Cardiac imaging phenotype in patients with coronavirus disease 2019 (COVID-19): results of the cocarde study.

Biological cardiac injury related to the Severe Acute Respiratory Syndrome Coronavirus-2 infection has been associated with excess mortality. However, its functional impact remains unknown. The aim of our study was to explore the impact of biological cardiac injury on myocardial functions in patients with COVID-19. 31 patients with confirmed COVID-19 (CoV+) and 16 controls (CoV-) were prospectively included in this observational study. Demographic data, laboratory findings, comorbidities, treatments and myocardial function assessed by transthoracic echocardiography were collected and analysed in CoV+ with (TnT+) and without (TnT-) elevation of troponin T levels and compared with CoV-. Among CoV+, 13 (42%) exhibited myocardial injury. CoV+/TnT + patients were older, had lower diastolic arterial pressure and were more likely to have hypertension and chronic renal failure compared with CoV+/TnT-. The control group was comparable except for an absence of biological inflammatory syndrome. Left ventricular ejection fraction and global longitudinal strain were not different among the three groups. There was a trend of decreased myocardial work and increased peak systolic tricuspid annular velocity between the CoV- and CoV + patients, which became significant when comparing CoV- and CoV+/TnT+ (2167 ± 359 vs. 1774 ± 521%/mmHg, P = 0.047 and 14 ± 3 vs. 16 ± 3 cm/s, P = 0.037, respectively). There was a decrease of global work efficiency from CoV- (96 ± 2%) to CoV+/TnT- (94 ± 4%) and then CoV+/TnT+ (93 ± 3%, P = 0.042). In conclusion, biological myocardial injury in COVID 19 has low functional impact on left ventricular systolic function.

Introduction

The pathophysiology of the Severe Acute Respiratory Syndrome Coronavirus-2 (SARS-CoV-2) infection is still poorly understood. Although lung involvement has all the usual characteristics of a severe acute respiratory syndrome, the natural history of infection goes beyond the simple respiratory failure. The intense systemic inflammatory stimuli that occurs after the viral replication phase is a major contributor to the systemic effects of the disease [1] and their consequences in terms of morbidity and mortality.

Myocardial injury, manifested by an increase in troponin, has been reported in 8 to 20% of infected patients [2-4], reaching 31% in the most severe patients [2, 5], and is associated with excess mortality [4, 5]. Although myocardial injury has been linked to the severity of inflammation [5], the exact mechanism of the myocardial injury that may accompany the infection remains unknown. Many arguments suggest a type 2 myocardial infarction via an oxygen supply/demand imbalance mechanism alone attributable to the cytokine storm. Alternatively, cardiovascular risk factors such as diabetes and hypertension, as well as coronary or cerebral cardiovascular history, have been associated with severe forms of infection [6-8]. Consequently, cytokine storm could lead to atherosclerotic plaque instability and rupture [9] (i.e. type 1 myocardial infraction). On the other hand, the supposed affinity of the virus for the myocardial angiotensin-converting enzyme 2 receptors [10] could lead to direct inflammation of the myocardium as suggested by several articles reporting acute/fulminant myocarditis [11-13].

However, to date, although there is a link between increased troponin and myocardial dysfunction through the increase in natriuretic peptides [5], the real segmental and global functional impact of the infection on the myocardium remains unknown. Complete cardiac data on infected patients, such as electrocardiography, echocardiography, coronary angiography and magnetic resonance imaging are missing [9].

The objective of this study was to perform cardiac imaging phenotype of Coronavirus Disease 19 (COVID-19) infected patients to assess the impact of the infection on myocardial work and function.

