Predictive Value of Classical and Emerging Autoantibodies for Cardiac Dysfunction in Systemic Sclerosis: Systematic Review
Abstract
1. Introduction
2. Methods
2.1. Protocol, Registration and Criteria
- Enrolled adult patients diagnosed with SSc based on American College of Rheumatology/European League Against Rheumatism (ACR/EULAR) criteria [18];
- Reported cardiac involvement (e.g., myocardial fibrosis, arrhythmias, conduction abnormalities, left ventricular (LV) dysfunction);
- Assessed classical or emerging autoantibodies (e.g., anti-centromere antibodies [ACA], anti-topoisomerase I antibodies [anti-Scl-70], anti-RNA polymerase III [anti-RNAP III], anti-U3 ribonucleoprotein [anti-U3 RNP], anti-heart antibodies [AHA], anti-intercalated disk antibodies [AIDA]);
- Used imaging (e.g., cardiac magnetic resonance [CMR], echocardiography) or biomarker-based methods (e.g., N-terminal pro-brain natriuretic peptide [NT-proBNP], troponin) for cardiac assessment.
- Non-human studies, editorials, and conference abstracts.
2.2. Information Sources
- PubMed
- Web of Science
- Scopus
- Cochrane Library
2.3. Search Strategy and Study Selection
2.4. Data Collection Process
- Study design and setting;
- Sample size and demographics;
- Diagnostic criteria for SSc;
- Autoantibody types and titers;
- Cardiac outcome measures (e.g., fibrosis, LV dysfunction, arrhythmias);
- Imaging and biomarkers used;
- Main findings and statistical associations.
2.5. Risk of Bias Assessment
2.6. Synthesis of Results and Assessment of Evidence Quality
3. Results
3.1. Study Selection
3.2. Study Characteristics and Quality Assessment
4. Pathogenesis of Primary Cardiac Involvement in SSc
5. Autoantibodies and Cardiac Manifestations in SSc
5.1. Anticentromere Antibodies
5.2. Anti-Topoisomerase I Antibodies
5.3. Emerging Autoantibodies and Cardiac Manifestations in SSc
5.4. Associations Between Autoantibody Profiles and Cardiac Outcomes
6. Future Research Directions
7. Conclusions
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Conflicts of Interest
Abbreviations
ACA | anti-centromere antibodies |
ACR/EULAR | American College of Rheumatology/European League Against Rheumatism |
AHA | anti-heart antibodies |
AIDA | anti–intercalated disk antibodies |
Anti-NOR90 | anti–nucleolar organizing region 90 antibodies |
anti-Mi2 | antibodies targeting Mi-2 helicase |
anti-PL-7 | anti–PL7 antibodies |
anti-PL12 | anti–PL-12 antibodies |
anti-PmScl | anti–Pm/Scl antibodies |
anti-RNAP III | anti–RNA polymerase III |
anti-Ro/SSA | anti–Ro/Sjögren’s-syndrome-related antigen A antibodies |
anti-Scl-70 | anti–topoisomerase I antibodies |
anti-U1 RNP | anti–U1 ribonucleoprotein antibodies |
anti-U3 RNP | anti–U3 ribonucleoprotein |
AV | atrioventricular |
CMR | cardiac magnetic resonance |
CPET | cardiopulmonary exercise testing |
CTGF | connective tissue growth factor |
CV | cardiovascular |
dc | diffuse cutaneous |
DLCO | diffusing capacity of the lungs for carbon monoxide |
DNA | deoxyribonucleic acid |
ECG | Electrocardiographic |
EndMT | endothelial-to-mesenchymal transition |
EUSTAR | European League Against Rheumatism Scleroderma Trials and Research |
FRS | Framingham Risk Score |
HFA | Heart Failure Association |
IL | interleukin |
ILD | interstitial lung disease |
IRR | incidence rate ratio |
lc | limited cutaneous |
LGE | late gadolinium enhancement |
LV | left ventricular |
LVDD | left ventricular diastolic dysfunction |
microRNA | micro-ribonucleic acid |
NOS | Newcastle–Ottawa Scale |
NT-proBNP | N-terminal pro–brain natriuretic peptide |
PAH | pulmonary arterial hypertension |
PDGF | platelet-derived growth factor |
PRISMA | Preferred Reporting Items for Systematic Reviews and Meta-Analyses |
PVCs | premature ventricular contractions |
RNA | ribonucleic acid |
RP | Raynaud’s phenomenon |
RSS | Reynolds Risk Score |
SCORE | Systematic Coronary Risk Evaluation |
SSc | systemic sclerosis |
SSc-pHI | SSc-primary cardiac involvement |
TGF-β | transforming growth factor-beta |
WSF | World Scleroderma Foundation |
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Study (First Author, Year) | Reference No. | Study Design | NOS Score | Risk of Bias |
---|---|---|---|---|
Bairkdar et al., 2024 | [4] | Cohort | 9 | Low |
Muresan et al., 2016 | [7] | Cohort | 7 | Low |
Tzelepis et al., 2007 | [11] | Cohort | 8 | Low |
