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衰老中免疫功能障碍的表观基因组驱动因素。

Epigenomic drivers of immune dysfunction in aging.

机构信息

The Walter and Eliza Hall Institute of Medical Research, Parkville, Victoria, Australia.

Department of Medical Biology, The University of Melbourne, Parkville, Victoria, Australia.

出版信息

Aging Cell. 2019 Feb;18(1):e12878. doi: 10.1111/acel.12878. Epub 2018 Nov 28.

Abstract

Aging inevitably leads to reduced immune function, leaving the elderly more susceptible to infections, less able to respond to pathogen challenges, and less responsive to preventative vaccinations. No cell type is exempt from the ravages of age, and extensive studies have found age-related alterations in the frequencies and functions of both stem and progenitor cells, as well as effector cells of both the innate and adaptive immune systems. The intrinsic functional reduction in immune competence is also associated with low-grade chronic inflammation, termed "inflamm-aging," which further perpetuates immune dysfunction. While many of these age-related cellular changes are well characterized, understanding the molecular changes that underpin the functional decline has proven more difficult. Changes in chromatin are increasingly appreciated as a causative mechanism of cellular and organismal aging across species. These changes include increased genomic instability through loss of heterochromatin and increased DNA damage, telomere attrition, and epigenetic alterations. In this review, we discuss the connections between chromatin, immunocompetence, and the loss of function associated with mammalian immune aging. Through understanding the molecular events which underpin the phenotypic changes observed in the aged immune system, it is hoped that the aged immune system can be restored to provide youthful immunity once more.

摘要

衰老是不可避免的,会导致免疫功能下降,使老年人更容易感染,对病原体的挑战反应能力降低,对预防性疫苗的反应能力降低。没有任何细胞类型能免受衰老的影响,广泛的研究发现,衰老与干细胞和祖细胞的频率和功能以及先天和适应性免疫系统的效应细胞都有关系。固有免疫能力的内在功能下降也与低度慢性炎症有关,称为“炎性衰老”,这进一步加剧了免疫功能障碍。虽然这些与年龄相关的细胞变化有很多已经得到很好的描述,但要理解支持功能下降的分子变化却更加困难。染色质的变化越来越被认为是跨物种细胞和机体衰老的一种因果机制。这些变化包括通过异染色质丢失和增加 DNA 损伤、端粒磨损和表观遗传改变导致的基因组不稳定性增加。在这篇综述中,我们讨论了染色质、免疫能力和与哺乳动物免疫衰老相关的功能丧失之间的联系。通过了解支撑衰老免疫系统中观察到的表型变化的分子事件,希望能够恢复衰老的免疫系统,使其再次拥有年轻的免疫能力。

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