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Molecular Mechanisms of Facultative Heterochromatin Formation: An X-Chromosome Perspective

机译:兼致铬甘草素形成的分子机制:X-染色体的观点

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Facultative heterochromatin (fHC) concerns the developmentally regulated heterochromatinization of different regions of the genome and, in the case of the mammalian X chromosome and imprinted loci, of only one allele of a homologous pair. The formation of fHC participates in the timely repression of genes, by resisting strong trans activators. In this review, we discuss the molecular mechanisms underlying the establishment and maintenance of fHC in mammals using a mouse model. We focus on X-chromosome inactivation (XCI) as a paradigm for fHC but also relate it to genomic imprinting and homeobox (Hox) gene cluster repression. A vital role for noncoding transcription and/or transcripts emerges as the general principle of triggering XCI and canonical imprinting. However, other types of fHC are established through an unknown mechanism, independent of noncoding transcription (Hox clusters and noncanonical imprinting). We also extensively discuss polycomb-group repressive complexes (PRCs), which frequently play a vital role in fHC maintenance.
机译:兼性异铬醇(FHC)涉及基因组不同区域的发育调节异质化,并且在哺乳动物X染色体和印迹基因座的情况下,仅是同源对的一种等位基因。 FHC的形成通过抵抗强反式激活剂来及时抑制基因。在本综述中,我们讨论了使用小鼠模型在哺乳动物中建立和维持FHC的分子机制。我们专注于X-染色体灭活(XCI)作为FHC的范例,但也将其与基因组印记和Homeobox(Hox)基因群集抑制相关。非加入转录和/或转录物的至关重要作用是作为触发XCI和规范印记的一般原则。然而,通过未知机制建立其他类型的FHC,与非编码转录(HOX簇和非甘露透露的印刷)无关。我们还广泛地讨论了多元群体压抑复合物(中国),这在FHC维护中经常发挥重要作用。

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