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Linker histone H1.5 is an underestimated factor in differentiation and carcinogenesis

机译:链接器组蛋白H1.5是分化和致癌产生的低估因子

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Human histone H1.5, in mice called H1b, belongs to the family of linker histones (H1), which are key players in chromatin organization. These proteins sit on top of nucleosomes, in part to stabilize them, and recruit core histone modifying enzymes. Through subtype-specific deposition patterns and numerous post-translational modifications, they fine-tune gene expression and chromatin architecture, and help to control cell fate and homeostasis. However, even though it is increasingly implicated in mammalian development, H1.5 has not received as much research attention as its relatives. Recent studies have focused on its prognostic value in cancer patients and its contribution to tumorigenesis through specific molecular mechanisms. However, many functions of H1.5 are still poorly understood. In this review, we will summarize what is currently known about H1.5 and its function in cell differentiation and carcinogenesis. We will suggest key experiments that are required to understand the molecular network, in which H1.5 is embedded. These experiments will advance our understanding of the epigenetic reprogramming occurring in developmental and carcinogenic processes.
机译:在称为H1b的小鼠中,人组蛋白H1.5属于链接组组蛋白(H1)的系列,其是染色质组织中的关键球员。这些蛋白质坐在核心的顶部,部分稳定它们,并募集核心组蛋白改性酶。通过亚型特异性沉积模式和许多翻译后修饰,它们微调基因表达和染色质架构,并帮助控制细胞命运和稳态。然而,尽管它越来越涉及哺乳动物的发展,但H1.5没有作为其亲属获得的研究。最近的研究侧重于其通过特定分子机制对癌症患者的预后价值及其对肿瘤发生的贡献。然而,H1.5的许多功能仍然明白。在本综述中,我们将总结目前已知的H1.5及其在细胞分化和致癌中的功能。我们将建议理解分子网络所需的关键实验,其中嵌入了H1.5。这些实验将推进我们对发育和致癌过程中发生的表观遗传重编程的理解。

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