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解析社区居住的老年墨西哥成年人中生物年龄与虚弱之间的关系。

Disentangling the relationship between biological age and frailty in community-dwelling older Mexican adults.

机构信息

Research Division, Instituto Nacional de Geriatría, Mexico City, Mexico.

Combined Study Program in Medicine, School of Medicine,, Universidad Nacional Autónoma de México, Mexico City, Mexico.

出版信息

Gac Med Mex. 2024;160(3):290-300. doi: 10.24875/GMM.24000115.

DOI:10.24875/GMM.24000115
PMID:39602606
Abstract

BACKGROUND

Older adults have highly heterogeneous aging rates.

OBJECTIVE

To explore the association of biological age (BA) and accelerated aging with frailty in community-dwelling older adults.

METHODS

We assessed 735 community-dwelling older adults from the Coyocan Cohort. BA was measured using AnthropoAge, accelerated aging with AnthropoAgeAccel, and frailty using Fried's phenotype and the frailty index. We explored the association of BA and accelerated aging (AnthropoAgeAccel ≥ 0) with frailty at baseline and characterized the body composition and physical function phenotype of accelerated aging in non-frail/frail participants. We also explored accelerated aging as a risk factor for frailty progression after 3-years of follow-up.

RESULTS

Older adults with accelerated aging have higher frailty prevalence and indices, lower handgrip strength and gait speed. AnthropoAgeAccel was associated with higher frailty indices (β = 0.0053, 95%CI 0.0027-0.0079), and increased odds of frailty at baseline (OR 1.16, 95%CI 1.09-1.25). We observed sex-based differences in body composition and physical function linked to accelerated aging in non-frail participants; however, these differences were absent in pre-frail/frail participants. Accelerated aging at baseline was associated with higher risk of frailty progression over time (OR 1.74, 95%CI 1.11-2.75).

CONCLUSIONS

Despite being intertwined, biological accelerated aging is largely independent of frailty in community-dwelling older adults.

摘要

背景

老年人的衰老速度存在高度异质性。

目的

探讨生物年龄(BA)和加速衰老与社区居住的老年人虚弱的关系。

方法

我们评估了来自 Coyocan 队列的 735 名社区居住的老年人。BA 使用 AnthropoAge 进行测量,加速衰老使用 AnthropoAgeAccel 进行测量,虚弱使用 Fried 的表型和虚弱指数进行测量。我们探讨了 BA 和加速衰老(AnthropoAgeAccel ≥ 0)与基线时虚弱的关系,并描述了非虚弱/虚弱参与者中加速衰老的身体成分和身体功能表型。我们还探讨了加速衰老作为 3 年随访后虚弱进展的危险因素。

结果

有加速衰老的老年人虚弱发生率和指数更高,握力和步速更低。AnthropoAgeAccel 与更高的虚弱指数(β = 0.0053,95%CI 0.0027-0.0079)和更高的基线虚弱几率(OR 1.16,95%CI 1.09-1.25)相关。我们观察到,在非虚弱参与者中,与加速衰老相关的身体成分和身体功能存在性别差异;然而,在虚弱参与者中则不存在这些差异。基线时的加速衰老与随着时间的推移虚弱进展的风险增加相关(OR 1.74,95%CI 1.11-2.75)。

结论

尽管相互交织,但生物加速衰老在社区居住的老年人中与虚弱基本独立。

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