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首页> 外文期刊>Nucleic acids research >Periphilin self-association underpins epigenetic silencing by the HUSH complex
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Periphilin self-association underpins epigenetic silencing by the HUSH complex

机译:Periphilin自我关联由嘘声复合物的表观遗传沉默

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Transcription of integrated DNA from viruses or transposable elements is tightly regulated to prevent pathogenesis. The Human Silencing Hub (HUSH), composed of Periphilin, TASOR and MPP8, silences transcriptionally active viral and endogenous transgenes. HUSH recruits effectors that alter the epigenetic landscape and chromatin structure, but how HUSH recognizes target loci and represses their expression remains unclear. We identify the physicochemical properties of Periphilin necessary for HUSH assembly and silencing. A disordered N-terminal domain (NTD) and structured C-terminal domain are essential for silencing. A crystal structure of the Periphilin-TASOR minimal core complex shows Periphilin forms an α-helical homodimer, bound by a single TASOR molecule. The NTD forms insoluble aggregates through an arginine/tyrosine-rich sequence reminiscent of low-complexity regions from self-associating RNA-binding proteins. Residues required for TASOR binding and aggregation were required for HUSH-dependent silencing and genome-wide deposition of repressive mark H3K9me3. The NTD was functionally complemented by low-complexity regions from certain RNA-binding proteins and proteins that form condensates or fibrils. Our work suggests the associative properties of Periphilin promote HUSH aggregation at target loci.
机译:从病毒或转移元件的整合DNA转录被紧密调节以预防发病机制。由Periphilin,Tasor和MPP8组成的人沉默的枢纽(肿瘤),沉默转录活性病毒和内源转基因。 Hush recuity endery excuments改变了表观遗传景观和染色质结构,但如何抑制目标基因座并抑制它们的表达仍然不清楚。我们确定嘘声组装和沉默所需必要的哌啶的物理化学性质。无序的N末端结构域(NTD)和结构化C末端域对于沉默是必不可少的。 Periphilin-Tasor最小核心复合物的晶体结构显示Periphilin形成α-螺旋同型二聚体,由单个促催化剂结合。 NTD通过从自相关RNA结合蛋白的低复杂性区域让富络合物中的富含精氨酸/酪氨酸的序列形成不溶性聚集体。栓塞结合和聚集所需的残留物是抑制沉默的沉默和基因组沉积的抑制标记H3K9ME3所需的残留物。 NTD通过来自某些RNA结合蛋白和蛋白质的低复杂性区域在功能上互补,形成缩合物或原纤蛋白。我们的作品表明Periphilin促进目标基因座的联合特性。

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