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首页> 外文期刊>Nature Communications >The methyltransferase Suv39h1 links the SUMO pathway to HP1α marking at pericentric heterochromatin
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The methyltransferase Suv39h1 links the SUMO pathway to HP1α marking at pericentric heterochromatin

机译:甲基转移酶Suv39h1将SUMO途径连接至外周中心异染色质的HP1α标记

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摘要

The trimethylation of histone H3 on lysine 9 (H3K9me3) – a mark recognized by HP1 that depends on the Suv39h lysine methyltransferases (KMTs) – has provided a basis for the reader/writer model to explain HP1 accumulation at pericentric heterochromatin in mammals. Here, we identify the Suv39h1 paralog, as a unique enhancer of HP1α sumoylation both in vitro and in vivo . The region responsible for promoting HP1α sumoylation (aa1–167) is distinct from the KMT catalytic domain and mediates binding to Ubc9. Tethering the 1–167 domain of Suv39h1 to pericentric heterochromatin, but not mutants unable to bind Ubc9, accelerates the de novo targeting of HP1α to these domains. Our results establish an unexpected feature of Suv39h1, distinct from the KMT activity, with a major role for heterochromatin formation. We discuss how linking Suv39h1 to the SUMO pathway provides conceptual implications for our general view on nuclear domain organization and physiological functions.
机译:赖氨酸9(H3K9me3)上的组蛋白H3的三甲基化-HP1识别的标记,取决于Suv39h赖氨酸甲基转移酶(KMT)-为读/写模型提供了基础,以解释HP1在哺乳动物周缘异染色质上的积累。在这里,我们确定Suv39h1旁系同源物,作为HP1αsumoylation在体外和体内的独特增强剂。负责促进HP1α磺酰化的区域(aa1-167)与KMT催化域不同,并介导与Ubc9的结合。将Suv39h1的1–167结构域与外周中心异染色质束缚在一起,但不能将不能结合Ubc9的突变体束缚在一起,可以将HP1α从头开始靶向这些结构域。我们的研究结果建立了Suv39h1的意外功能,与KMT活性不同,主要是异染色质的形成。我们讨论如何将Suv39h1链接到SUMO途径如何为我们对核域组织和生理功能的一般观点提供概念上的启示。

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