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Original research
Mortality and ventricular arrhythmia after acute myocarditis: a nationwide registry-based follow-up study
  1. Kristian Hay Kragholm1,2,
  2. Filip Lyng Lindgren1,
  3. Tomas Zaremba1,
  4. Phillip Freeman1,
  5. Niels Holmark Andersen1,
  6. Sam Riahi1,
  7. Manan Pareek3,
  8. Lars Køber4,
  9. Christian Torp-Pedersen5,
  10. Peter Søgaard1,
  11. Andreas Hagendorff6 and
  12. Bhupendar Tayal1
  1. 1Department of Cardiology, Aalborg University Hospital, Aalborg, Denmark
  2. 2Unit of Clinical Biostatistics and Epidemiology, Aalborg University Hospital, Aalborg, Denmark
  3. 3Department of Cardiology, Nordsjællands Hospital, Hillerod, Denmark
  4. 4Department of Cardiology, Rigshospitalet, Copenhagen, Denmark
  5. 5Department of Cardiology, Nordsjaellands Hospital, Hillerod, Denmark
  6. 6Department of Cardiology, Leipzig University, Leipzig, Germany
  1. Correspondence to Dr Kristian Hay Kragholm; kdks{at}rn.dk

Abstract

Objective Incidence and severity of acute myocarditis vary significantly in previous reports and there is a lack of epidemiological studies on the short-term risks of mortality, heart failure and ventricular arrhythmias in patients with acute myocarditis. Therefore, study aims were to examine 90-day risks of mortality, heart failure (HF) and ventricular arrhythmias in patients with acute myocarditis in comparison to age-matched and sex-matched background population controls.

Methods In this nationwide register-based follow-up study of patients hospitalised with myocarditis between 2002 and 2018 in Denmark, 90-day risks of all-cause mortality, HF, ventricular arrhythmias (ventricular tachycardia, ventricular fibrillation (VF)), cardiac arrest and implantable cardioverter-defibrillator (ICD) implantation were compared with age-matched and sex-matched controls from the background population (1:5 matching). Absolute risks standardised to the age, sex and comorbidity distribution of the entire study population were derived from multivariable Cox regression.

Results A total of 2523 patients hospitalised with myocarditis were included. Median age was 48 years (Q1–Q3: 30–69) and 67.7% were men. Comorbidity burden was more pronounced among patients with myocarditis relative to controls. Standardised 90-day all-cause mortality risk was 4.9% for patients with acute myocarditis versus 0.3% for controls (p<0.001). Ninety-day standardised risks for other endpoints were 7.5% versus 0.1% for HF, 1.9% versus <0.1% for VF/VF/arrest risk and 1.6% versus <0.1% for ICD implantation (all p<0.001).

Conclusions In this large nationwide register-based follow-up study, patients hospitalised with myocarditis had significantly higher 90-day risks of all-cause mortality, HF, ventricular arrhythmias, cardiac arrest and ICD implantation compared with background population controls.

  • myocarditis
  • tachycardia
  • ventricular
  • ventricular fibrillation
  • defibrillators
  • implantable

Data availability statement

Data may be obtained from a third party and are not publicly available. According to Statistics Denmark regulations, data used for this study cannot be shared, as data is stored on and may not leave secure servers on Statistics Denmark. Access to data on these servers can be granted upon adequate permission.

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Key questions

What is already known about this subject?

  • Incidence and severity of acute myocarditis vary significantly in previous reports and there is a lack of epidemiological studies on the short-term risks of mortality, heart failure and ventricular arrhythmias in patients with acute myocarditis.

What does this study add?

  • In this large nationwide register-based follow-up study of 2523 patients hospitalised with myocarditis, 90-day risks of all-cause mortality, heart failure, ventricular arrhythmias, cardiac arrest and implantable cardioverter-defibrillator implantation were significantly higher when compared with background population controls.

How might this impact on clinical practice?

  • These findings suggest that patients with acute myocarditis may benefit from careful diagnostic work-up including cardiac monitoring in the early phase after diagnosis. Further studies focusing on risk stratification for these patients are warranted.

