Association between telomere length, frailty and death in older adults

被引:0
|
作者
Mariam El Assar
Javier Angulo
José A. Carnicero
Stefan Walter
Francisco J. García-García
Fernando Rodríguez-Artalejo
Leocadio Rodríguez-Mañas
机构
[1] Fundación de Investigación Biomédica del Hospital Universitario de Getafe,Centro de Investigación Biomédica en Red de Fragilidad y Envejecimiento Saludable (CIBERFES)
[2] Instituto de Salud Carlos III,Servicio de Histología
[3] Hospital Universitario Ramón y Cajal,Investigación, Unidad de Investigación Traslacional en Cardiología (IRYCIS
[4] Complejo Hospitalario de Toledo,UFV)
[5] Universidad Autónoma de Madrid/IdiPaz,Hospital Virgen del Valle
[6] CIBERESP,Department of Preventive Medicine and Public Health
[7] and IMDEA Food Institute,Servicio de Geriatría
[8] Hospital Universitario de Getafe,Division of Geriatric Medicine
[9] Hospital Universitario de Getafe,undefined
来源
GeroScience | 2021年 / 43卷
关键词
Ageing; Telomere; Functional decline; Frailty; Mortality; Biomarker;
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摘要
Frailty is considered a clinical marker of functional ageing. Telomere length (TL) has been proposed as a biomarker of biological age but its role in human ageing is controversial. The main aim of the study was to evaluate the longitudinal association of TL with incident frailty and mortality in two cohorts of Spanish community–dwelling older adults. TL was determined at baseline in blood samples from older adults included in Toledo Study for Healthy Aging and ENRICA cohorts while frailty was determined by frailty phenotype (FP) at baseline and at follow-up (3.5 years). Deaths occurring during follow-up were also recorded. Associations of TL with frailty and mortality were analysed by logistic regression with progressive adjustment. Data were separately analysed in the two cohorts and in all subjects by performing a meta-analysis. TL was not different between frail and non-frail subjects. Longer telomeres were not associated with lower risk of prevalent frailty. Similarly, TL at baseline failed to predict incident frailty (OR: 1.04 [0.88–1.23]) or even the development of a new FP criterion (OR: 0.97 [0.90–1.05]) at follow-up. Lack of association was also observed when analysing the development of specific FP criteria. Finally, while frailty at baseline was significantly associated with higher risk of death at follow-up (OR: 4.08 [1.97–8.43], p < 0.001), TL did not significantly change the mortality risk (OR: 1.05 [0.94–1.16]). Results show that TL does not predict incident frailty or mortality in older adults. This suggests that TL is not a reliable biomarker of functional age.
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页码:1015 / 1027
页数:12
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