Abstract
Background Cardiac sarcoidosis (CS) is a life-threatening condition in which clear recommendations are lacking. We aimed to systematically review the literature on cardiac sarcoidosis treated by corticosteroids and/or immunosuppressive agents in order to update the management of CS.
Methods Using PubMed, Embase and Cochrane Library databases, we found original articles on corticosteroid and standard immunosuppressive therapies for CS that provided at least a fair Scottish Intercollegiate Guidelines Network (SIGN) overall assessment of quality and we analysed the relapse rate, major cardiac adverse events (MACEs) and adverse events. We based our methods on the PRISMA statement and checklist.
Results We retrieved 21 studies. Mean quality provided by SIGN assessment was 6.8 out of 14 (range 5–9). Corticosteroids appeared to have a positive impact on left ventricular function, atrioventricular block and ventricular arrhythmias. For corticosteroids alone, nine studies (45%, n=351) provided data on relapses, representing an incidence of 34% (n=119). Three studies (14%, n=73) provided data on MACEs (n=33), representing 45% of MACEs in patients treated by corticosteroid alone. Nine studies provided data on adjunctive immunosuppressive therapy, of which four studies (n=78) provided data on CS relapse, representing an incidence of 33% (n=26). Limitations consisted of no randomised control trial retrieved and unclear data on MACEs in patients treated by combined immunosuppressive agents and corticosteroids.
Conclusion Corticosteroids should be started early after diagnosis but the exact scheme is still unclear. Studies concerning adjunctive conventional immunosuppressive therapies are lacking and benefits of adjunctive immunosuppressive therapies are unclear. Homogenous data on CS long-term outcomes under corticosteroids, immunosuppressive therapies and other adjunctive therapies are lacking.
Abstract
Corticosteroids are the mainstay treatment for cardiac sarcoidosis. Conventional immunosuppressive agents might be of interest at diagnosis. Cohort studies are clearly heterogeneous. Large cohort and prospective studies using “strong” end-points are lacking. https://bit.ly/3t9Rv8O
Introduction
Sarcoidosis is a rare multisystemic granulomatous disease of unknown aetiology, which most frequently involves the lungs, lymph nodes, skin, eyes, liver and spleen [1]. Cardiac sarcoidosis (CS) is a rare condition, with symptomatic cardiac features reported in 2.3–39% of patients with sarcoidosis [2, 3]. Cardiac involvement in sarcoidosis ranges from 27% to 50% in morphological studies [4, 5]. Although CS is rare, it can be a life-threatening condition, mainly with left ventricular (LV) systolic failure, ventricular arrhythmias (VAs) and atrioventricular (AV) conduction abnormalities, which can lead to disability or cardiac sudden death [6]. There has been a great deal of progress in research [7], diagnosis and management [8] of CS over the past few years. Corticosteroid therapy (CT) remains the mainstay treatment for CS, although there is a lack of prospective controlled studies, and treatment should be started early after CS diagnosis [9]. The treatment is recommended on the basis of clinicians’ experience, expert opinions and observational cohort studies. To our knowledge, only two studies have investigated the impact of adjunctive immunosuppressive therapy on CS [10, 11]. In 2013, Sadek et al. [9] published a systematic review of CT as the mainstay treatment for CS.
We conducted a systematic review of the literature on CT and/or immunosuppressive therapy (IT) for CS. The aim of this study was to evaluate the impact of CT and/or immunosuppression on CS relapse, on the effects of sparing CT and on major adverse cardiovascular events (MACEs) (defined as cardiac death, ventricular fibrillation, sustained ventricular tachycardia or hospitalisation for heart failure), as well as to study adverse drug events.
Methods
Data collection
We searched the PubMed, Embase and Cochrane Library databases using the search terms “cardiac sarcoidosis” and “immunosuppressive treatment” and “corticosteroid” (full search terms shown in supplement 1) and included all studies dealing with CS treatment from January 1980 to June 2019, excluding studies with tumour necrosis factor-α (TNF-α) antagonists’ therapy because of their recent use in refractory CS cases after CT or IT failure [12].
Study selection
Studies were reviewed by two independent reviewers (J. Stievenart and V. Grobost). The inclusion criteria for relevant studies were as follows: English-language studies of CS diagnosed by endomyocardial biopsy, Heart Rhythm Society criteria [13], Japanese Ministry of Health and Welfare criteria [14] or World Association of Sarcoidosis and Other Granulomatous Diseases (WASOG) criteria [15]; follow-up of ≥1 year; CT and/or IT (methotrexate, azathioprine, mycophenolate mofetil, cyclophosphamide or other conventional immunosuppressive agents) data on used schemes; and outcomes provided. We excluded studies that did not contain sufficient data or fulfil the inclusion criteria, and studies that treated patients with TNF-α antagonists. Studies were reviewed and included on the agreement of two independent reviewers (V. Grobost and J. Stievenart) using the title, abstract and full-text article if necessary; in cases of disagreement, we used a third reviewer (M. Ruivard). We included studies if there were enough data to supply a 2×2 table based on treatments used and outcomes. Duplicate publications were excluded, as were review articles, conference papers, isolated case reports, case series with fewer than five patients and letters.