Introduction

Myocarditis is an inflammation of the myocardium, primarily affecting young and otherwise healthy individuals, although it may also appear in patients with a history of cardiovascular disease.1 Its clinical presentation spans from almost asymptomatic patients, with mild palpitations or chest pain, to cardiovascular collapse and death.2 In its mild form, myocarditis often resolves without any treatment. However, in its more fulminant form, it may account for up to 42% of the events of sudden cardiac death among young, often athletic, individuals.3–5 Patients who survive have an increased risk of arrhythmias, dilated cardiomyopathy and death compared with the general population.6–9 Autopsy reports estimate an incidence of acute myocarditis ranging from 0.1% to up to 10%.3 10–12 Given a lack of epidemiological studies, and because estimates of incidence and severity of acute myocarditis vary significantly, we investigated short-term (90-day) risks of mortality, heart failure (HF) and ventricular arrhythmias (ventricular tachycardia (VT), ventricular fibrillation (VF), cardiac arrest and implantable cardioverter-defibrillator (ICD) implantation procedures) in patients hospitalised with myocarditis in Denmark between 2002 and 2018 and compared with age-matched and sex-matched population controls using a nationwide registry-based follow-up design.

Methods

Data sources and study population

This nationwide registry-based follow-up study is based on The Danish Civil Registration System containing all registered Danish citizens, their unique personal identification numbers, sex, date of birth and date of death.13 This registry can be used to link data to other nationwide administrative databases. The Danish National Patient Register was used to include all patients between 2002 and 2018 with a first-time hospitalisation with a myocarditis diagnosis, either as a primary or a secondary diagnosis with a primary diagnosis of HF, VT/VF/arrest, ICD implantation or atrial fibrillation or flutter (AF).14 These secondary diagnoses were chosen as the clinical presentation of acute myocarditis may involve HF, VT/VF/arrest, AF and/or lead to ICD implantation. The acute myocarditis population was age-matched and sex-matched to population controls, without a diagnosis of prior acute myocarditis, in a 1:5 ratio.

Diagnostic work-up for acute myocarditis

The Danish National Patient Register was used to obtain data on pre-existing medical conditions, medical examinations and hospital and outpatient contacts including relevant diagnoses, procedures and surgical codes. The diagnostic work-up for acute myocarditis includes echocardiography and although we did have data on whether coronary CT angiography (CCTA), coronary angiogram (CAG), positron emission tomography CT (PET-CT), endomyocardial biopsy (EMB) and cardiac MRI (CMR) additionally were performed, results of all these investigations including echocardiography, as well as ECG and cardiac biomarkers (troponins) were not available from the registry. The role of CCTA and CAG in the diagnostic work-up was to rule out ischaemic heart disease. Diagnostic work-up was assessed in a 30-day time span both prior to and 30 days after the diagnosis of acute myocarditis. Furthermore, data on mortality at follow-up were collected in relation to each diagnostic work-up. As CMR was first introduced as a diagnostic tool in Denmark in 2007, the number of performed CMRs relative to other examinations was expected to be low.

Other study variables

In addition to patient age and sex, prior cardiac procedures including percutaneous coronary intervention (PCI), coronary artery bypass grafting (CABG) and ICD implantations as well as the following comorbid conditions were assessed within the last 5 years prior to the acute myocarditis index date using the Danish National Patient Registry: hypertension, diabetes, chronic obstructive pulmonary disease (COPD), prior myocardial infarction (MI), prior ischaemic heart disease (IHD), AF, stroke, peripheral artery disease (PAD), prior HF, prior VT/VF, cardiac arrest and chronic kidney disease (CKD). Hypertension, diabetes and COPD were defined as either a relevant diagnosis code or relevant and specific prescription medication within the last 180 days prior to the acute myocarditis index date using data from the Danish Prescription Registry.15 As done previously, the prescription medication definition of hypertension was redemption of at least two antihypertensive drugs in two consecutive quarters prior to study inclusion.16

Outcomes

The primary outcome was 90-day all-cause mortality. Secondary outcomes were 90-day presumed cardiovascular cause of death and 90-day risks of HF, a composite of VT or VF or cardiac arrest (VT/VF/arrest) and ICD implantation. Cardiac arrest was defined as a diagnosis made in the hospital and registered in The Danish National Patient Register.

