | 1.4 | 2 | 1.8 | ||
FiO2 (%) | 50% | 50% | 45% | 50% | 30% | 40% | |||||
PaO2 (mmHg) | 79 | 77 | 56 | 61 | 90 | 123 | |||||
PH | 7.35 to 7.45 | 7.37 | 7.56 | 7.47 | 7.36 | 7.43 | 7.42 | ||||
Lactate | 0.5-2.2 mmol/L | 1.4 | 2.6 | 3.4 | 5.6 | 1.6 | 0.8 |
VA -Venous Arterial; ECMO - Extracorporeal membrane oxygenation; VV - Venous Venous
In the ICU, the patient was intubated. On Day 3, her antibiotic regime was increased to include to 4 grams piperacillin intravenous every six hours for seven days, in combination with 0.5 g tazobactam intravenous every six hours for seven days (Tazocin™, Wyeth, Italy). Also, initially, intravenously 600 mg teicoplanin (Targocid™, Sanofi, Italy) was prescribed twice daily for two days after which the dose was reduced to 400 mg intravenously once daily for eight days to cover for hospital-acquired bacterial infections.
Given the concern that a cytokine storm was the possible the aetiology underlying the patient deterioration, on Day 3, 40 mg intravenous methylprednisolone (Depo-medrol™, Pfizer, Belgium), was administered twice daily for twelve days, together with 400 mg intravenous tocilizumab (Actemra™, Roche, Switzerland).
On Day 3, she also received 400 mg lopinavir with 100 mg ritonavir (Lopinavir / Ritonavir™, Mylan, India) orally twice daily for five days. These were given in addition to the continuation of hydroxychloroquine, oseltamivir, and azithromycin.
Later, on Day 3 of hospitalization, the patient was moved to the prone position to improve her oxygenation. Initial transthoracic echocardiography, on Day 5, demonstrated preservation of left ventricular ejection fraction of 58% with no regional wall motion abnormalities. The patient was maintained on minute-ventilation with a PEEP of 10 and FiO2 of 40%, to keep her blood oxygen saturation within the acceptable range.
The patient clinical condition gradually improved with decreasing ventilator support. Blood analyses showed a reduction in inflammatory markers with a drop in C-reactive protein from 428 to 23 mg/L until Day 7. On Day 7 she had a fever spike, her temperature recorded as 38.9 °C, and she became hypotensive requiring initiation of vasopressors, norepinephrine (Veraline™, Verve, India) 0.1 mcg/kg/min as a continuous intravenous infusion. Peak high sensitivity Troponin T levels of 1,401 ng/L and Pro- BNP at 34,198 pg/mL were recorded, indicative of myocardial injury (Figure 2).
A follow-up transthoracic echocardiogram on Day 8 showed a significant reduction in the left ventricular ejection fraction to 25% with diffusely hypokinetic walls and a reduction in right ventricular function. The patient’s inflammatory markers were significantly elevated (Table 1).
Given the presence of severe biventricular dysfunction on transthoracic echocardiogram, low cardiac output at 2.5 L/min measured by pulse contour cardiac output PiCCO (Pulsion Medical Systems, Munich, Germany), elevated central venous pressure of 24 mmHg, and low central venous saturation of 50% measured from the right internal jugular central line, a diagnosis of cardiogenic shock secondary to severe myocarditis was made. Severe myocarditis was thought to be secondary to the cytokine storm syndrome. Therefore, it was decided to administer a second dose of tocilizumab in addition to intravenous immunoglobulin and an additional course of pulse steroid therapy.
Organ hypoperfusion and shock physiology were refractory to the pharmacological therapy, Norepinephrine, Dobutamine, and Vasopressin, which were first prescribed on Days 7, 8 and 9 respectively. On Day 9, the patient was started on veno-arterial extra-corporeal membrane oxygenation (VA-ECMO) and continuous venous-venous haemodiafiltration using CytoSorb (
On Day 10, a sub-segmental pulmonary embolism was confirmed by computed tomography, (Figure 3) and treated with a continuous intravenous infusion of heparin at 1040 unit/ per hour (16 unit/kg/hr).