Quality assessment and data extraction
Study quality was assessed independently by two reviewers (J. Stievenart and V. Grobost) using the Scottish Intercollegiate Guidelines Network (SIGN) checklist (supplement 2) [16]. Only studies with good or fair quality were included in the final review. Relevant information such as demographic characteristics, treatment, outcomes and relapse were abstracted.
End-points
The end-points were relapse (clinical and/or imaging relapse defined as onset of new CS manifestations or worsening of pre-existing manifestations), MACEs (defined as cardiac death, ventricular fibrillation, sustained ventricular tachycardia and hospitalisation for heart failure) and adverse drug events.
Results
Description of selected studies
A total of 1698 references were retrieved from PubMed, Embase and Cochrane Library databases. After abstract review and full-text assessment, 21 published studies were selected (figure 1). Authors, study design, diagnostic criteria, inclusion and exclusion criteria and sample size are summarised in table 1. Fourteen (66%) of the selected studies were Japanese. Only one study was prospective. Four studies were multicentric. No randomised control trial was retrieved. Using the SIGN overall assessment for cohort studies, the mean quality was 6.8 out of 14 (range 5–9). All studies provided good overall assessment.
Quantitative analysis
Baseline characteristics
Main baseline patient characteristics, including average age, mean follow-up, clinical outcomes and treatment, are summarised in table 2. The selected studies included 950 patients, whose average age ranged from 38 to 65 years. Mean follow-up ranged from 12 to 118.8 months. Prevalence of LV dysfunction or congestive heart failure ranged from 0% to 64% at baseline. Prevalence of atrioventricular block (AVB), ventricular tachycardia (VT), ventricular fibrillation (VF) and pacemaker or implantable cardioverter defibrillator implantation varied depending on study design, from 2.4% to 91.9% of selected patients from retrieved studies. Data on implantation indications and devices were scarce.
Treatment regimen
Among the 950 patients, 709 were treated with corticosteroid alone and 155 with corticosteroids and immunosuppressive agents. CT regimens are listed in supplementary table S1. Prednisone dose ranged from 20 to 60 mg·day−1, tapered every 6–8 weeks or over a 6-month period, until a maintenance dose of 5–10 mg·day−1 was reached, until relapse or the end of the study. Data on the duration of maintenance doses were unavailable. The immunosuppressive agents included cyclophosphamide, methotrexate, cyclosporin, azathioprine, mycophenolate mofetil and leflunomide. In two studies [23, 24], data on the chosen immunosuppressive agents were not provided. Antiarrhythmic drugs and classical cardiac treatment were given depending on study design and available data. In most cases, β-blockers, angiotensin-converting enzyme inhibitors, diuretics, digitalics and antiarrhythmic drugs were used. Treatment was prescribed individually and based on individual clinical and rhythmic findings, as were pacemakers or implantable cardioverter defibrillator devices.
Outcomes
CT alone
In 20 (95%) of the selected studies, 709 patients received CT. Nine studies (45%, n=351) provided data on relapses, representing an incidence of 34% (n=119) in patients who received CT alone (mean follow-up 15–118.8 months). Twelve studies (57%) did not provide clear data on relapses in the CT group. Only three studies (14%, n=73) provided data on MACEs (n=33), representing 45% of MACEs in patients treated by CT alone (mean follow-up 15–77.3 months).
ITs associated with CT
In nine (43%) of the selected studies, 155 patients received combined CT and IT. Only four studies (n=78) provided data on CS relapse, representing an incidence of 33% (n=26) in patients who received CT and IT (mean follow-up 39–66 months). Five studies did not provide clear data on relapse in this group. No study provided clear data on MACEs in patients who received combined CT and IT.