Statistical analysis

Continuous data are presented as median and first to third quartiles (Q1–Q3) and categorical data as counts and percentages. Mann-Whitney and Pearson’s χ2 tests were performed to report crude between-group differences. Kaplan-Meier and Aalen-Johansen estimators were calculated to present crude absolute risks of mortality and outcomes of HF, a composite of VT or VF or cardiac arrest (VT/VF/arrest) and ICD implantation. Adjusted HRs and absolute risks for patients with acute myocarditis versus population controls standardised to the age, sex and comorbidity distribution of the entire study population were derived from multivariable Cox regression.17 Standardisation ensures that when patients with myocarditis are compared with population controls, all covariates including age, sex and comorbidities are held equal between the two comparison groups. The following covariates were included in the models: age, sex, hypertension, diabetes, COPD, prior MI, prior IHD, PCI, CABG, stroke, PAD, AF, HF, prior VT/VF/arrest and CKD. Sensitivity analyses were performed on patients <60 years since a prior study showed that the diagnostic accuracy of acute myocarditis from the Danish National Patient Registry was high in this age group.18 Since IHD is a potential differential diagnosis to myocarditis, a sensitivity analysis in which MI or revascularisation events were treated as competing risks were additionally performed to exclude that outcome events were driven by IHD. Two-sided p values <0.05 were considered statistically significant. Data management and analyses were performed using SAS, V.9.4 and R, V.3.6.1.19

Patient consent and ethical approval

According to Danish legislation, ethical committee approval or patient consent is not required for the conduct of register-based studies. In compliance with the General Data Protection Regulation, the data responsible institute in the Capital Region of Denmark has approved the use of the data sources for research purposes (approval number P-2019–404).

Results

Patients, characteristics and diagnostic work-up

A total of 15 138 subjects were included, 2523 in the acute myocarditis group and 12 615 in the control group. Of the 2523 patients hospitalised with myocarditis, 2104 had a primary diagnosis of myocarditis and 419 had a diagnosis of myocarditis secondary to HF, VT/VF/arrest, ICD device implantation or AF. Median age of patients with acute myocarditis was 48 years (Q1–Q3: 30–69 years) and approximately two-thirds were men (67.7%). The distribution of comorbidities in patients with acute myocarditis and population controls is listed in table 1. Diagnostic studies performed for patients with acute myocarditis are shown in table 2. Approximately 45% and 5% underwent CAG and CCTA, respectively, to rule out IHD as part of the diagnostic work-up. During 2002–2007, 33 of 796 (4.2%) patients underwent either CMR (n=3) or EMB (n=30), whereas 250 of 1727 (14.5%) underwent EMB (n=68) and/or CMR (n=211) during 2008–2018. EMB use was stable over time, with 30 procedures recorded during 2002–2007 (3.8%) versus 68 (3.9%) during 2008–2018. CMR was performed in 3 (0.4%) patients during 2002–2007 and in 211 (12.2%) patients during 2008–2018. In total, only nine patients (0.4%) underwent PET-CT.

Table 1

Characteristics for patients with acute myocarditis versus age-matched and sex-matched population controls

Table 2

Diagnostic work-up, advanced in-hospital treatment and selected post-discharge medications for the 2523 patients with acute myocarditis

Outcomes for patients with acute myocarditis versus population controls

Relative to population controls, patients with acute myocarditis had significantly higher crude incidences of all-cause mortality, HF, VT or VF or cardiac arrest and ICD implantation within 90 days of follow-up (figure 1). These differences remained significant when standardising the absolute risks to the age, sex and comorbidity distribution of the entire study population: 90-day all-cause mortality risks of 4.9% versus 0.3%, 90-day HF risks of 7.5% versus 0.1%, 90-day VF/VF/arrest risks of 1.9% versus <0.1% and 90-day ICD implantation risks of 1.6% versus <0.1% (figure 2). The corresponding HRs are shown in figure 3.

Figure 1

Crude 90-day outcomes of all-cause mortality, HF, ventricular arrhythmias and ICD implantation. HF, heart failure; ICD, implantable cardioverter-defibrillator; VF, ventricular fibrillation; VT, ventricular tachycardia.

