人类PBMC衰老定量生物标志物的评估。

IF 3.3 Q2 GERIATRICS & GERONTOLOGY Frontiers in aging Pub Date : 2023-09-15 eCollection Date: 2023-01-01 DOI:10.3389/fragi.2023.1260502
Brady M Owen, James Phie, Jennifer Huynh, Scott Needham, Cameron Fraser
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引用次数: 0

摘要

在发达国家,随着年龄的增长,功能下降在很大程度上加重了疾病负担。人们对开发减缓甚至逆转衰老的治疗干预措施越来越感兴趣。由于时间和成本的限制,无法在模式生物中测试大量的健康和寿命延长干预措施。基于细胞的衰老模型可以实现对潜在干预措施的高通量测试。尽管文献中有大量关于细胞特性与供体年龄相关的报道,但在不同的实验室中很少能有力地观察到。这让人怀疑在培养细胞中捕捉到衰老特征的程度。我们测试了先前报道的外周血单核细胞(PBMC)中与供体年龄相关的分子变化,并评估了它们是否适合纳入一组功能性衰老指标。测试的指标涵盖了与衰老有关的几种途径,包括表观遗传学变化、细胞凋亡、蛋白稳定和细胞内通讯。令人惊讶的是,只有两个标记物与供体年龄相关。DNA甲基化年龄准确地预测了供体年龄,证实了这是一个强大的衰老生物标志物。此外,凋亡标志物CD95与供体年龄相关,但仅在PBMC亚群内。为了证明细胞对治疗的再生反应,需要整合细胞功能的多个读数。然而,建立一组检测细胞衰老的措施是具有挑战性的,需要进一步的研究来确定人类年龄的可靠预测因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Evaluation of quantitative biomarkers of aging in human PBMCs.

Functional decline with age contributes significantly to the burden of disease in developed countries. There is growing interest in the development of therapeutic interventions which slow or even reverse aging. Time and cost constraints prohibit the testing of a large number of interventions for health and lifespan extension in model organisms. Cell-based models of aging could enable high throughput testing of potential interventions. Despite extensive reports in the literature of cell properties that correlate with donor age, few are robustly observed across different laboratories. This casts doubt on the extent that aging signatures are captured in cultured cells. We tested molecular changes previously reported to correlate with donor age in peripheral blood mononuclear cells (PBMCs) and evaluated their suitability for inclusion in a panel of functional aging measures. The tested measures spanned several pathways implicated in aging including epigenetic changes, apoptosis, proteostasis, and intracellular communication. Surprisingly, only two markers correlated with donor age. DNA methylation age accurately predicted donor age confirming this is a robust aging biomarker. Additionally, the apoptotic marker CD95 correlated with donor age but only within subsets of PBMCs. To demonstrate cellular rejuvenation in response to a treatment will require integration of multiple read-outs of cell function. However, building a panel of measures to detect aging in cells is challenging and further research is needed to identify robust predictors of age in humans.

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3.00
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审稿时长
13 weeks
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