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猪胎儿骨骼肌肉发育与全基因组 DNA 低甲基化以及转录物和 microRNA 表达的相应改变有关。

Pig fetal skeletal muscle development is associated with genome-wide DNA hypomethylation and corresponding alterations in transcript and microRNA expression.

机构信息

Genetics & Genome Sciences Graduate Program, Michigan State University, East Lansing, MI 48824, USA.

Department of Animal Science, Michigan State University, East Lansing, MI 48824, USA.

出版信息

Genome. 2023 Apr 1;66(4):68-79. doi: 10.1139/gen-2022-0008. Epub 2023 Mar 6.

DOI:10.1139/gen-2022-0008
PMID:36876850
Abstract

Fetal myogenesis represents a critical period of porcine skeletal muscle development and requires coordinated expression of thousands of genes. Epigenetic mechanisms, including DNA methylation, drive transcriptional regulation during development; however, these processes are understudied in developing porcine tissues. We performed bisulfite sequencing to assess DNA methylation in pig muscle at 41- and 70-days gestation (dg), as well as RNA- and small RNA-sequencing to identify coordinated changes in methylation and expression between myogenic stages. We identified 45 739 differentially methylated regions (DMRs) between stages, and the majority ( = 34 232) were hypomethylated at 70 versus 41 dg. Integration of methylation and transcriptomic data revealed strong associations between differential gene methylation and expression. Differential miRNA methylation was significantly negatively correlated with abundance, and dynamic expression of assayed miRNAs persisted postnatally. Motif analysis revealed significant enrichment of myogenic regulatory factor motifs among hypomethylated regions, suggesting that DNA hypomethylation may function to increase accessibility of muscle-specific transcription factors. We show that developmental DMRs are enriched for GWAS SNPs for muscle- and meat-related traits, demonstrating the potential for epigenetic processes to influence phenotypic diversity. Our results enhance understanding of DNA methylation dynamics of porcine myogenesis and reveal putative -regulatory elements governed by epigenetic processes.

摘要

胎儿肌发生代表了猪骨骼肌发育的关键时期,需要数千个基因的协调表达。表观遗传机制,包括 DNA 甲基化,在发育过程中驱动转录调控;然而,这些过程在发育中的猪组织中研究甚少。我们进行了亚硫酸氢盐测序,以评估 41 日龄和 70 日龄妊娠(dg)猪肌肉中的 DNA 甲基化,以及 RNA 和小 RNA 测序,以鉴定肌生成阶段之间甲基化和表达的协调变化。我们在阶段之间鉴定了 45739 个差异甲基化区域(DMRs),其中大多数(= 34232 个)在 70 dg 时比 41 dg 时低甲基化。甲基化和转录组数据的整合表明,差异基因甲基化与表达之间存在很强的关联。差异 miRNA 甲基化与丰度呈显著负相关,并且检测到的 miRNA 的动态表达在出生后持续存在。基序分析表明,低甲基化区域中富含肌生成调节因子基序,表明 DNA 低甲基化可能有助于增加肌肉特异性转录因子的可及性。我们表明,发育性 DMR 富集了与肌肉和肉质相关性状的 GWAS SNP,表明表观遗传过程具有影响表型多样性的潜力。我们的研究结果增强了对猪肌发生中 DNA 甲基化动态的理解,并揭示了受表观遗传过程调控的潜在调控元件。

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