Relapses and MACEs
Data on MACEs and relapse rate are presented in table 3. Only one study [10] was designed to compare relapse rates between patients who received CT and CT+IT. Data on MACEs were not provided. Patients with cardiac relapse were more frequently male (p=0.052), less frequently black (p=0.008) and tended to be less frequently treated with IT (p=0.085). Frequency of cardiac relapse was lower in patients who received CT and IT at CS diagnosis than in patients who received CT alone (p=0.048). Among nine patients with severe cardiac relapse, seven (78%) received CT alone. MACEs were the chosen primary end-point in two studies [22, 27], indicating that MACEs during CS were significantly associated with initial presentation, including New York Heart Association class III or IV dyspnoea (p=0.024) and history of sustained VT or VF (p=0.002) [18, 36], and showing that the survival rate without MACEs was better in patients with a high degree of AVB as the initial presentation than in patients with VT and/or heart failure [27].
Cardiac or sudden death was the chosen primary end-point in three studies [17, 24, 29]. Myoren et al. [17] found that greater baseline urinary 8-hydroxy-2′-deoxyguanosine (p=0.020) and greater baseline B-natriuretic peptide (p=0.028) were significantly associated with cardiovascular-related death in multivariate analysis. Nagai et al. [24] investigated the effect of CT discontinuation on cardiac death. In this study, the continuation group had significantly better survival than the discontinuation group (p=0.035) with a maintenance CT dose of 5–10 mg·day−1 after nearly 10 years’ mean follow-up. Yazaki et al. [29] found significantly better survival if patients had a baseline left ventricular ejection fraction (LVEF) ≥50% (p<0.001). Nagai et al. [23] found that CT at diagnosis was the only multivariate negative predictive factor for all-cause death, or hospitalisation for heart failure or symptomatic arrhythmias.
Adverse drug events
Available data on adverse drug events were scarce. Only four studies (19%, n=156) provided data on adverse events under CT alone or combined with IT. Ballul et al. [10] provided adverse event data by treatment group, and no difference was found in infection rates between CT and CT+IT groups.
Discussion
In this study, we investigated the current literature on conventional CT and IT for CS. Reviews and expert consensus consider that LV dysfunction, arrhythmias and prevention of sudden cardiac death in CS should be managed in the same way as in patients without CS, following national and international recommendations [8, 13]. Treatment of LV dysfunction is based on angiotensin receptor II blockers, aldosterone inhibitors and diuretics. β-blockers should be used prudently owing to the risk of severe AVB in some cases. Severe AVB should be detected as soon as possible in the course of CS so that patients can benefit from cardiac device implantation (pacemaker) [37], even before IT. In refractory VA, mapping and radiofrequency ablation might be effective in some cases [38, 39].
Corticosteroids are the mainstay treatment of CS and can notably improve outcomes for recurrent LVEF, AVB and VA [26, 30], or imaging extension of the disease [40]. CT dose and duration remain unclear. In a Japanese cohort, there was no impact on outcomes between high versus low starting dose of CT [29]. Padala et al. [26] emphasised the necessity of early CT initiation after CS diagnosis. Yodogawa et al. [41] described less ventricular extrasystole and VT after CT in patients with LVEF ≥35%. In our systematic review, different initial doses and tapering regimens were used. Some studies used prednisone 20–60 mg·day−1 as the initial dose, tapered over a period of 6 weeks to 12 months up to a maintenance dose of 5–10 mg·day−1, without data on CT duration and heterogeneous CT regimens. Nonetheless, all these data taken together emphasise the importance of early initiation of CT after CS diagnosis, before the establishment of myocardial scars and worsening LVEF.
This systematic review reveals that IT is used in accordance with the design of the study concerned, analogous to extracardiac sarcoidosis. Indications for IT are generally for corticosteroid sparing, more severe clinical presentation at diagnosis or add-on therapy when relapse occurs. Only a few studies used combined IT and CT [10, 11, 20, 34] in a pre-specified method. The most-used immunosuppressant was methotrexate. Ballul et al. [10] found lower survival, although not significant, without relapse in the IT group, whereas IT combined with CT at CS diagnosis was significantly associated with fewer relapses than using CT alone. Nagai et al. [34] compared low-dose CT (5–15 mg·day−1) to low-dose CT associated with methotrexate (6 mg·week−1). LVEF was significantly better at 3 years’ follow-up in the methotrexate group (44.5±13.8% versus 60.7±14.3%) but not at 5 years’ follow-up (45.7±15.5% versus 53.6±13.3%). Ten studies (48%) stated use of IT in reported patients; only nine studies gave data on patients treated by IT and four studies indicated relapse rate under IT. No data on MACEs were provided in any study using IT. Only one study [10] provided comparative data on adverse events in patients receiving CT alone and in combination with IT, and there was no significant difference. In this systematic review, we found a similar rate of relapse in patients receiving CT alone (34%) and combined with IT (33%) but the two groups could not be compared. However, it was not possible to draw any conclusions on those rates due to the heterogeneity of the study design, follow-up, treatment schemes, different end-points and missing data. For these reasons, reliable meta-analysis on CS treatments is impossible. There is a clear lack of long-term outcomes in CS, which is an unpredictable disease.
