Atrial Fibrillation and Clonal Hematopoiesis in TET2 and ASXL1

Seyedmohammad Saadatagah; Mohammadreza Naderian; Mesbah Uddin; Ozan Dikilitas; Abhishek Niroula; Art Schuermans; Elizabeth Selvin; Ron C Hoogeveen; Kunihiro Matsushita; Vijay Nambi; Bing Yu; Lin Yee Chen; Alexander G Bick; Benjamin L Ebert; Michael C Honigberg; Na Li; Amil Shah; Pradeep Natarajan; Iftikhar J Kullo; Christie M Ballantyne

doi:10.1001/jamacardio.2024.0459

Atrial Fibrillation and Clonal Hematopoiesis in TET2 and ASXL1

JAMA Cardiol. 2024 Apr 10:e240459. doi: 10.1001/jamacardio.2024.0459. Online ahead of print.

Authors

Seyedmohammad Saadatagah^{1

2}, Mohammadreza Naderian³, Mesbah Uddin⁴, Ozan Dikilitas^{3

5}, Abhishek Niroula^{5

6

7

8}, Art Schuermans^{4

5

9}, Elizabeth Selvin¹⁰, Ron C Hoogeveen¹, Kunihiro Matsushita¹⁰, Vijay Nambi^{1

11}, Bing Yu¹², Lin Yee Chen¹³, Alexander G Bick¹⁴, Benjamin L Ebert^{5

8

15

16

17}, Michael C Honigberg^{4

5

17}, Na Li¹, Amil Shah¹⁸, Pradeep Natarajan^{4

5

17}, Iftikhar J Kullo^{3

19}, Christie M Ballantyne¹

Affiliations

¹ Department of Medicine, Baylor College of Medicine, Houston, Texas.
² Center for Translational Research on Inflammatory Diseases, Baylor College of Medicine, Houston, Texas.
³ Department of Cardiovascular Medicine, Mayo Clinic, Rochester, Minnesota.
⁴ Cardiovascular Research Center, Massachusetts General Hospital, Boston.
⁵ Program in Medical and Population Genetics and Cardiovascular Disease Initiative, Broad Institute of Harvard and MIT, Cambridge, Massachusetts.
⁶ Department of Laboratory Medicine, Lund University, Lund, Sweden.
⁷ Institute of Biomedicine, SciLifeLab, University of Gothenburg, Gothenburg, Sweden.
⁸ Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, Massachusetts.
⁹ Faculty of Medicine, KU Leuven, Leuven, Belgium.
¹⁰ Department of Epidemiology, Johns Hopkins Bloomberg School of Public Health, Baltimore, Maryland.
¹¹ Department of Medicine, Michael E. DeBakey VA Medical Center, Veterans Affairs Hospital, Houston, Texas.
¹² Department of Epidemiology, Human Genetics and Environmental Sciences, School of Public Health, The University of Texas Health Science Center at Houston, Houston.
¹³ Department of Medicine, University of Minnesota, Minneapolis.
¹⁴ Department of Medicine, Vanderbilt University, Nashville, Tennessee.
¹⁵ Center for Prevention of Progression, Dana-Farber Cancer Institute, Boston, Massachusetts.
¹⁶ Howard Hughes Medical Institute, Boston, Massachusetts.
¹⁷ Department of Medicine, Harvard Medical School, Boston, Massachusetts.
¹⁸ Department of Medicine, University of Texas Southwestern, Dallas.
¹⁹ Gonda Vascular Center, Mayo Clinic, Rochester, Minnesota.

PMID: 38598228
PMCID: PMC11007653 (available on 2025-04-10)
DOI: 10.1001/jamacardio.2024.0459

Abstract

Importance: Clonal hematopoiesis of indeterminate potential (CHIP) may contribute to the risk of atrial fibrillation (AF) through its association with inflammation and cardiac remodeling.

Objective: To determine whether CHIP was associated with AF, inflammatory and cardiac biomarkers, and cardiac structural changes.

Design, setting, and participants: This was a population-based, prospective cohort study in participants of the Atherosclerosis Risk in Communities (ARIC) study and UK Biobank (UKB) cohort. Samples were collected and echocardiography was performed from 2011 to 2013 in the ARIC cohort, and samples were collected from 2006 to 2010 in the UKB cohort. Included in this study were adults without hematologic malignancies, mitral valve stenosis, or previous mitral valve procedure from both the ARIC and UKB cohorts; additionally, participants without hypertrophic cardiomyopathy and congenital heart disease from the UKB cohort were also included. Data analysis was completed in 2023.

Exposures: CHIP (variant allele frequency [VAF] ≥2%), common gene-specific CHIP subtypes (DNMT3A, TET2, ASXL1), large CHIP (VAF ≥10%), inflammatory and cardiac biomarkers (high-sensitivity C-reactive protein, interleukin 6 [IL-6], IL-18, high-sensitivity troponin T [hs-TnT] and hs-TnI, N-terminal pro-B-type natriuretic peptide), and echocardiographic indices.

Main outcome measure: Incident AF.

Results: A total of 199 982 adults were included in this study. In ARIC participants (4131 [2.1%]; mean [SD] age, 76 [5] years; 2449 female [59%]; 1682 male [41%]; 935 Black [23%] and 3196 White [77%]), 1019 had any CHIP (24.7%), and 478 had large CHIP (11.6%). In UKB participants (195 851 [97.9%]; mean [SD] age, 56 [8] years; 108 370 female [55%]; 87 481 male [45%]; 3154 Black [2%], 183 747 White [94%], and 7971 other race [4%]), 11 328 had any CHIP (5.8%), and 5189 had large CHIP (2.6%). ARIC participants were followed up for a median (IQR) period of 7.0 (5.3-7.7) years, and UKB participants were followed up for a median (IQR) period of 12.2 (11.3-13.0) years. Meta-analyzed hazard ratios for AF were 1.12 (95% CI, 1.01-1.25; P = .04) for participants with vs without large CHIP, 1.29 (95% CI, 1.05-1.59; P = .02) for those with vs without large TET2 CHIP (seen in 1340 of 197 209 [0.67%]), and 1.45 (95% CI, 1.02-2.07; P = .04) for those with vs without large ASXL1 CHIP (seen in 314 of 197 209 [0.16%]). Large TET2 CHIP was associated with higher IL-6 levels. Additionally, large ASXL1 was associated with higher hs-TnT level and increased left ventricular mass index.

Conclusions and relevance: Large TET2 and ASXL1, but not DNMT3A, CHIP was associated with higher IL-6 level, indices of cardiac remodeling, and increased risk for AF. Future research is needed to elaborate on the mechanisms driving the associations and to investigate potential interventions to reduce the risk.