On Day 14, the patient’s arterial ECMO access was de-cannulated, and she was converted to venous-venous ECMO to provide respiratory support only.
A follow-up transthoracic echocardiogram showed a left ventricular ejection fraction of 26% with an improvement of cardiac output. The patient’s blood lactate levels normalized, and she was weaned of inotropic support. She was de-cannulated from VV ECMO on Day 16 and was successfully extubated on Day 23.
The patient’s condition improved gradually, off oxygen, and a repeat transthoracic echocardiogram at 60 days showed improved cardiac function with a left ventricular ejection fraction of 50%.
At the time of reporting this case, she was actively undergoing rehabilitation for critical illness-induced myopathy.
A case of COVID-19 infection resulting in severe ARDS followed by myocarditis with ensuing cardiogenic shock managed with VA ECMO support is reported. At the time of writing this case, a survey of the literature indicated that this is the first COVID-19 myocarditis reported from the Middle East and 12th reported patient worldwide (Table 2). The first reported patient with COVID-19 myocarditis was from China [2]. Since then, ten more cases [3, 4, 5, 6, 7, 8, 9, 10, 11, ,15,16] were reported worldwide. The age range of the patients was two to sixty-nine years. The patient's symptoms varied from being asymptomatic to presenting with typical angina symptoms and shock. The reported ECGs, at presentation, were also variable with changes consistent of T-elevation myocardial infarction. Few of the patients had undergone a coronary evaluation to exclude obstructive coronary artery disease. The diagnosis of myocarditis in most of the cases was based on clinical grounds. Cardiovascular magnetic resonance imaging (CMR) was used in some cases to confirm the diagnosis, and three patients underwent myocardial biopsies [6,11,15,16]. Sala et al. (2020) [6] reported a forty-three year old Italian woman who presented with a three-day history of oppressive chest pain and dyspnoea; her past medical history was unremarkable. An electrocardiogram (ECG) showed an ST-segment elevation in leads V1-2 and a VR with reciprocal ST depression. There was a reduction in myocardial function as seen on the transthoracic echocardiogram with an elevation of myocardial enzymes. Cardiovascular magnetic resonance imaging showed features consistent with Takotsubo cardiomyopathy and a myocardial biopsy demonstrated diffuse T-lymphocytic inflammatory infiltrates with interstitial oedema and limited foci of necrosis. There was an absence of the SARS-CoV-2 genome within the myocardium. Ruihai Zhou (2020) [12] argued that the patient might have had Takotsubo cardiomyopathy rather than myocarditis because of the lack of evidence of myocardial viral genome and the shared CMR features with Takotsubo cardiomyopathy.
Reported studies of COVID-19 and Myocarditis
Author | Country | Age/ Gender | Cardiac Symptoms | ECG | EF (%) | Myocarditis Means of diagnosis | Troponin level | NT-BNP | IL-6 Level | Treatment * | ECMO | Outcome | |
---|---|---|---|---|---|---|---|---|---|---|---|---|---|
Zeng [2] | China | 63/M | Chest tightness | Sinus tachycar dia, no STE | 32% | Clinical echo and | 11.37 g/L | 22,600 | 272.4 | 1,2,6,7( | DayYes 11) | days Died later 33 | |
Hongde Hu [7] | China | 37/M | Chest dyspnea pain, | STE (III,aVF) | 27% | Clinical echo and | >10,000 ng/L | 21,025 | 1,2 | No | Survived | ||
Inciardi RM [5] | Italy | 53/W | No symptoms cardiac | Diffuse STE | 35% | Clinical, MRI Echo, | 0.89 ng/mL | 8465 ng/L | No | Survived | |||
Sala S [6] | Italy | 43/W | Chest dyspnea pain, | Mild STE (V1-2, aVR), cal ST reciprodepres- sion V4-6 | 43 | Clinical, MRI, biopsy Echo, | 135-107-106 ng/L | 7,9 | No | Survived | |||
