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核型特异性 DNA 甲基组学揭示了骨骼肌中先前适应的表观遗传“记忆”。

Nucleus Type-Specific DNA Methylomics Reveals Epigenetic "Memory" of Prior Adaptation in Skeletal Muscle.

机构信息

Department of Physiology, University of Kentucky, Lexington, KY 40508, USA.

The Center for Muscle Biology, University of Kentucky, Lexington, KY 40536, USA.

出版信息

Function (Oxf). 2021 Aug 5;2(5):zqab038. doi: 10.1093/function/zqab038. eCollection 2021.

Abstract

Using a mouse model of conditional and inducible fluorescent myonuclear labeling (HSA-GFP), sorting purification of nuclei, low-input reduced representation bisulfite sequencing (RRBS), and a translatable and reversible model of exercise (progressive weighted wheel running, PoWeR), we provide the first nucleus type-specific epigenetic information on skeletal muscle adaptation and detraining. Adult (>4 mo) HSA-GFP mice performed PoWeR for 8 wk then detrained for 12 wk; age-matched untrained mice were used to control for the long duration of the study. Myonuclei and interstitial nuclei from plantaris muscles were isolated for RRBS. Relative to untrained, PoWeR caused similar myonuclear CpG hypo- and hyper-methylation of promoter regions and substantial hypomethylation in interstitial nuclear promoters. Over-representation analysis of promoters revealed a larger number of hyper- versus hypo-methylated pathways in both nuclear populations after training and evidence for reciprocal regulation of methylation between nucleus types, with hypomethylation of promoter regions in Wnt signaling-related genes in myonuclei and hypermethylation in interstitial nuclei. After 12 wk of detraining, promoter CpGs in documented muscle remodeling-associated genes and pathways that were differentially methylated immediately after PoWeR were persistently differentially methylated in myonuclei, along with long-term promoter hypomethylation in interstitial nuclei. No enduring gene expression changes in muscle tissue were observed using RNA-sequencing. Upon 4 wk of retraining, mice that trained previously grew more at the whole muscle and fiber type-specific cellular level than training naïve mice, with no difference in myonuclear number. Muscle nuclei have a methylation epi-memory of prior training that may augment muscle adaptability to retraining.

摘要

利用条件性和诱导性荧光肌核标记(HSA-GFP)的小鼠模型、核分选纯化、低输入简化代表性亚硫酸氢盐测序(RRBS),以及可翻译和可逆的运动模型(渐进式加权轮跑,PoWeR),我们提供了骨骼肌适应和停训的第一个核类型特异性表观遗传信息。成年(>4 个月)HSA-GFP 小鼠进行 PoWeR 8 周,然后停训 12 周;年龄匹配的未经训练的小鼠用于控制研究的长时间。从小鼠比目鱼肌中分离肌核和间质核进行 RRBS。与未经训练的相比,PoWeR 导致启动子区域的肌核 CpG 低甲基化和高甲基化相似,间质核启动子发生大量低甲基化。启动子的过表达分析表明,在两种核群体中,训练后有更多的高甲基化和低甲基化途径,并且核类型之间存在甲基化的相互调节,肌核中 Wnt 信号相关基因的启动子区域低甲基化,间质核中高甲基化。停训 12 周后,PoWeR 后立即出现差异甲基化的记录在案的与肌肉重塑相关的基因和途径的启动子 CpG 在肌核中持续差异甲基化,间质核中存在长期启动子低甲基化。使用 RNA-seq 未观察到肌肉组织中持久的基因表达变化。在 4 周的再训练后,之前接受过训练的小鼠在整个肌肉和纤维类型特异性细胞水平上的生长速度都高于初次接受训练的小鼠,而肌核数量没有差异。肌肉核具有先前训练的甲基化表观遗传记忆,可能增强肌肉对再训练的适应性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e8b5/8833862/71696dfb3f55/zqab038fig1g.jpg

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