In the literature, methotrexate seems to be the first-choice immunosuppressant for extracardiac sarcoidosis, and as second-line treatment in steroid-refractory cases or in the presence of steroid-associated adverse events in WASOG recommendations (2b level of evidence) [42]. In 2013, Vorselaars et al. [43] published a retrospective case–control study that compared methotrexate and azathioprine for steroid-sparing effect, pulmonary function and adverse effects as second-line treatment of pulmonary sarcoidosis. They found similar significant steroid sparing and adverse effects, except for a higher infection rate with azathioprine, in a 1-year follow-up study. To our knowledge, there is no study providing such information for CS.
In our systematic review, only 11 studies provided relapse rates, and only two established MACEs as a clear end-point, which might underestimate the relapse rate and MACEs in CS.
Recently, cohort studies were published on TNF-α antagonist use in refractory CS cases after CT and IT failure. In these cohorts, adalimumab suppressed fluorodeoxyglucose uptake on positron emission tomography [44] in 66% of responders under infliximab therapy in 36 patients refractory to CT and IT [12], and there was a corticosteroid sparing effect with adalimumab or infliximab without worsening of LVEF [45]. No data are published in early therapy of CS with TNF-α antagonists.
Several limitations must be mentioned. No randomised control trial was found, only one study was prospective and most studies took place in Japanese centres. These limitations prevent us from extrapolating recommendations to Western European countries and Caucasian patients because CS presentation can show ethnic and national differences [3]. The lack of prospective or randomised control trials could largely be explained by the urgent need for treatment when CS is diagnosed and the scarcity of CS in each centre. There were only cohort studies with fair quality according to the SIGN rating. Another limitation was the heterogeneity of the end-points, which did not allow comparison between outcomes. Strong end-points, such as relapse and MACEs, were selected in only three studies [10, 22, 24] and some studies were excluded based on imaging changes and because they did not provide sufficient data on end-points such as relapse or MACEs. Heterogeneous treatment regimens and a lack of data made it difficult to interpret the immunosuppressive effects on CS disease course, steroid sparing and comparison between CT alone and in combination with IT. Finally, data on adverse drug events were provided in only four studies, making comparison difficult between CT and IT in terms of safety.
Taking into account these results, and the potential life-threatening issues in CS, we suggest an early CT of 0.5–1 mg·kg−1·day−1 with a 3–6 months tapering scheme in case of clinical and imaging remission, and an adjunctive therapy with a steroid-sparing agent such as methotrexate at usual dose. We cannot clearly select patients who will most benefit from IT; therefore, IT prescription should be wide and adapted to each patient's conditions.
Patients’ follow-up should be based on initial presentation (cardiac failure and/or rhythmic presentation), and further studies should split patients into groups upon their initial presentation based on function and rhythm.
Recently, studies on TNF-α antagonists have shown interesting outcomes in patients with resistant or relapsing CS [12, 44–47]. Further studies, including comparative groups between CT-, IT- and TNF-α antagonist-treated patients, are needed to clarify which treatment schemes could be recommended.
Conclusion
Currently, CS is a life-threatening condition and treatment is based on corticosteroids, which should be administered as soon as possible after the diagnosis of cardiac involvement in sarcoidosis. Conventional IT as add-on therapy or a steroid-sparing agent seems to have a good tolerance profile and safety, but its efficacy on outcomes in terms of relapse rate and major cardiac events is not clear. Heterogeneity in study design prevents us from making any clear recommendations. Further studies with homogenous groups, comparisons between the different treatments schemes and with reproducible strong end-points are needed.
Supplementary material
Supplementary Material
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Search strategy ERJ-00449-2021.Supplement_1
SIGN checklist ERJ-00449-2021.Supplement_2
Supplementary table S1 ERJ-00449-2021.Table
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Supplementary Material
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Shareable PDF ERJ-00449-2021.Shareable
Acknowledgements
We thank Bruno Pereira for his advice on this work.
Footnotes
This article has supplementary material available from erj.ersjournals.com
The datasets obtained and/or analysed during the current study are available from the corresponding author on reasonable request.
Conflict of interest: J. Stievenart has nothing to disclose.
Conflict of interest: G. Le Guenno has nothing to disclose.
Conflict of interest: M. Ruivard has nothing to disclose.
Conflict of interest: V. Rieu has nothing to disclose.
Conflict of interest: M. André has nothing to disclose.
Conflict of interest: V. Grobost has nothing to disclose.
- Received February 12, 2021.
- Accepted August 26, 2021.
- Copyright ©The authors 2022.
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