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选择性自噬作为年龄相关疾病的潜在治疗靶点

Selective Autophagy as a Potential Therapeutic Target in Age-Associated Pathologies.

作者信息

Papandreou Margarita-Elena, Tavernarakis Nektarios

机构信息

Institute of Molecular Biology and Biotechnology, Foundation for Research and Technology-Hellas, 70013 Heraklion, Greece.

Department of Basic Sciences, Faculty of Medicine, University of Crete, 70013 Heraklion, Greece.

出版信息

Metabolites. 2021 Aug 31;11(9):588. doi: 10.3390/metabo11090588.

Abstract

Progressive accumulation of damaged cellular constituents contributes to age-related diseases. Autophagy is the main catabolic process, which recycles cellular material in a multitude of tissues and organs. Autophagy is activated upon nutrient deprivation, and oncogenic, heat or oxidative stress-induced stimuli to selectively degrade cell constituents and compartments. Specificity and accuracy of the autophagic process is maintained via the precision of interaction of autophagy receptors or adaptors and substrates by the intricate, stepwise orchestration of specialized integrating stimuli. Polymorphisms in genes regulating selective autophagy have been linked to aging and age-associated disorders. The involvement of autophagy perturbations in aging and disease indicates that pharmacological agents balancing autophagic flux may be beneficial, in these contexts. Here, we introduce the modes and mechanisms of selective autophagy, and survey recent experimental evidence of dysfunctional autophagy triggering severe pathology. We further highlight identified pharmacological targets that hold potential for developing therapeutic interventions to alleviate cellular autophagic cargo burden and associated pathologies.

摘要

受损细胞成分的渐进性积累会导致与年龄相关的疾病。自噬是主要的分解代谢过程,可在众多组织和器官中循环利用细胞物质。自噬在营养剥夺以及致癌、热或氧化应激诱导的刺激下被激活,以选择性地降解细胞成分和区室。通过自噬受体或衔接子与底物之间相互作用的精确性,以及专门整合刺激的复杂、逐步编排,维持了自噬过程的特异性和准确性。调节选择性自噬的基因多态性与衰老和年龄相关疾病有关。自噬紊乱在衰老和疾病中的作用表明,在这些情况下,平衡自噬通量的药物可能有益。在这里,我们介绍选择性自噬的模式和机制,并综述自噬功能障碍引发严重病理的最新实验证据。我们进一步强调已确定的药理学靶点,这些靶点具有开发治疗干预措施以减轻细胞自噬货物负担和相关病理的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7c22/8472713/68540e1ee9e0/metabolites-11-00588-g001.jpg

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