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Histone H2A ubiquitination in transcriptional regulation and DNA damage repair.

机译:组蛋白H2A泛素化在转录调控和DNA损伤修复中。

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摘要

The precise molecular strategies that coordinate patterns of transcriptional response to specific signals is central for understanding normal development and disease. Precise control of transcriptional programs underlying metazoan development is modulated by enzymatically active coregulatory complexes, coupled with epigenetic strategies. Epigenetic modifications, particularly DNA methylation and covalent histone modifications, for instance acetylation, methylation, phosphorylation and ubiquitination, play an essential role in transcription regulation, chromatin remodeling, genome instability and X chromosome inactivation. Recently, the ubiquitinases and deubiquitinases responsible for histone H2A ubiquitination and deubiquitination have been identified and characterized. These studies suggest that histone H2A ubiquitination play important roles in many cellular events, such as transcription initiation and elongation, silencing, and DNA repair. Alteration of histone H2A ubiquitination modifications may contribute human diseases, such as cancer. In this review, we discuss enzymes involved in H2A ubiquitination/deubiquitination and that possible molecular mechanisms underlying histone H2A ubiquitination/deubiquitination in transcriptional regulation and DNA damage repair.
机译:协调转录对特定信号的反应模式的精确分子策略对于理解正常发育和疾病至关重要。对后生动物发育的转录程序的精确控制是通过酶活性共调节复合物以及表观遗传学策略来调节的。表观遗传修饰,特别是DNA甲基化和共价组蛋白修饰,例如乙酰化,甲基化,磷酸化和泛素化,在转录调控,染色质重塑,基因组不稳定和X染色体失活中起着至关重要的作用。最近,已经鉴定和鉴定了负责组蛋白H2A泛素化和去泛素化的泛素化酶和去泛素化酶。这些研究表明,组蛋白H2A泛素化在许多细胞事件中起重要作用,例如转录起始和延伸,沉默和DNA修复。组蛋白H2A泛素修饰的改变可能导致人类疾病,例如癌症。在这篇综述中,我们讨论了涉及H2A泛素化/去泛素化的酶,以及在转录调控和DNA损伤修复中组蛋白H2A泛素化/去泛素化的潜在分子机制。

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