Figure 2

Standardised 90-day absolute risks of all-cause mortality, HF, ventricular arrhythmias and ICD implantation. The reported absolute risks for patients with acute myocarditis versus population controls standardised to the age, sex and comorbidity distribution of all patients were derived from multivariable Cox regression. The following covariates were included in the models: patient age, sex, hypertension, diabetes, chronic obstructive pulmonary disease, prior myocardial infarction, prior ischaemic heart disease, percutaneous cardiac intervention, coronary artery bypass grafting, stroke, peripheral artery disease, atrial fibrillation or flutter, HF, prior ventricular VT/VF/arrest and chronic kidney disease. HF, heart failure; ICD, implantable cardioverter-defibrillator; VF, ventricular fibrillation; VT, ventricular tachycardia.

Figure 3

Adjusted HRs of 90-day all-cause mortality, HF, ventricular arrhythmias and ICD implantation for patients with acute myocarditis vs age-matched and sex-matched population controls. The multivariable Cox regression models included the following covariates: patient age, sex, hypertension, diabetes, chronic obstructive pulmonary disease, prior myocardial infarction, prior ischaemic heart disease, percutaneous cardiac intervention, coronary artery bypass grafting, stroke, peripheral artery disease, atrial fibrillation or flutter, HF, prior ventricular VT/VF/arrest and chronic kidney disease. HF, heart failure; ICD, implantable cardioverter-defibrillator; VF, ventricular fibrillation; VT, ventricular tachycardia.

Ventricular arrhythmic events among patients with myocarditis

Among the 2523 patients with myocarditis, 54 (2.1%) had an arrhythmic event of either VT/VF or cardiac arrest within 90 days of follow-up. Of these 54 cases, 12 (22.2%) died within 90 days of follow-up and 23 (42.6%) had an ICD implanted within 90 days of follow-up. Among 57 (2.3%) of the patients with myocarditis who had an ICD implanted within 90 days, the 23 patients with a VT/VF/arrest event represented 38.3% of all who had an ICD implanted.

Sensitivity analyses of patients below 60 years of age

A total of 1445 patients with acute myocarditis and 7225 controls formed the basis for the sensitivity analyses of patients <60 years of age. Although overall event rates were lower compared with the complete study population, the risks remained significantly higher for patients with acute myocarditis relative to controls, with 90-day mortality risks of 1.1% (95% CI 0.5% to 1.7%) versus <0.1% (p<0.001), 90-day HF risks of 5.8% (95% CI 4.6% to 7.1%) versus <0.1% (p<0.001), 90-day VT/VF/arrest risks of 1.5% (95% CI 0.8% to 2.2%) versus <0.1% (p<0.001) and 90-day ICD implantation risks of 1.7% (95% CI 1.0% to 2.4%) versus <0.1% (p<0.001).

Other sensitivity analyses

All-cause mortality in relation to whether specific diagnostic studies were performed is shown in table 3. Patients who underwent EMB had significantly higher mortality, potentially indicating a more severe disease course of the myocarditis condition. Standardised absolute risks of the study outcomes among patients with myocarditis diagnosed before versus after increasing availability and use of CMR (years 2002–2007 vs 2008–2018) are shown in table 4. The standardised absolute 90-day VT/VF/arrest risk was significantly lower in 2008–2018 versus in 2002–2007, with 1.6% versus 3.3%. Results from analyses of the 90-day HF risk in patients with acute myocarditis on exclusion of patients with prior HF (6.8% for patients with acute myocarditis versus <0.1% for controls), as well as results from analyses of the 90-day risk of VT/VF/arrest in patients with acute myocarditis without prior VT/VF/arrest (1.8% for patients with acute myocarditis versus <0.1% for controls) were comparable to the main study findings. Outcomes when MI or revascularisation events during the 90-day follow-up period were considered competing risks were comparable to the overall results and can be found in figure 4.

Figure 4

Standardised 90-day absolute risks of all-cause mortality, HF, ventricular arrhythmias and ICD implantation, with myocardial infarction or revascularisation events during the 90-day follow-up period as competing risks. The reported absolute risks for patients with acute myocarditis versus population controls standardised to the age, sex and comorbidity distribution of all patients were derived from multivariable Cox regression. The following covariates were included in the models: patient age, sex, hypertension, diabetes, chronic obstructive pulmonary disease, prior myocardial infarction, prior ischaemic heart disease, percutaneous cardiac intervention, coronary artery bypass grafting, stroke, peripheral artery disease, atrial fibrillation or flutter, HF, prior ventricular VT/VF/arrest and chronic kidney disease. HF, heart failure; ICD, implantable cardioverter-defibrillator; VF, ventricular fibrillation; VT, ventricular tachycardia.