Allanore et al., 2010 | [20] | Cohort | 9 | Low |
Höppner et al., 2023 | [21] | Cross-sectional Observational | 9 | Low |
Radwan et al., 2021 | [22] | Cohort | 8 | Low |
Lopez Nunez et al., 2023 | [23] | Cross-sectional | 8 | Low |
Avouac et al., 2015 | [24] | Cohort | 8 | Low |
Dumitru et al., 2021 | [25] | Cohort | 8 | Low |
Cusma Piccione et al., 2013 | [26] | Cohort | 7 | Low |
Barison et al., 2015 | [27] | Cross-sectional observational | 7 | Low |
Hachulla et al., 2009 | [28] | Cohort | 7 | Low |
Krumm et al., 2016 | [29] | Cross-sectional cohort | 7 | Low |
Kobayashi et al., 2009 | [30] | Cohort | 7 | Low |
Hui et al., 2021 | [31] | Cohort | 7 | Low |
Vacca et al., 2014 | [32] | Cohort | 7 | Low |
D’Andrea et al., 2004 | [33] | Cohort | 6 | Moderate |
Autoantibody | Associated Cardiac Manifestations | Clinical Utility |
---|---|---|
Anti-centromere (ACA) | Conduction abnormalities, arrhythmias (esp. in older adults); potential risk of PAH | Common marker for lcSSc; useful for PAH risk but limited in predicting fibrosis |
Anti-topoisomerase I (anti-Scl-70) | Myocardial fibrosis, diastolic dysfunction, elevated NT-proBNP and troponin, arrhythmias | High-risk marker for early cardiac fibrosis and dysfunction; strong clinical relevance |
Anti-RNA polymerase III | Pericardial effusion, arrhythmias, potential tamponade | Predictive for scleroderma renal crisis and cardiac effusion |
Anti-U3 RNP (anti-fibrillarin) | Myocardial fibrosis, conduction system disease, pericarditis (especially in African-American patients) | Ethnic-specific marker (African-American); strong indicator of cardiac involvement |
Anti-Ku/Anti-Histone | Increased risk of heart disease | Supportive marker; less specific |
Anti-Th/To | Greater association with pericarditis compared to ACA | More specific than ACA for pericardial involvement |
AHA/AIDA | Potential myocardial specificity; associated with cardiac fibrosis | Emerging biomarkers; require further validation |
Anti-U1 RNP | Mild conduction system disease; may coexist with PAH and overlap syndromes | Overlap syndromes (e.g., MCTD); cardiac risk less well-defined |
Anti-PmScl | Occasional myocardial involvement; more often linked with myositis-overlap | Useful in overlap syndrome diagnostics; less specific for cardiac disease |
Anti-Ro/SSA | Occasionally pericardial effusion; mostly linked with systemic autoimmune overlap | Non-specific marker; may aid in overlap diagnosis |
Anti-PL7/PL12 | Rarely cardiac involvement; more associated with inflammatory myopathy | More relevant in ILD and myositis; cardiac links unclear |
Anti-NOR90 | Limited evidence for direct cardiac involvement | Rare; not clinically routine for cardiac screening |
Anti-Mi-2 | Primarily associated with dermatomyositis; occasional myocardial fibrosis | Muscle-specific; used in differential diagnosis with myositis-cardiac overlap |
Autoantibody | Strength of Evidence for Cardiac Involvement |
---|---|
Anti–Scl-70 | High |
ACA | Moderate |
Anti–RNAP III | Moderate |
Anti–U3 RNP | Moderate |
AHA/AIDA | Preliminary |
Others (Ku, histone, Th/To, U1 RNP, PmScl, Ro/SSA, PL7/PL12, NOR90, Mi-2) | Low to minimal |
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Radić, M.; Bečić, T.; Šimac, P.; Đogaš, H.; Jukić, I.; Fabijanić, D.; Radić, J. Predictive Value of Classical and Emerging Autoantibodies for Cardiac Dysfunction in Systemic Sclerosis: Systematic Review. J. Clin. Med. 2025, 14, 6383. https://doi.org/10.3390/jcm14186383
Radić M, Bečić T, Šimac P, Đogaš H, Jukić I, Fabijanić D, Radić J. Predictive Value of Classical and Emerging Autoantibodies for Cardiac Dysfunction in Systemic Sclerosis: Systematic Review. Journal of Clinical Medicine. 2025; 14(18):6383. https://doi.org/10.3390/jcm14186383
Chicago/Turabian StyleRadić, Mislav, Tina Bečić, Petra Šimac, Hana Đogaš, Ivana Jukić, Damir Fabijanić, and Josipa Radić. 2025. "Predictive Value of Classical and Emerging Autoantibodies for Cardiac Dysfunction in Systemic Sclerosis: Systematic Review" Journal of Clinical Medicine 14, no. 18: 6383. https://doi.org/10.3390/jcm14186383
APA StyleRadić, M., Bečić, T., Šimac, P., Đogaš, H., Jukić, I., Fabijanić, D., & Radić, J. (2025). Predictive Value of Classical and Emerging Autoantibodies for Cardiac Dysfunction in Systemic Sclerosis: Systematic Review. Journal of Clinical Medicine, 14(18), 6383. https://doi.org/10.3390/jcm14186383