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组蛋白变体 MacroH2A1 以剪接异构体依赖的方式调控成肌细胞融合的关键基因。

The Histone Variant MacroH2A1 Regulates Key Genes for Myogenic Cell Fusion in a Splice-Isoform Dependent Manner.

机构信息

Cancer and Leukemia Epigenetics and Biology Program, Josep Carreras Leukaemia Research Institute (IJC), Campus ICO-GTP-UAB, 08916 Badalona, Spain.

Program for Predictive and Personalized Medicine of Cancer, Germans Trias i Pujol Research Institute (PMPPC-IGTP), 08916 Badalona, Spain.

出版信息

Cells. 2020 Apr 30;9(5):1109. doi: 10.3390/cells9051109.

Abstract

MacroH2A histone variants have functions in differentiation, somatic cell reprogramming and cancer. However, at present, it is not clear how macroH2As affect gene regulation to exert these functions. We have parted from the initial observation that loss of total macroH2A1 led to a change in the morphology of murine myotubes differentiated ex vivo. The fusion of myoblasts to myotubes is a key process in embryonic myogenesis and highly relevant for muscle regeneration after acute or chronic injury. We have focused on this physiological process, to investigate the functions of the two splice isoforms of macroH2A1. Individual perturbation of the two isoforms in myotubes forming in vitro from myogenic C2C12 cells showed an opposing phenotype, with macroH2A1.1 enhancing, and macroH2A1.2 reducing, fusion. Differential regulation of a subset of fusion-related genes encoding components of the extracellular matrix and cell surface receptors for adhesion correlated with these phenotypes. We describe, for the first time, splice isoform-specific phenotypes for the histone variant macroH2A1 in a physiologic process and provide evidence for a novel underlying molecular mechanism of gene regulation.

摘要

组蛋白变体 macroH2A 具有在分化、体细胞重编程和癌症中的功能。然而,目前尚不清楚 macroH2A 如何影响基因调控以发挥这些功能。我们最初的观察是,总 macroH2A1 的缺失导致体外分化的鼠肌管形态发生变化。成肌细胞融合形成肌管是胚胎肌发生的关键过程,对于急性或慢性损伤后的肌肉再生非常重要。我们专注于这个生理过程,以研究 macroH2A1 的两种剪接异构体的功能。在体外从肌源性 C2C12 细胞形成的肌管中单独扰动两种异构体,表现出相反的表型,macroH2A1.1 增强融合,而 macroH2A1.2 减少融合。与这些表型相关的是,对一组与融合相关的基因进行了差异调控,这些基因编码细胞外基质的成分和细胞表面粘附受体。我们首次在生理过程中描述了组蛋白变体 macroH2A1 的剪接异构体特异性表型,并为基因调控的新的潜在分子机制提供了证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/00e9/7290658/62bd600d8010/cells-09-01109-g001.jpg

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