Methods

Study participants

Patients admitted to Rangueil Hospital of Toulouse University for dyspnea or chest pain with suspected COVID-19 disease were included in this prospective cohort study from April 6, 2020, to May 1, 2020. Data were collected in consecutive patients referred to either the medical unit or the intensive care unit for COVID-19. All patients underwent collection specimens from the upper respiratory tract by real-time reverse transcriptase–polymerase chain reaction (RT-PCR) testing for the SARS-COV-2, chest computed tomography (CT), cardiac biomarkers, including high-sensitivity troponin T (hs-TnT) and NT-proBNP, electrocardiography and transthoracic echocardiography (TTE) at admission, as part of the standard of care. Diagnosis of COVID-19 was retained in the presence of an evocative chest CT and a positive RT-PCR for COVID-19 or an evocative chest CT in the presence of a negative RT-PCR for COVID-19 after ruling out other common respiratory viral and bacterial infections [14]. Biological cardiac injury was defined as blood levels of hs-TnT above the 99th -percentile upper reference limit, regardless of new abnormalities in electrocardiography and TTE. Patients were then categorized into 3 groups based on the presence of COVID-19 infection and/or biological cardiac injury: patients without COVID-19 infection and without biological cardiac injury (CoV−), patients with COVID-19 infection without biological cardiac injury (CoV+/TnT− and patients with COVID-19 infection with biological cardiac injury (CoV+/TnT+).

Patients with history of heart disease and atrial fibrillation were excluded from the study.

The vital status of the patients was collected 3 months after discharge from the hospital by a phone call.

The study has been notified to national ethics committees as appropriate (protocol number ID-RCB: 2020-A00852-37, positive endorsement of the protection of persons committee West IV dated April 8, 2020) and to the French Data Protection Agency. The study has been registered with Clinicaltrials.gov NCT04358952. The investigation conforms to the principles outlined in the Declaration of Helsinki. All patients or their beneficiaries were informed of the study and gave their consent.

Data collection

The demographic characteristics (age and sex), clinical data (symptoms, comorbidities, treatments) and laboratory findings for patients during hospitalization were collected from electronic medical records and entered into the database by 2 investigators. Cardiovascular risk factors included hypertension, diabetes, hypercholesterolemia, previous or current smoking and obesity (defined by a body mass index ≥ 30 kg/m²). Arterial blood pressure was measured and collected at the time of TTE. Electrocardiography and TTE were performed by 3 investigators and analyzed by 2 independent investigators blinded to the clinical characteristics of the patients.

Transthoracic echocardiography

Transthoracic echocardiography was performed with either a Vivid E95 or Vivid S70 ultrasound system (GE Healthcare) using a 3.5 MHz transducer, allowing archiving acquisitions for a deferred analysis. Doppler, M-mode and two-dimensional gray scale echocardiography including the three standard apical views (four-, three- and two-chambers) using high frame rates (> 60 frames/s), pulsed-Doppler transmitral inflow and left ventricular outflow and pulsed-Doppler tissue imaging lateral mitral and tricuspid annular velocities were performed for each patient with simultaneous arterial blood pressure recording.

Images analysis

Image analysis was performed offline using the offline EchoPAC V.202 software (GE Medical Systems). Two-dimensional and Doppler echocardiography measurements and quantification were performed according to the American Society of Echocardiography and the European Association of Cardiovascular Imaging guidelines [15, 16]. The following measurements were collected: diastolic parameters, including peak early (E) and late (A) diastolic mitral inflow velocities, E/A ratio, deceleration time, lateral mitral annular diastolic velocity (Ea), peak systolic tricuspid annular velocity and tricuspid annular plane systolic excursion (TAPSE). All Doppler measurements were made over three cardiac cycles and averaged. Left ventricular end-diastolic and -systolic volumes, and ejection fraction were measured using the modified biplane Simpson’s method from apical two- and four-chambers views. Longitudinal strain (LS) was calculated using two-dimensional speckle tracking from greyscale images and the automated function imaging technique from the apical four-chambers, two-chambers and three-chambers views [17]. Strain values from all segments were averaged to obtain the global LS. Myocardial work was calculated from left ventricular LS and an estimated left ventricular pressure curve as proposed by Russell et al. [18]. After calculating global LS, indicating the time of aortic and mitral valve events by echocardiography and inserting values of arterial blood pressure, the software derived non-invasive pressure-strain loop. Peak systolic left ventricular pressure was assumed to be equal to the peak systolic blood pressure. Strain and pressure data were synchronized using the onset R wave on electrocardiogram as a common time reference. Myocardial work was calculated by integrating the power over time from mitral valve closure until mitral valve opening. Wasted work was defined by the work performed by the myocardium during segmental elongation, and constructive work by the work performed during segmental shortening represented. During isovolumetric relaxation, this definition was reversed such that myocardial work during shortening was considered wasted work and work during lengthening was considered constructive work. Work efficiency was then calculated as constructive work divided by the sum of constructive and wasted works. A “bull’s-eye” plots illustrating segmental and global LS, work index and work efficiency were automatically generated.

