Scientific Sessions 2025  /  Cardiovascular Metabolism and Myocardial Remodeling  /  Mitochondrial DNA Copy Number (mtDNA-CN): Associations with Mortality and Gene Expression in the International Study of Comparative Health Effectiveness with Medical and Invasive Approaches (ISCHEMIA) Biorepository
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Final ID: MP2747

Mitochondrial DNA Copy Number (mtDNA-CN): Associations with Mortality and Gene Expression in the International Study of Comparative Health Effectiveness with Medical and Invasive Approaches (ISCHEMIA) Biorepository

Abstract Body (Do not enter title and authors here): Introduction: Higher mtDNA-CN reflects better mitochondrial function, while lower levels indicate mtDNA release and increased inflammation. Although mtDNA-CN serves as a marker of cardiovascular health, the importance and mechanism of risk associated with mtDNA in high-risk individuals with chronic coronary artery disease (CAD) remains poorly understood. To address this gap, we leveraged the ISCHEMIA Biorepository to: (1) evaluate the association between mtDNA-CN and all-cause death (ACD); and (2) define a transcriptomic profile associated with high mtDNA-CN and ACD risk for high-risk patients with CAD.

Hypothesis: Higher mtDNA-CN is associated with reduced ACD risk and inflammation in high-risk patients enrolled in the ISCHEMIA Biorepository.

Methods: Low pass whole genome sequencing and whole blood RNA-Seq were performed on 594 ISCHEMIA and ISCHEMIA-CKD participants with moderate-severe ischemia. Data were processed using the NYU deciphEHR pipeline and mtDNA was quantified using mitoAnalyzer. mtDNA-CN was median split, with samples having values ≤ median classified as the 'low' group and those > median as the 'high' group. Unadjusted group differences were assessed using Chi-squared tests. Survival analysis was performed using Cox proportional hazard models, adjusted for age, sex, diabetes, eGFR, dialysis status, ischemia severity, and left ventricular ejection fraction. Adjusted differential gene expression (DGE) and gene set enrichment analysis (GSEA) were performed to explore molecular mechanisms underlying mtDNA-CN.

Results: Median age was 67 (IQR: 57–78); 19% were female, 84% white, and 6% Hispanic. Hypertension (84%), diabetes (43%), and obesity (45%) were common; 26% had eGFR <60 mL/min/1.73 m2. Median mtDNA-CN was 153 counts per sample. After multivariate adjustment, mtDNA-CN > median was associated with a 48% reduction in ACD (aHR = 0.52, 95% CI: 0.30–0.90; P = 0.020) (Figure 1A). DGE revealed downregulation of inflammatory genes in the mtDNA-CN group, including S100A9 (FC=-.41, p=3.32e-10) and S100A12 (FC=-.56, p=3.32e-10). Inflammatory pathways such as the inflammasome complex (NES=-2.17, p=9.32e-03) and interleukin-1 production (NES= -2.02, p=6.60e-03) were downregulated among participants in the high mtDNA-CN (Figure 1B).

