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Telomere length measurement as a clinical biomarker of aging and disease

机译:端粒长度测量作为衰老和疾病的临床生物标志物

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摘要

Telomere length measurement is increasingly recognized as a clinical gauge for age-related disease risk. There are several methods for studying blood telomere length (BTL) as a clinical biomarker. The first is an observational study approach, which directly measures telomere lengths using either cross-sectional or longitudinal patient cohorts and compares them to a population of age- and sex-matched individuals. These direct traceable measurements can be considered reflective of an individual's current health or disease state. Escalating interest in personalized medicine, access to high-throughput genotyping and resulting acquisition of large volumes of genetic data corroborates the second method, Mendelian randomization (MR). MR employs telomere length-associated genetic variants to indicate predisposition to disease risk based on the genomic composition of the individual. When assessed from cells in the bloodstream, telomeres can show variation from their genetically predisposed lengths due to environmental-induced changes. These alterations in telomere length act as an indicator of cellular health, which, in turn, can provide disease risk status. Overall, BTL measurement is a dynamic marker of biological health and well-being that together with genetically defined telomere lengths can provide insights into improved healthcare for the individual.
机译:端粒长度测量越来越被认为是针对年龄相关疾病风险的临床仪表。存在几种研究血液端粒长度(BTL)作为临床生物标志物的方法。首先是一种观察性研究方法,它使用横截面或纵向患者群体直接测量端粒长度,并将其与年龄和性别匹配的个体群体进行比较。这些直接可追踪的测量可以被认为是个体当前健康或疾病状态的反映。升级对个性化医学的兴趣,获得高通量基因分型和产生大量的遗传数据的收购证实了第二种方法,孟德尔随机化(MR)。 MR采用端粒长度相关的遗传变体,基于个体的基因组组成表示疾病风险的易感性。当从血液中的细胞评估时,端粒可以显示由于环境诱导的变化引起的遗传倾斜长度的变化。端粒长度的这些改变作为细胞健康的指标,又可以提供疾病风险状况。总体而言,BTL测量是生物健康的动态标记,与遗传定义的端粒长度一起,可以提供对个体改善的医疗保健的见解。

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