Statistical analysis

Continuous variables were tested for normal distribution using the Kolmogorov–Smirnov test and expressed as mean ± standard deviation. Laboratory findings and number of cardiovascular risk factors were not normally distributed, and results are, therefore, presented as medians with interquartile ranges (IQR). Nominal values were expressed as numbers and percentages. Group comparisons were made using nonparametric Kruskal–Wallis or Mann-Whitney rank sum tests when appropriate for continuous variables; and χ2 or Fischer exact tests when appropriate for categorical variables. Relationships between variables were assessed using Spearman correlation analysis and expressed by R. Differences were considered statistically significant for P-values of < 0.05. All analyses were performed using standard statistical software SPSS version 20 (SPSS Inc., Chicago, Illinois).

Results

We excluded 6 and 2 patients with history of heart disease and atrial fibrillation, respectively; 5 patients because of inadequate image quality for speckle tracking analysis, and 4 patients for prone position ventilation. Finally, 31 patients with COVID-19 and 16 controls were included for final analysis.

Baseline characteristics

Table 1 presents demographic characteristics by group according to the presence of SARS-CoV-2 infection and/or biological cardiac injury. Among the 31 patients with COVID-19 included in the study, all had bilateral pneumonia on chest computed tomography; 21 (68%) required invasive mechanical ventilation and were admitted to intensive care unit (ICU). 13 (42%) exhibited myocardial injury as indicated by elevated hs-TnT levels. hs-TnT ranged from 15 to 79 µg/L. On admission, none showed evidence of acute myocardial infarction, thromboembolic diseases, or chronic liver disease. No difference was found concerning cardiovascular risk factors: 1 [0-2], 0 [0-2] and 0 [1-3] among CoV−, CoV+/TnT− and CoV+/TnT+, respectively (P = 0.076). Patients CoV+/TnT + were older, had lower diastolic arterial pressure and were more likely to have hypertension and chronic renal failure, which were associated with a trend for presenting diabetes. Inotropic and/or vasopressor support was present in 4 (22%) CoV+/TnT− and 5 (38%) CoV+/TnT + patients (P = 0.433). Biologically, in addition to the cardiac injury, CoV+/TnT + had higher level of NT-proBNP and lower estimated glomerular filtration rate (CKD-epi), as well as lower hemoglobin level. Finally, nine (50%) CoV+/TnT− and 12 (92%) CoV+/TnT + patients were admitted in ICU (P = 0.020). No patient died during hospitalization and all patients were still alive 3 months after hospital discharge. The control group was broadly comparable except for characteristics defining infection by SARS-CoV2 (clinical symptoms, CRP and lymphocyte count).

Table 1

Baseline characteristics and laboratory and echocardiographic findings of the study population