Table 3

Standardised 90-day all-cause mortality risks in relation to diagnostic work-up

Table 4

Standardised 90-day risks in relation to periods 2008–2018 versus 2002–2007 among the 2523 patients with acute myocarditis

Discussion

This Danish nationwide registry-based study showed that 90-day incidences of all-cause mortality, HF, ventricular arrhythmias, cardiac arrest and ICD implantation were significantly higher among patients with acute myocarditis compared with controls. This may entail a more careful diagnostic work-up and monitoring strategy in the early phase after diagnosis of acute myocarditis to identify patients at high risk for incident cardiovascular events.

There are a very limited numbers of study with large data who have investigated the incidence of adverse cardiovascular events after acute myocarditis. There is a wide variability in the incidences of adverse cardiovascular outcomes among patients with acute myocarditis. As an example, reported incidences of dilated cardiomyopathy among patients with histologically positive acute myocarditis have ranged between 14% and 50%.20 In a recent series of 174 patients with EMB (and thus Dallas criteria21) positive myocarditis, 17% suffered death or heart transplantation within the first 2 years.22 Moreover, a large Spanish national health service registry study (N=14 147) reported a 3% in-hospital mortality among patients admitted with acute myocarditis between 2003 and 2015.23 This appears to be fairly compatible with our results considering that our study included follow-up data until 3 months post diagnosis. Part of the variability in outcomes is likely related to the heterogeneity of the myocarditis condition, with multiple underlying causes with distinct prognosis, warranting further investigation.

Complementing prior research,3–5 8 24 our study also suggests that acute myocarditis is a severe disease associated with a significantly increased short-term risk of death. Even though patients with acute myocarditis had more pre-existing comorbidities compared with the age-matched and sex-matched population controls in our study, the acute myocarditis population still had a significantly elevated mortality risk when standardising to the age, sex and comorbidity distribution of all individuals included. In this analysis, the 90-day mortality risk was 4.9% for patients with acute myocarditis versus 0.3% for the age-matched and sex-matched population controls. This emphasises the importance of rapid diagnosis and targeted management to potentially improve survival. In addition to the increased mortality risk, risks of ventricular arrhythmias, cardiac arrest and ICD implantation were also substantially higher among patients with acute myocarditis relative to the population controls. Accordingly, in-hospital and additionally post-discharge cardiac monitoring of patients with acute myocarditis may aid in early arrhythmia detection to potentially prevent fatal outcomes. As for the increased short-term risk of HF, this may have clinical implications in the sense that early detection of left ventricular dysfunction would allow for earlier initiation of guideline-directed medical and device therapy.

EMB use was stable just below 4% throughout the study period. Although this seems low, use of EMB is limited in routine clinical practice and generally reserved for the most severe cases. This is also supported by our results, as we observed significantly higher event rates in patients who underwent EMB relative to those who did not. Several explanations may be provided for the limited use of EMB. First, acute myocarditis is usually associated with focal inflammation and may involve a region inaccessible by biopsy.25 Second, there seems to be poor agreement between observers.26 Finally, timely performance of EMB is important as the degree of inflammation may decrease over time, but this may not always be possible due to lack of facilities or adequate clinical expertise.

CMR use was limited prior to 2007, but its subsequent use in diagnosing acute myocarditis increased substantially. CMR is relatively safe and accessible, and has very high sensitivity, specificity and accuracy in diagnosing acute myocarditis.27 28 Applying the three proposed criteria by Friedrich et al of T2-weighted focal myocardial oedema, T1-weighted early gadolinium enhancement suggesting hyperaemia and late gadolinium enhancement suggesting fibrosis or inflammation, identification of acute myocarditis by CMR is relatively accurate.28 However, there can be some technical limitations, and similar to EMB, timely performance is key for the accuracy in diagnosis. Interestingly, the recent focus on performing CMR in patients with MI and non-obstructive coronary artery disease also appears to have led to an increased detection of acute myocarditis.29 Furthermore, CMR could potentially be used for risk stratification into groups who are at risk of developing fatal cardiac complications, and those who are not.19–21 The studies in this field are limited, both in number of studies and of patients within the studies and should be a field of future research.

