小鼠视网膜色素上皮细胞不同年龄和性别的转位反应

IF 3.7 3区 医学 Q2 GERIATRICS & GERONTOLOGY Neurobiology of Aging Pub Date : 2024-05-03 DOI:10.1016/j.neurobiolaging.2024.04.012
Ana J. Chucair-Elliott , Sarah R. Ocañas , Kevin Pham , Adeline Machalinski , Scott Plafker , Michael B. Stout , Michael H. Elliott , Willard M. Freeman
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引用次数: 0

摘要

衰老是老年性黄斑变性(AMD)的主要风险因素,AMD 是一种视网膜神经退行性疾病,会导致不可逆转的失明,尤其是 60 岁以上的老年人。视网膜色素上皮(RPE)萎缩是老年性黄斑变性的标志。对 AMD 和对照 RPE 进行的全基因组染色质可及性、DNA 甲基化和基因表达研究表明,在 AMD 发病和发展过程中会发生表观基因组/转录组变化。然而,正常衰老的分子改变损害 RPE 功能并导致 AMD 发病的机制尚不清楚。在此,我们在一种新型 RPE 报告小鼠模型中,专门研究了随着年龄的增长和不同性别的 RPE 易位组。我们发现与年龄和性别相关的转录本表达存在差异,与炎症相关的通路在 RPE 中的代表性过高。与 RPE 功能受损相一致的是,老年转录组的表型变化表明,老年 RPE 变得免疫活跃,男性和女性都是如此,并具有一些性别特异性特征,这支持了体内研究对性别代表性的需求。
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Age- and sex- divergent translatomic responses of the mouse retinal pigmented epithelium

Aging is the main risk factor for age-related macular degeneration (AMD), a retinal neurodegenerative disease that leads to irreversible blindness, particularly in people over 60 years old. Retinal pigmented epithelium (RPE) atrophy is an AMD hallmark. Genome-wide chromatin accessibility, DNA methylation, and gene expression studies of AMD and control RPE demonstrate epigenomic/transcriptomic changes occur during AMD onset and progression. However, mechanisms by which molecular alterations of normal aging impair RPE function and contribute to AMD pathogenesis are unclear.

Here, we specifically interrogate the RPE translatome with advanced age and across sexes in a novel RPE reporter mouse model. We find differential age- and sex- associated transcript expression with overrepresentation of pathways related to inflammation in the RPE. Concordant with impaired RPE function, the phenotypic changes in the aged translatome suggest that aged RPE becomes immunologically active, in both males and females, with some sex-specific signatures, which supports the need for sex representation for in vivo studies.

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来源期刊
Neurobiology of Aging
Neurobiology of Aging 医学-老年医学
CiteScore
8.40
自引率
2.40%
发文量
225
审稿时长
67 days
期刊介绍: Neurobiology of Aging publishes the results of studies in behavior, biochemistry, cell biology, endocrinology, molecular biology, morphology, neurology, neuropathology, pharmacology, physiology and protein chemistry in which the primary emphasis involves mechanisms of nervous system changes with age or diseases associated with age. Reviews and primary research articles are included, occasionally accompanied by open peer commentary. Letters to the Editor and brief communications are also acceptable. Brief reports of highly time-sensitive material are usually treated as rapid communications in which case editorial review is completed within six weeks and publication scheduled for the next available issue.
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