	CoV−	CoV+/TnT−	CoV+/TnT+	P-value	Post-hoc analysis
	(n = 16)	(n = 18)	(n = 13)		1 vs. 2	2 vs. 3	3 vs. 1
Age, median (range), y	62 ± 16	52 ± 13	66 ± 8	0.015	0.234	0.002	0.203
Male, n (%)	10 (63)	16 (89)	11 (85)	0.143
Body mass index	25.2 ± 3.3	26.6 ± 3.9	27.9 ± 4.3	0.116
Signs and symptoms at admission, n (%)
Fever	0 (0)	17 (94)	12 (92)	< 0.001	< 0.001	1.000	< 0.001
Cough	2 (13)	16 (89)	9 (69)	< 0.001	< 0.001	0.208	0.003
Shortness of breath	6 (38)	15 (83)	8 (62)	0.023	0.012	0.228	0.272
Fatigue	3 (19)	12 (67)	8 (62)	0.012	0.007	1.000	0.027
Chest pain	12 (75)	3 (17)	0 (0)	< 0.001	0.001	0.225	< 0.001
Sore throat	1 (6)	4 (22)	0 (0)	0.110
Diarrhea	0 (0)	5 (28)	5 (38)	0.029	0.046	0.701	0.011
Chronic medical condition, n (%)
Hypertension	8 (50)	5 (28)	10 (77)	0.026	0.291	0.011	0.249
Diabetes	2 (13)	3 (17)	7 (54)	0.022	1.000	0.052	0.041
Hypercholesterolemia	2 (13)	2 (11)	2 (15)	0.939
Obesity	2 (13)	3 (17)	4 (31)	0.228
Cerebrovascular disease	1 (6)	0 (0)	1 (8)	0.513
Chronic renal failure	0 (0)	0 (0)	7 (54)	< 0.001	N/A	0.001	0.001
Chronic obstructive pulmonary disease	2 (13)	1 (6)	3 (23)	0.353
Sleep disordered breathing	1 (6)	1 (6)	3 (23)	0.231
Smoking habits, n (%)
Current smoking	2 (13)	0 (0)	1 (8)	0.322
Previous smoking	2 (13)	4 (22)	1 (8)	0.505
Medication at admission, n (%)
ACEI or ARB	5 (31)	4 (22)	7 (54)	0.179
Beta-blockers	1 (6)	0 (0)	2 (15)	0.224
Calcium channel blockers	4 (25)	2 (11)	5 (38)	0.203
Aspirin	3 (19)	0 (0)	1 (8)	0.147
Statin	4 (25)	1 (6)	2 (15)	0.282
Insulin	1 (6)	2 (11)	1 (8)	0.873
Systolic arterial pressure (mmHg)	134 ± 21	125 ± 23	125 ± 29	0.628
Diastolic arterial pressure (mmHg)	76 ± 14	71 ± 15	59 ± 11	0.007	0.227	0.034	0.002
Heart rate (bpm)	79 ± 19	77 ± 11	68 ± 15	0.099
Laboratory findings at admission, median (IQR)
High-sensitivity troponin T, µg/L	8 [0–14]	0 [0–11]	28 [17–45]	< 0.001	N/A	N/A	< 0.001
NT-proBNP, pg/mL	51 [0–1072]	84 [0–160]	233 [143–1590]	0.002	0.711	< 0.001	0.019
Creatinine, mg/dL	64 [59–87]	66 [61–81]	121 [89–199]	0.001	0.592	0.001	0.001
Leukocytes × 106/µL	7.7 [6.3–12.2]	7.6 [4.8–10.5]	6.5 [4.2–6.8]	0.262
Lymphocytes × 106/µL	2.1 [1.3–3.0]	1.0 [0.9–1.2]	0.8 [0.6–1.1]	0.002	0.004	0.366	0.002
Platelets × 103/µL	270 [215–324]	206 [158–258]	181 [128–275]	0.019	0.018	0.380	0.020
Hemoglobin, g/dL	14.2 [12.1–15.2]	13.0 [12.5–14.7]	11.8 [9.3–13.8]	0.013	0.313	0.017	0.010
C-reactive protein, mg/dL	2.8 [1.0–6.8]	129 [47–214]	131 [91–212]	< 0.001	< 0.001	0.631	< 0.001
Alanine aminotransferase, U/L	24 [20–33]	38 [33–105]	34 [26–47]	0.055
Aspartate aminotransferase, U/L	27 [24–44]	45 [22–78]	44 [24–68]	0.480
eGFR, mL/min	91 ± 18	99 ± 20	53 ± 28	< 0.001	0.120	< 0.001	0.001

ACEI angiotensin conversion enzyme inhibitor; ARB angiotensin receptor blockade; eGFR estimated glomerular filtration rate; IQR interquartile range; N/A not applicable

Cardiac phenotype by transthoracic echocardiography

Transthoracic echocardiographic findings according to the presence of SARS-CoV-2 infection and/or biological cardiac injury are presented in Table 2. No patients had wall motion abnormality.