Strengths and limitations

Strengths of our study include the large sample size and the negligible loss to follow-up. The short-term risk assessment window increases the possibility of an underlying plausible and causal relation between the myocarditis condition and events. Limitations include the register-based, observational design and potential uncertainty regarding the myocarditis diagnosis, including the lack of results from the diagnostic work-up. Nevertheless, a diagnosis of acute myocarditis in the context of a CMR, a PET-CT or an EMB suggests high diagnostic certainty. The positive predictive value of acute myocarditis in the Danish National Patient Register was previously shown to be >80% for patients <60 years of age, but ≈65% for older patients.18 Although event rates were lower for patients <60 years of age, this sensitivity analysis still found significantly higher mortality risk for patients with acute myocarditis relative to population controls, and as such, results were in agreement with the overall study results. In addition, the 90-day mortality risk was significantly elevated among patients with myocarditis who were examined with an EMB, indicating on one hand a more severe disease condition but also underscoring the likely causal association between myocarditis and fatal event risk. In continuation, staging of myocarditis including fulminant and non-fulminant conditions were otherwise not possible to define. Because myocardial ischaemia represents a common differential diagnosis of acute myocarditis, it was reassuring that results from analyses in which MI or revascularisation events during the 90-day follow-up period were considered competing risks were comparable to the overall results. Lastly, and as pointed out in the methods section, the study lacks several important clinical data and test results of troponins, ECGs (including QRS parameters), imaging modalities including echocardiography (including left ventricular ejection fraction), CMR, coronary artery status from CCTA and CAG and the actual EMB diagnosis and indication for ICD implantation. Nonetheless, the significantly elevated arrhythmic risk in the short run, which was consistent in younger patients with myocarditis, for whom the diagnostic performance of diagnosis coding has been shown to be of high quality, speaks towards a plausible link between myocarditis and an elevated arrhythmic risk. Future studies are needed to examine predictors of these adverse outcomes and the role and timing of cardiac monitoring to prevent these potentially fatal events. An important aspect of such future studies involves identification of the underlying causes for risk stratification and adverse outcome prevention.

Conclusion

This large nationwide register-based follow-up study of patients with acute myocarditis showed that patients with acute myocarditis have increased 90-day risks of all-cause mortality, HF, ventricular arrhythmias, cardiac arrest and ICD implantation when compared with age-matched and sex-matched background population controls. These findings suggest that patients with acute myocarditis may benefit from careful diagnostic work-up including cardiac monitoring in the early phase after diagnosis. Further studies focusing on risk stratification for these patients are warranted.

Data availability statement

Data may be obtained from a third party and are not publicly available. According to Statistics Denmark regulations, data used for this study cannot be shared, as data is stored on and may not leave secure servers on Statistics Denmark. Access to data on these servers can be granted upon adequate permission.

Ethics statements

Patient consent for publication

References

Footnotes

  • Contributors KHK, BT, AH and PS designed the study. KHK and FLL drafted the manuscript. KHK performed all statistical analyses. All authors provided substantial contributions to data interpretation and critical revisions, and all authors approved the final manuscript. KHK, FLL and BT are responsible for the overall content as guarantor and thereby accept full responsibility for the finished work and the conduct of the study, including access to the data.

  • Funding The authors have not declared a specific grant for this research from any funding agency in the public, commercial or not-for-profit sectors.

  • Competing interests KHK: Speaker’s honoraria from Novartis. PS: Speaker for GE Healthcare, advisory board member (Novartis Pharmaceuticals Corp, AstraZeneca Pharmaceuticals, Biotronik), research grants Wics, Bayer and GE Healthcare. MP: Advisory board for AstraZeneca and Janssen-Cilag, speaker’s free from AstraZeneca, Bayer, Boehringer Ingelheim and Janssen-Cilag. TZ: Speaker’s fee from AstraZeneca. AH: Speaker for AstraZeneca, Cardiac Dimensions, Daiichi-Sankyo, GE Healthcare and Novartis.

  • Provenance and peer review Not commissioned; externally peer reviewed.