Establishing evidence for immune surveillance of β-cell senescence

Nayara Rampazzo Morelli, Jasmine Pipella, Peter J. Thompson
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Abstract

Cellular senescence is a programmed state of cell cycle arrest that involves a complex immunogenic secretome, eliciting immune surveillance and senescent cell clearance. Recent work has shown that a subpopulation of pancreatic β-cells becomes senescent in the context of diabetes; however, it is not known whether these cells are normally subject to immune surveillance. In this opinion article, we advance the hypothesis that immune surveillance of β-cells undergoing a senescence stress response normally limits their accumulation during aging and that the breakdown of these mechanisms is a driver of senescent β-cell accumulation in diabetes. Elucidation and therapeutic activation of immune surveillance mechanisms in the pancreas holds promise for the improvement of approaches to target stressed senescent β-cells in the treatment of diabetes.

建立免疫监视β细胞衰老的证据
细胞衰老是一种细胞周期停滞的程序化状态,涉及复杂的免疫原性分泌组,引起免疫监视和衰老细胞清除。最近的研究表明,在糖尿病的情况下,胰腺β细胞的一个亚群会发生衰老;然而,这些细胞是否通常会受到免疫监视尚不清楚。在这篇观点性文章中,我们提出了一个假设,即对发生衰老应激反应的β细胞的免疫监视通常会限制它们在衰老过程中的积累,而这些机制的破坏是糖尿病中β细胞衰老积累的驱动因素。阐明和治疗性激活胰腺中的免疫监视机制有望改进针对受压衰老β细胞的方法,从而治疗糖尿病。
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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