Table 2

Transthoracic echocardiographic findings of the study population

	CoV−	CoV+/TnT−	CoV+/TnT+	P-value	Post-hoc analysis
	(n = 16)	(n = 18)	(n = 13)		1 vs. 2	2 vs. 3	3 vs. 1
LVEDV index, mL/m2	39 ± 8	40 ± 9	48 ± 17	0.180
Left ventricular systolic function
Left ventricular ejection fraction, %	64 ± 5	68 ± 6	66 ± 8	0.186
Global longitudinal strain, %	− 20 ± 3	− 19 ± 3	− 18 ± 3	0.277
Global myocardial work, %/mmHg	2167 ± 359	1922 ± 461	1774 ± 521	0.102
Global work efficiency, %	96 ± 2	94 ± 4	93 ± 3	0.042	0.285	0.192	0.007
Left ventricular diastolic function
E velocity, cm/s	69 ± 19	69 ± 12	75 ± 22	0.712
Deceleration time, ms	276 ± 101	227 ± 41	233 ± 41	0.220
A velocity, cm/s	76 ± 31	66 ± 24	72 ± 22	0.620
E/A ratio	1.0 ± 0.5	1.2 ± 0.4	1.1 ± 0.4	0.368
Ea lateral, cm/s	12 ± 3	13 ± 3	10 ± 3	0.028	0.280	0.008	0.101
E/Ea lateral ratio	6 ± 3	6 ± 2	8 ± 3	0.118
Right ventricular systolic function
TAPSE, mm	22 ± 4	20 ± 3	20 ± 4	0.137
Tricuspid annular S wave, cm/s	14 ± 3	15 ± 3	16 ± 3	0.074

LVEDV left ventricular end-diastolic volume; TAPSE tricuspid annular plane systolic excursion

Left ventricular end-diastolic volume index, ejection fraction and global longitudinal strain by speckle tracking were not different among the 3 groups. No patient exhibited right ventricular dilatation. There was a trend of decreased myocardial work and increased peak systolic tricuspid annular velocity between the CoV− and CoV + group (P = 0.047), which became significant when comparing CoV− and CoV+/TnT+ (P = 0.037). There was a decrease of global work efficiency between CoV− and then CoV+/TnT+ (P = 0.007). The left ventricular diastolic function did not discriminate between groups, except for the lateral Ea wave, which was lower in CoV+/TnT + patients when compared to CoV+/TnT− patients (P = 0.008). A summary of the main echocardiographic findings according to the presence of SARS-CoV-2 infection and/or biological cardiac injury is presented in Fig. 1.

Fig. 1

Bull’s-eye representation of longitudinal strain, myocardial work indices, and tricuspid annular S wave according to the presence of SARS-CoV-2 infection and/or biological cardiac injury. SARS-CoV-2: severe acute respiratory syndrome coronavirus-2

Finally, hs-TnT level was correlated with global work efficiency (R=-0.383, P = 0.009) but not with left ventricular ejection fraction (R = 0.160, P = 0.234), global LS (R = 0.154, P = 0.212) or global myocardial work (R = − 0.236, P = 0.114) (Fig. 2). NT-proBNP level was not correlated with any of left ventricular systolic function parameters (data not shown). Furthermore, there was a trend for a slight correlation between C-reactive protein and hs-TnT level (R = 0.287, P = 0.051).

Fig. 2

Correlations between hs-Troponin T and left ventricular systolic function parameters. GLS global longitudinal strain; GMW global myocardial work; GWE global work efficiency; LVEF left ventricular ejection fraction; TAPSE tricuspid annular plane systolic excursion

Discussion

This is the first study showing that SARS-CoV-2 infection have little impact on the heart. Even in the presence of cardiac injury, direct systolic function parameters such as left ventricular ejection fraction or global are not altered. Only myocardial work indices are impaired by the SARS-CoV-2 infection with a trend to decrease of global myocardial work in case of cardiac injury, as well as a decrease in global work efficiency, parameters that depend on the afterload. Finally, we show a trend for increase of right ventricular systolic function assessed by peak systolic tricuspid annular velocity between controls and patients with COVID-19, particularly in case of cardiac injury. Despite evidences showing the negative prognostic impact of biological cardiac injury (i.e. increased troponin) in the presence of SARS-CoV-2 infection [5, 19, 20], there are, to date, no data on the functional impact of this injury.

