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HP1BP3 is a novel histone H1 related protein with essential roles in viability and growth

机译:HP1BP3是一种新型的组蛋白H1相关蛋白,在生存能力和生长中起重要作用

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The dynamic architecture of chromatin is vital for proper cellular function, and is maintained by the concerted action of numerous nuclear proteins, including that of the linker histone H1 variants, the most abundant family of nucleosome-binding proteins. Here we show that the nuclear protein HP1BP3 is widely expressed in most vertebrate tissues and is evolutionarily and structurally related to the H1 family. HP1BP3 contains three globular domains and a highly positively charged C-terminal domain, resembling similar domains in H1. Fluorescence recovery after photobleaching (FRAP) studies indicate that like H1, binding of HP1BP3 to chromatin depends on both its C and N terminal regions and is affected by the cell cycle and post translational modifications. HP1BP3 contains functional motifs not found in H1 histones, including an acidic stretch and a consensus HP1-binding motif. Transcriptional profiling of HeLa cells lacking HP1BP3 showed altered expression of 383 genes, suggesting a role for HP1BP3 in modulation of gene expression. Significantly, Hp1bp3?/? mice present a dramatic phenotype with 60% of pups dying within 24 h of birth and the surviving animals exhibiting a lifelong 20% growth retardation. We suggest that HP1BP3 is a ubiquitous histone H1 like nuclear protein with distinct and non-redundant functions necessary for survival and growth.
机译:染色质的动态结构对于适当的细胞功能至关重要,并通过众多核蛋白的协同作用得以维持,包括接头组蛋白H1变异体(核小体结合蛋白家族中最丰富的家族)的协同作用。在这里,我们显示核蛋白HP1BP3在大多数脊椎动物组织中广泛表达,并且在进化和结构上与H1家族有关。 HP1BP3包含三个球状结构域和一个高度带正电的C端结构域,类似于H1中的类似结构域。光漂白后的荧光恢复(FRAP)研究表明,与H1一样,HP1BP3与染色质的结合取决于其C和N末端区域,并受细胞周期和翻译后修饰的影响。 HP1BP3包含在H1组蛋白中找不到的功能性基序,包括酸性延伸和共有的HP1结合基序。缺乏HP1BP3的HeLa细胞的转录谱分析显示383个基因的表达发生了改变,这表明HP1BP3在调节基因表达中的作用。值得注意的是,Hp1bp3 ?/?小鼠表现出戏剧性的表型,其中60%的幼崽在出生后24小时内死亡,而存活的动物则表现出终生20%的生长迟缓。我们建议,HP1BP3是一种普遍存在的组蛋白H1,就像核蛋白一样,具有独特的和非冗余的功能,对于生存和生长是必不可少的。

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