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稳定同位素标记揭示了泛素介导的蛋白质聚集在衰老、热量限制和雷帕霉素处理中的新见解。

Stable Isotope Labeling Reveals Novel Insights Into Ubiquitin-Mediated Protein Aggregation With Age, Calorie Restriction, and Rapamycin Treatment.

机构信息

Department of Pathology, University of Washington, Seattle.

Buck Institute for Research on Aging, Novato, California.

出版信息

J Gerontol A Biol Sci Med Sci. 2018 Apr 17;73(5):561-570. doi: 10.1093/gerona/glx047.

Abstract

Accumulation of protein aggregates with age was first described in aged human tissue over 150 years ago and has since been described in virtually every human tissue. Ubiquitin modifications are a canonical marker of insoluble protein aggregates; however, the composition of most age-related inclusions remains relatively unknown. To examine the landscape of age-related protein aggregation in vivo, we performed an antibody-based pulldown of ubiquitinated proteins coupled with metabolic labeling and mass spectrometry on young and old mice on calorie restriction (CR), rapamycin (RP)-supplemented, and control diets. We show increased abundance of many ubiquitinated proteins in old mice and greater retention of preexisting (unlabeled) ubiquitinated proteins relative to their unmodified counterparts-fitting the expected profile of age-increased accumulation of long-lived aggregating proteins. Both CR and RP profoundly affected ubiquitinome composition, half-live, and the insolubility of proteins, consistent with their ability to mobilize these age-associated accumulations. Finally, confocal microscopy confirmed the aggregation of two of the top predicted aggregating proteins, keratins 8/18 and catalase, as well as their attenuation by CR and RP. Stable-isotope labeling is a powerful tool to gain novel insights into proteostasis mechanisms, including protein aggregation, and could be used to identify novel therapeutic targets in aging and protein aggregation diseases.

摘要

蛋白质聚集体的积累早在 150 多年前就首次在衰老的人体组织中被描述,此后几乎在所有人类组织中都有描述。泛素修饰是不可溶性蛋白质聚集体的典型标志;然而,大多数与年龄相关的包含物的组成仍然相对未知。为了研究体内与年龄相关的蛋白质聚集的情况,我们对年轻和年老的接受热量限制(CR)、雷帕霉素(RP)补充和对照饮食的老鼠进行了基于抗体的泛素化蛋白下拉实验,并结合代谢标记和质谱分析。结果表明,老年小鼠中许多泛素化蛋白的丰度增加,与未修饰的蛋白相比,预先存在的(未标记)泛素化蛋白的保留更多——这符合预期的寿命延长的聚集蛋白积累的模式。CR 和 RP 都对泛素组组成、半衰期和蛋白质的不溶性产生了深远的影响,这与它们能够动员这些与年龄相关的积累物的能力一致。最后,共聚焦显微镜证实了两种预测的最易聚集的蛋白质角蛋白 8/18 和过氧化氢酶的聚集,以及 CR 和 RP 对其的抑制作用。稳定同位素标记是一种获得对蛋白质稳态机制(包括蛋白质聚集)的新见解的强大工具,可用于在衰老和蛋白质聚集疾病中识别新的治疗靶点。

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