- Hammadah, Muhammad;
- Al Mheid, Ibhar;
- Wilmot, Kobina;
- Ramadan, Ronnie;
- Abdelhadi, Naser;
- Alkhoder, Ayman;
- Obideen, Malik;
- Pimple, Pratik M;
- Levantsevych, Oleksiy;
- Kelli, Heval M;
- Shah, Amit;
- Sun, Yan V;
- Pearce, Brad;
- Kutner, Michael;
- Long, Qi;
- Ward, Laura;
- Ko, Yi-An;
- Hosny Mohammed, Kareem;
- Lin, Jue;
- Zhao, Jinying;
- Bremner, J Douglas;
- Kim, Jinhee;
- Waller, Edmund K;
- Raggi, Paolo;
- Sheps, David;
- Quyyumi, Arshed A;
- Vaccarino, Viola
Rationale
Leukocyte telomere length (LTL) is a biological marker of aging, and shorter LTL is associated with adverse cardiovascular outcomes. Reduced regenerative capacity has been proposed as a mechanism. Bone marrow-derived circulating progenitor cells are involved in tissue repair and regeneration.Objective
Main objective of this study was to examine the relationship between LTL and progenitor cells and their impact on adverse cardiovascular outcomes.Methods and results
We measured LTL by quantitative polymerase chain reaction in 566 outpatients (age: 63±9 years; 76% men) with coronary artery disease. Circulating progenitor cells were enumerated by flow cytometry. After adjustment for age, sex, race, body mass index, smoking status, and previous myocardial infarction, a shorter LTL was associated with a lower CD34+ cell count: for each 10% shorter LTL, CD34+ levels were 5.2% lower (P<0.001). After adjustment for the aforementioned factors, both short LTL (ConclusionsAlthough shorter LTL is associated with decreased regenerative capacity, both LTL and circulating progenitor cell levels are independent and additive predictors of adverse cardiovascular outcomes in coronary artery disease patients. Our results suggest that both biological aging and reduced regenerative capacity contribute to cardiovascular events, independent of conventional risk factors.