Although there may have been warnings of an association between ST-segment elevation myocardial infarction and COVID-19 [21], the epidemiological series suggested rather a decrease in the number of acute myocardial infarction to a decrease in the use of specialized channels [22, 23]. Despite biological cardiac injury, our study did not find electrocardiographic signs of acute coronary syndrome or echocardiographic wall motion abnormality. It appears that the increase in troponin is only a consequence of the severity of the inflammatory syndrome and systemic impairment [19], and that heart failure is not at the forefront. However, the fact remains that patients with concomitant cardiac disease and COVID-19 have a poor prognosis compared with patients without a history of cardiac disease. The higher mortality is not necessarily driven by cardiac etiology [24] and reflects incompetent hemodynamic adaptation. Our study shows that the direct effects on the myocardium are weak, with in particular an absence of repercussions on left ventricular ejection fraction and global LS. The effects of SARS-CoV-2 infection are manifested at most by an alteration in left ventricular relaxation as shown by the decrease of the lateral Ea velocity. In contrast, cardiac involvement is accompanied by a decrease in myocardial work indexes. This occurs in patients with many cardiovascular risk factors and more severe infection as shown by mechanical ventilation, decreased diastolic blood pressure, impaired renal function and strong biological inflammatory syndrome.

Right ventricular dilatation [25] and systolic function [26] have been reported as prognostic factors in COVID-19 patients. The right ventricle is known to be sensitive to afterload [27] and its dilatation and alteration of systolic function are most often related to an increase in systolic pulmonary pressures. As reported in the study by Li and co-authors [26], it reflects the severity of the acute respiratory distress syndrome associated with the SARS-CoV2 infection and explain its prognostic impact. On the other hand, the high frequency of coagulopathies and thromboembolic events, including pulmonary embolism [28], reported in COVID-19 patients could explain the prognostic impact of right ventricular dilatation and systolic function and D-dimer [29, 30]. On the contrary, in our study, we show an absence of right ventricle dilatation including in patients with acute respiratory distress syndrome. We found a tendency to improve right ventricular systolic function in COVID-19 patients, particularly in case of cardiac injury, through the increase of the tricuspid annular S-wave. This finding could simply be the consequence of an initial phase of right ventricle compensation for lung damage in COVID-19.

Finally, the slight functional impact of the biological cardiac injury on the myocardium, with regard to its prognostic impact, could be explained either by a type 2 myocardial infarction (oxygen supply/demand imbalance) as a consequence of the severity of the infection, or a direct inflammation of the myocardium without functional impact. Recent findings suggest that SARS-CoV-2 infection could facilitate the induction of endotheliitis in several organs as a direct consequence of viral involvement [31]. On the other hand, a recent autopsy study shows that the presence of large amounts of the virus in the heart is accompanied by a cytokine response without inflammatory cell infiltration [32]. Cardiac magnetic resonance imaging studies on patients recovered from COVID-19 with cardiac symptoms or unexplained elevated hs-TnT confirm the absence of left ventricular systolic dysfunction and suggest a mixed mechanism showing that cardiac injury in SARS-CoV-2 infection is associated with myocardial edema and then fibrosis [33, 34] with a heterogeneous pattern of late gadolinium enhancement including ischemic and non-ischemic patterns as myocarditis-like or non-specific mid-wall late gadolinium enhancement [35].

Limitations

The main limitation of our study is that it is a single-site and limited sample studies. However, it takes place in a teaching hospital of a wild suburban area. Moreover, all patients referred to either the medical or the intensive care units for COVID-19 were consecutively included. This study is therefore representative of a sample of the COVID-19 patients and is one of the few to describe the left ventricular functional impact of SARS-CoV2 acute phase infection using sensitive tools integrating after-load such as myocardial work indices.

Finally, our results are to be interpreted in the light of the low mortality of our population, which does not allow us to conclude that myocardial damage may be more pronounced in more severe patients. Furthermore, the absence of short-term impact does not allow to conclude on the absence of long-term consequences of cardiac injury during infection.

Conclusions

The cardiac injury associated with SARS-CoV-2 infection has a low functional impact on the myocardium, essentially reflected in a decrease in myocardial work indices, which are dependent on left ventricular after-load. The cardiac impact of SARS-CoV-2 infection appears to be related to cardiovascular risk factors and the severity of the sepsis.