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Histone H2A monoubiquitination and Polycomb repression

机译:组蛋白H2A单泛素化和多梳抑制

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Polycomb group (PcG) proteins were originally identified as negative regulators of HOX genes in Drosophila but have since emerged as a widely used transcriptional repression system that controls a variety of developmental processes in animals and plants. PcG proteins exist in multi-protein complexes that comprise specific chromatin-modifying enzymatic activities. Genomewide binding studies in Drosophila and in mammalian cells revealed that these complexes co-localize at a large set of genes encoding developmental regulators. Recent analyses in Drosophila have begun to explore how the different chromatin-modifying activities of PcG protein complexes contribute to the repression of individual target genes. These studies suggest that monoubiquitination of histone H2A ( H2Aub) by the PcG protein Sce is only essential for repression of a subset of PcG target genes but is not required for the Polycomb-mediated repression of other targets. Calypso/dBap1, a major deubiquitinase for H2Aub is also critically needed for repression of a subset of PcG target genes. Here, we review our current understanding of the role of H2A monoubiquitination and deubiquitination in Polycomb repression in Drosophila. We discuss unresolved issues concerning the immunological detection of H2Aub and critically evaluate experiments that used Sce and Ring1B point mutants with impaired H2A ubiquitinase activity to study H2Aub-dependent and -independent functions of these proteins in transcriptional repression.
机译:聚梳组(PcG)蛋白最初被鉴定为果蝇中HOX基因的负调控因子,但此后已成为一种广泛使用的转录抑制系统,可控制动植物的各种发育过程。 PcG蛋白存在于包含特异性染色质修饰酶活性的多蛋白复合物中。在果蝇和哺乳动物细胞中的全基因组结合研究表明,这些复合物共定位在一大批编码发育调节因子的基因上。果蝇的最新分析已开始探索PcG蛋白复合物的不同染色质修饰活性如何对单个靶基因的抑制。这些研究表明,PcG蛋白Sce对组蛋白H2A(H2Aub)的单泛素化作用仅对抑制PcG靶基因的一个子集至关重要,而对于由Polycomb介导的对其他靶点的抑制则不是必需的。 Calypso / dBap1,H2Aub的主要去泛素酶,也是抑制PcG靶基因子集的关键。在这里,我们回顾我们目前对H2A单泛素化和去泛素化在果蝇多梳抑制中的作用的理解。我们讨论了有关H2Aub免疫学检测的未解决问题,并严格评估了使用具有受损H2A泛素酶活性的Sce和Ring1B点突变体来研究这些蛋白在转录阻抑中的H2Aub依赖性和非依赖性功能的实验。

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