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We thank Campochiaro et al for their interesting comment1 on our work in which we used hierarchical clustering on principal components to define clinically meaningful subgroups of patients with anti-Ku antibodies.2
Among a bi-centric cohort of patients with systemic sclerosis (SSc), Campochiaro et al identified four patients with anti-Ku and retrospectively reviewed these cases.
All patients had increased creatine kinase (CK), three (75%) of whom had interstitial lung disease (ILD). These findings support our observations according to which anti-Ku patients with elevated CK are at risk of ILD.
Of particular interest, Campochiaro et al proposed that myocarditis could further represent a specific feature of anti-Ku patients with elevated CK given that all of their four anti-Ku SSc patients had cardiac magnetic resonance (CMR) imaging established myocarditis according to Lake Louise criteria. Two (50%) had heart failure while the remaining two had subclinical presentation. By contrast, in our cohort, one anti-Ku patient had heart failure with positive CMR (2% of all anti-Ku patients and 7% of anti-Ku patients with elevated CK).
Comparability between the Campochiaro et al’s study and our study is limited however since: (1) Campochiaro et al studied patients with SSc and all of their anti-Ku patients were diagnosed with myositis. The association of these two conditions has been associated with a high risk of myocarditis per se.3 4 By contrast, only two (5%) of our anti-Ku patients fulfilled the ACR/EULAR criteria for SSc and only one also fulfilled the EULAR/ACR criteria for myositis; (2) Campochiaro et al performed CMR in all patients with increased serum troponin T levels, an enzyme whose serum level is increased in myositis patients irrespectively of the presence of myocarditis.5 By opposition, our patients underwent CMR only when clinical signs of myocarditis were present.
To further address the interesting point raised by Campochiaro et al, we conducted an extensive review of the literature. The inclusion criteria were original articles in English pertaining to anti-Ku in which cardiac manifestations were defined and prevalence was directly mentioned or easily calculated from the available data. Pubmed and Web of Science were searched using ‘anti-Ku’, ‘auto-antibodies’, ‘myositis’, ‘systemic sclerosis’ and ‘myocarditis’. Reference lists of relevant papers were also reviewed. Results and ensuing meta-analysis are shown in table 1.
Nine articles were included, reporting the prevalence of cardiac involvement in a total of 198 anti-Ku patients with huge variations (0% to 100%). The meta-analysed prevalence of cardiac involvement in anti-Ku patients was 23% (95% CI 9% to 46%). A significant heterogeneity was also found (p<0.001), likely resulting from the heterogeneous screening and definition used for cardiac involvement; and/or from the heterogeneity of the studied populations.
Five studies were controlled (representing a total of 76 anti-Ku patients vs 435 anti-Ku negative patients). The meta-analysed risk of cardiac involvement was not significantly increased in anti-Ku patients vs anti-Ku negative patients (OR 1.60 (95% CI 0.66 to 3.87)).
The important comments of the Campochiaro et al study together with the above data highlight several crucial unmet needs for myocarditis in connective tissue diseases patients, namely:
There is no widely accepted definition of cardiac involvement. Notably, the authors of the Lake Louise criteria warned that CMR criteria for myocarditis are based on expert consensus in light of the limited evidence of its performance compared with endomyocardial biopsy.6
The screening strategies as well as definition for cardiac involvement are heterogeneous among centres.
There is a need for identifying biomarker(s) of cardiac involvement of which auto-antibodies could be useful toward this aim.
The prognosis of patients with subclinical CMR myocarditis is currently unknown and whether such patients benefit from increased immunomodulation (vs its potential risks for the patient) is unanswered.
Future research agendas should address these points.
Handling editor Josef S Smolen
Contributors LS, FS and AM: substantialy contribute to the conception and design of the work; or the acquisition, analysis and interpretation of data for the work; draft the work or revising it critically for important intellectual content; approve the final version to be published; agree to be accountable for all aspects of the work in ensuring that questions related to the accuracy or integrity of any part of the work are appropriately investigated and resolved.
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 None declared.
Patient consent for publication Not required.
Provenance and peer review Commissioned; internally peer reviewed.
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