Justin Coyle [4] | USA | 57/M | Dyspnea | ST only | 40% | Clinical, MRI Echo, | 7.33 ng/L | 1300 mL P g/ | 1,3,5 | No | Survived | ||
Angela Irabien- Ortiz [10] | Spain | 59/W | Angina | PR depression, Concave upwards STE | depressed | Clinical, echo | 110 ng/L | 4421 ng/L | 1,6,7 | Yes | Survived | ||
Dayen [8] | France | (69Italian) /M | No symptoms cardiac | LVH depression and ST | Normal LVH and EF | Clinical, MRI | 9002 ng/L | 1 | No | Survived | |||
Massi- miliano Gnecchi [9] | Italy | 16/M | Chest pain with radiation to the left arm | Inferolateral STE | 54%, inferolateral hypokinesia | Clinical, Echo, MRI | 14,810 ng/L | Intravenous ibuprofen | No | Survived | |||
Kesci [11] | Turkey | 2/M | Biopsy | Yes | |||||||||
Guido Tavazzi [15] | Italy | 69/M | No cardiac symptoms | 25% Global | Biopsy, ECHO, Normal CAG | 4332 ng/L | Yes | Died 12 days later | |||||
Quentin Fischer [16] | France | 15/M | chest pain | diffuse STE | 50%, Glob- al, Mild effusion | MRI | 13.1 μg/L | 65 ng/L | Beta blocker ACE I | No | Survived | ||
Current report | Qatar | 49/W | No cardiac symptoms | T inversion on lateral leads | 25%, Global | Clinical, Echo | 1401 ng/L | 34198 pg/ mL | 1,2,3, 7,9 | Yes (day 9) | Survived |
More recently, Kesci et al. (2020) reported COVID-19 RT-PCR positivity in the cardiac tissue of a two-year old Turkish boy with COVID-19 myocarditis; the patient also required ECMO mechanical support for management [11].
The localization of viral particles in cardiac tissue of a patient with COVID-19 cardiogenic shock was subsequently reported by Tavazzi et al. (2020), who stated that they were mainly present in cytopathic and structurally damaged interstitial cells [15].
In our case, the presence of global hypokinesia with the absence of typical echocardiographic characteristics, ECG features of Takotsubo cardiomyopathy, the sudden onset of cardiogenic shock and the significant rise in cardiac markers, supported the diagnosis of acute myocarditis.
The exact mechanism of cardiac involvement in COVID-19 remains under investigation [17]. One potential mechanism is direct myocardial involvement mediated by angiotensin-converting enzyme ACE2. Other suggested mechanisms of COVID-19–related cardiac involvement include a cytokine storm, mediated by an imbalanced response among subtypes of T helper cells, and hypoxia-induced excessive intracellular calcium leading to cardiac myocyte apoptosis [13]. Our patient suffered from an acute pulmonary embolism, in the absence of obvious secondary cause, which we think is linked to the hypercoagulable state related to COVID-19.
At the time of writing this case, the only therapy that had shown improved survival in severe intubated COVID-19 patients was systemic steroids [14]. The role of intervention with mechanical circulatory support in COVID-19 cases is also unclear.
In the present case, the medical team deemed that the patient would not survive without mechanical circulatory support due to her continuing deteriorate, despite escalating doses of inotropes and vasopressors. Given that both lung and cardiac function were deteriorating, VA ECMO was the preferred choice of mechanical circulatory support.
The use of ECMO has been reported in four COVID-19 patients [2, 10, 11, 15], two of them died from secondary infections [2, 15], and the other two patients recovered [10, 11]. Although the clinical outcome of patients with COVID-19 myocarditis is unknown, it should be noted that only two out of eleven reported patients died due to secondary infections.
Myocarditis is a rare complication of COVID-19 infection that may result in cardiogenic shock and death. In severe cases, initiation of mechanical circulatory support might be vital as a bridge to complete recovery.