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晚期肩袖肌腱病中组蛋白修饰的特征。

Characterization of Histone Modifications in Late-Stage Rotator Cuff Tendinopathy.

机构信息

Centre for Sports, Exercise and Life Sciences, Coventry University, Coventry CV1 5FB, UK.

School of Infection and Immunity, College of Medicine, Veterinary and Life Sciences, University of Glasgow, Glasgow G12 8TA, UK.

出版信息

Genes (Basel). 2023 Feb 15;14(2):496. doi: 10.3390/genes14020496.

Abstract

The development and progression of rotator cuff tendinopathy (RCT) is multifactorial and likely to manifest through a combination of extrinsic, intrinsic, and environmental factors, including genetics and epigenetics. However, the role of epigenetics in RCT, including the role of histone modification, is not well established. Using chromatin immunoprecipitation sequencing, differences in the trimethylation status of H3K4 and H3K27 histones in late-stage RCT compared to control were investigated in this study. For H3K4, 24 genomic loci were found to be significantly more trimethylated in RCT compared to control ( < 0.05), implicating genes such as , , and in RCT. For H3K27, 31 loci were shown to be more trimethylated ( < 0.05) in RCT compared to control, inferring a role for , , and . Furthermore, 14 loci were significantly less trimethylated ( < 0.05) in control compared to RCT, implicating , , and . Finally, the TGFβ signaling, axon guidance, and regulation of focal adhesion assembly pathways were found to be enriched in RCT. These findings suggest that the development and progression of RCT is, at least in part, under epigenetic control, highlighting the influence of histone modifications in this disorder and paving the way to further understand the role of epigenome in RCT.

摘要

肩袖肌腱病(RCT)的发展和进展是多因素的,可能通过外在、内在和环境因素的组合表现出来,包括遗传和表观遗传。然而,表观遗传学在 RCT 中的作用,包括组蛋白修饰的作用,尚未得到很好的确立。本研究使用染色质免疫沉淀测序,研究了晚期 RCT 与对照组相比 H3K4 和 H3K27 组蛋白三甲基化状态的差异。对于 H3K4,发现 24 个基因组位点在 RCT 中比对照组显著更多甲基化(<0.05),暗示 、 、 等基因在 RCT 中起作用。对于 H3K27,与对照组相比,31 个位点在 RCT 中显示出更多的三甲基化(<0.05),暗示 、 、 等基因起作用。此外,与 RCT 相比,对照组中 14 个位点的三甲基化显著减少(<0.05),暗示 、 、 等基因起作用。最后,TGFβ 信号通路、轴突导向和焦点黏附组装途径的调控在 RCT 中被富集。这些发现表明,RCT 的发展和进展至少部分受到表观遗传控制,突出了组蛋白修饰在这种疾病中的作用,并为进一步了解表观基因组在 RCT 中的作用铺平了道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d248/9956879/933fb90db4d5/genes-14-00496-g001.jpg

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