Telomere Shortening & Metabolic/vascular Diseases

Overview

Journal Indian J Med Res

Specialty General Medicine

Date 2007 May 15

PMID 17496367

Citations 20

Authors

M Balasubramanyam

A Adaikalakoteswari

S Finny Monickaraj

V Mohan

Affiliations

Soon will be listed here.

Abstract

Telomeres are specialized DNA-protein structures located at the ends of eukaryotic chromosomes whose length is progressively reduced in most somatic cells during ageing. Over the past decade, emerging evidence has shown that the telomeres are essential regulators of cellular life span and chromosome integrity in a dynamic fashion. By inducing genomic instability, replicative senescence and apoptosis, shortening of telomeres is thought to contribute to organismal ageing. While the aetiology of cardiovascular diseases and diabetes represent a complex interaction between various risk factors overlaid on different genetic backgrounds, the conventional risk factors often did not explain the inter-individual variability related to predisposition of disease states. This underscores the need for biological indicators of ageing in evaluating the aetiology of several age-related disorders, and recent studies indicate that telomere length could qualify as an ideal marker of biological ageing. Short telomeres have been detected in senescent endothelial cells and vascular smooth muscle cells from human atherosclerotic plaque as well as in myocardial tissue from patients with end-stage heart failure and cardiac hypertrophy. In addition, telomere shortening has been demonstrated in WBCs from patients with coronary heart disease, premature myocardial infarction, hypertension and diabetes mellitus. In this review, we discuss the telomere hypothesis of ageing as well as human studies that address the role of telomeres in cardiovascular, diabetes and other cardio-metabolic pathologies.

Citing Articles

Conventional Risk Factors, Telomere Length, and Ischemic Heart disease: Insights into the Mediation Analysis.

Piplani S, Prabhu M, Alemao N, Akash C, Ram P, Ambar S Genome Integr. 2021; 12:1.

PMID: 34221339 PMC: 8230014. DOI: 10.4103/genint.genint_1_21.

Altered circulatory levels of miR-128, BDNF, cortisol and shortened telomeres in patients with type 2 diabetes and depression.

Prabu P, Poongothai S, Shanthirani C, Anjana R, Mohan V, Balasubramanyam M Acta Diabetol. 2020; 57(7):799-807.

PMID: 32025863 DOI: 10.1007/s00592-020-01486-9.

Association of rs1333040 SNPs with susceptibility, risk factors, and clinical characteristics of acute myocardial infarction patients in a Chinese Han population.

Huang D, Chen Q, Wang W, Huang Z, Li T, Li J Int J Clin Exp Pathol. 2020; 11(2):727-738.

PMID: 31938159 PMC: 6958057.

Influence of rs1746048 SNPs on clinical manifestations and incidence of acute myocardial infarction in Guangxi Han population.

Wang F, Wang W, Qin S, Chen Q, Huang Z, Huang D Int J Clin Exp Pathol. 2020; 12(1):282-294.

PMID: 31933744 PMC: 6944007.

The individual's signature of telomere length distribution.

Toupance S, Villemonais D, Germain D, Gegout-Petit A, Albuisson E, Benetos A Sci Rep. 2019; 9(1):685.

PMID: 30679552 PMC: 6345926. DOI: 10.1038/s41598-018-36756-8.