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Sex-Based Mhrt Methylation Chromatinizes MeCP2 in the Heart

机译:基于性的MHRT甲基化在心脏中的MECP2染色

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Summary: In the heart, primary microRNA-208b (pri-miR-208b) and Myheart (Mhrt) are long non-coding RNAs (lncRNAs) encoded by the cardiac myosin heavy chain genes. Although preclinical studies have shown that lncRNAs regulate gene expression and are protective for pathological hypertrophy, the mechanism underlying sex-based differences remains poorly understood. In this study, we examined DNA- and RNA-methylation-dependent regulation of pri-miR-208b and Mhrt. Expression of pri-miR-208b is elevated in the left ventricle of the female heart. Despite indistinguishable DNA methylation between sexes, the interaction of MeCP2 on chromatin is subject to RNase digestion, highlighting that affinity of the methyl-CG reader is broader than previously thought. A specialized procedure to isolate RNA from soluble cardiac chromatin emphasizes sex-based affinity of an MeCP2 co-repressor complex with Rest and Hdac2. Sex-specific Mhrt methylation chromatinizes MeCP2 at the pri-miR-208b promoter and extends the functional relevance of default transcriptional suppression in the heart. : Molecular Physiology; Molecular Genetics; Molecular Mechanism of Gene Regulation Subject Areas: Molecular Physiology, Molecular Genetics, Molecular Mechanism of Gene Regulation
机译:小结:在心脏中,初级微小RNA-208B(PRI-MIR-208B)和Myheart(MHRT)是长由心肌肌球蛋白重链基因编码的非编码RNA(lncRNAs)。虽然临床前研究表明,lncRNAs调节基因表达,并且保护用于病理性肥大,底层基于性别的差异的机制仍然知之甚少。在这项研究中,我们研究了DNA和PRI-MIR-208B和MHRT的RNA甲基化依赖的调节。在女性心脏的左心室升高PRI-MIR-208b的表达。尽管两性之间难以区分DNA甲基化,MeCP2的对染色质相互作用是受RNA酶消化,突出甲基CG读者的那个亲和性比以前认为的更为广泛。一个专门的过程可从可溶性心肌染色质分离物的RNA强调的MeCP2的共抑制复合物与休息和HDAC2的基于性别的亲和力。性别特异性MHRT甲基chromatinizes的MeCP2在PRI-MIR-208B子和延伸默认转录抑制在心脏功能相关。 :分子生理学;分子遗传学;分子生理学,分子遗传学,基因表达调控的分子机制:基因调控学科领域的分子机制

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