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端粒长度作为生物年龄的标志物:现状、未解决问题及未来展望

Telomere Length as a Marker of Biological Age: State-of-the-Art, Open Issues, and Future Perspectives.

作者信息

Vaiserman Alexander, Krasnienkov Dmytro

机构信息

Laboratory of Epigenetics, D.F. Chebotarev Institute of Gerontology, Kyiv, Ukraine.

出版信息

Front Genet. 2021 Jan 21;11:630186. doi: 10.3389/fgene.2020.630186. eCollection 2020.

Abstract

Telomere shortening is a well-known hallmark of both cellular senescence and organismal aging. An accelerated rate of telomere attrition is also a common feature of age-related diseases. Therefore, telomere length (TL) has been recognized for a long time as one of the best biomarkers of aging. Recent research findings, however, indicate that TL can only allow a rough estimate of aging rate and can hardly be regarded as a clinically important risk marker for age-related pathologies and mortality. Evidence is obtained that other indicators such as certain immune parameters, indices of epigenetic age, etc., could be stronger predictors of the health status and the risk of chronic disease. However, despite these issues and limitations, TL remains to be very informative marker in accessing the biological age when used along with other markers such as indices of homeostatic dysregulation, frailty index, epigenetic clock, etc. This review article is aimed at describing the current state of the art in the field and at discussing recent research findings and divergent viewpoints regarding the usefulness of leukocyte TL for estimating the human biological age.

摘要

端粒缩短是细胞衰老和机体老化的一个众所周知的标志。端粒损耗加速也是与年龄相关疾病的一个常见特征。因此,端粒长度(TL)长期以来一直被认为是衰老的最佳生物标志物之一。然而,最近的研究结果表明,TL只能对衰老速率进行粗略估计,很难被视为与年龄相关的病理和死亡率的临床重要风险标志物。有证据表明,其他指标,如某些免疫参数、表观遗传年龄指数等,可能是健康状况和慢性病风险的更强预测指标。然而,尽管存在这些问题和局限性,当与其他标志物如内稳态失调指数、衰弱指数、表观遗传时钟等一起使用时,TL在评估生物年龄方面仍然是一个非常有信息量的标志物。这篇综述文章旨在描述该领域的当前技术水平,并讨论关于白细胞TL用于估计人类生物年龄的有用性的最新研究结果和不同观点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/999b/7859450/981b06da9070/fgene-11-630186-g0001.jpg

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