Conclusion: Higher mtDNA-CN is associated with lower risk of ACD and reduced inflammasome activity, suggesting that enhanced mitochondrial health may mitigate inflammasome-related pathology linked to ACD in patients with CAD.
  • Amsalem, Jonathan  ( NEW YORK UNIVERSITY MEDICAL CENTER , New York , New York , United States )
  • Hochman, Judith  ( NYU GROSSMAN SCHOOL OF MEDICINE , New York , New York , United States )
  • Maron, David  ( STANFORD UNIVERSITY , Palo Alto , California , United States )
  • Ruggles, Kelly  ( NYU Grossman School of Medicine , New York , New York , United States )
  • Berger, Jeffrey  ( New York University School Med , New York , New York , United States )
  • Newman, Jonathan  ( NEW YORK UNIVERSITY MEDICAL CENTER , New York , New York , United States )
  • Muller, Matthew  ( NEW YORK UNIVERSITY MEDICAL CENTER , New York , New York , United States )
  • Held, Claes  ( Uppsala Clinical Research Center , Uppsala , Sweden )
  • Kullo, Iftikhar  ( MAYO CLINIC , Rochester , Minnesota , United States )
  • Mcmanus, Bruce  ( University of British Columbia , Vancouver , British Columbia , Canada )
  • Wallentin, Lars  ( UPPSALA CLINICAL RESEARCH CENTRE , Uppsala , Sweden )
  • Newby, L. Kristin  ( Duke Clinical Research Institute , Durham , North Carolina , United States )
  • Bangalore, Sripal  ( NEW YORK UNIVERSITY SCHOOL OF MED , New York , New York , United States )
  • Reynolds, Harmony  ( NYU GROSSMAN SCHOOL MEDICINE , New York , New York , United States )
    • Author Disclosures:
    Jonathan Amsalem: DO NOT have relevant financial relationships | Judith Hochman: DO have relevant financial relationships ; Research Funding (PI or named investigator):NIH/NHLBI:Active (exists now) ; Research Funding (PI or named investigator):NIH/NHLBI:Past (completed) ; Research Funding (PI or named investigator):NIH/NEI:Past (completed) ; Research Funding (PI or named investigator):NIH/NHLBI:Past (completed) ; Research Funding (PI or named investigator):NHLBI – RTI:Past (completed) ; Research Funding (PI or named investigator):NIH/NHLBI:Active (exists now) | David Maron: DO have relevant financial relationships ; Advisor:New Amsterdam:Past (completed) ; Individual Stocks/Stock Options:Ablative Solutions:Active (exists now) ; Consultant:Inno Med:Past (completed) ; Consultant:Scilex:Past (completed) ; Independent Contractor:J&J:Active (exists now) ; Consultant:Regeneron:Past (completed) ; Consultant:Hearlflow:Active (exists now) ; Research Funding (PI or named investigator):Omada Health:Active (exists now) ; Research Funding (PI or named investigator):Cleerly:Active (exists now) | Kelly Ruggles: No Answer | Jeffrey Berger: DO NOT have relevant financial relationships | Jonathan Newman: DO NOT have relevant financial relationships | Matthew Muller: No Answer | Claes Held: No Answer | Iftikhar Kullo: DO NOT have relevant financial relationships | Bruce McManus: No Answer | Lars Wallentin: DO NOT have relevant financial relationships | L. Kristin Newby: DO have relevant financial relationships ; Research Funding (PI or named investigator):Roche Diagnostics:Past (completed) ; Other (please indicate in the box next to the company name):Boehringer Ingelheim; editorial support for publications:Active (exists now) ; Consultant:BMS:Past (completed) ; Consultant:Medtronic:Active (exists now) ; Research Funding (PI or named investigator):Medtronic:Past (completed) | Sripal Bangalore: DO have relevant financial relationships ; Consultant:Abbott Vascular:Active (exists now) ; Consultant:Recor:Active (exists now) ; Consultant:Shockwave:Active (exists now) ; Consultant:Imperative Care:Active (exists now) ; Consultant:Inari:Active (exists now) ; Consultant:Boston Scientific:Active (exists now) | Harmony Reynolds: DO have relevant financial relationships ; Other (please indicate in the box next to the company name):National Heart, Lung and Blood Institute Grants:Active (exists now) ; Other (please indicate in the box next to the company name):SHL Telemedicine- non-financial support:Active (exists now) ; Other (please indicate in the box next to the company name):Philips- non-financial support:Active (exists now) ; Other (please indicate in the box next to the company name):Siemens- non-financial support:Active (exists now) ; Other (please indicate in the box next to the company name):Abbott Vascular- non-financial support:Active (exists now)
Meeting Info:

Scientific Sessions 2025

2025

New Orleans, Louisiana

Session Info:

Cardiovascular Metabolism and Myocardial Remodeling

Monday, 11/10/2025 , 09:15AM - 10:15AM

Moderated Digital Poster Session

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