首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >PNAS Plus: Screen for multi-SUMO–binding proteins reveals a multi-SIM–binding mechanism for recruitment of the transcriptional regulator ZMYM2 to chromatin
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PNAS Plus: Screen for multi-SUMO–binding proteins reveals a multi-SIM–binding mechanism for recruitment of the transcriptional regulator ZMYM2 to chromatin

机译:PNAS Plus:多重SUMO结合蛋白筛选揭示了多重SIM结合机制可将转录调节因子ZMYM2募集到染色质

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摘要

Protein SUMOylation has emerged as an important regulatory event, particularly in nuclear processes such as transcriptional control and DNA repair. In this context, small ubiquitin-like modifier (SUMO) often provides a binding platform for the recruitment of proteins via their SUMO-interacting motifs (SIMs). Recent discoveries point to an important role for multivalent SUMO binding through multiple SIMs in the binding partner as exemplified by poly-SUMOylation acting as a binding platform for ubiquitin E3 ligases such as ring finger protein 4. Here, we have investigated whether other types of protein are recruited through multivalent SUMO interactions. We have identified dozens of proteins that bind to multi-SUMO platforms, thereby uncovering a complex potential regulatory network. Multi-SUMO binding is mediated through multi-SIM modules, and the functional importance of these interactions is demonstrated for the transcriptional corepressor ZMYM2/ZNF198 where its multi-SUMO–binding activity is required for its recruitment to chromatin.
机译:蛋白质SUMOylation已作为重要的调节事件出现,特别是在核过程中,例如转录控制和DNA修复。在这种情况下,小的泛素样修饰剂(SUMO)通常为通过其SUMO相互作用基序(SIM)募集蛋白质提供结合平台。最近的发现指出了通过结合伴侣中多个SIM进行多价SUMO结合的重要作用,例如聚SUMOylation充当泛素E3连接酶(如无名指蛋白4)的结合平台。在这里,我们研究了其他类型的蛋白通过多价SUMO交互招募。我们已经鉴定出数十种与多种SUMO平台结合的蛋白质,从而揭示了一个复杂的潜在监管网络。多重SUMO结合是通过多重SIM模块介导的,这些相互作用的功能重要性对于转录共抑制物ZMYM2 / ZNF198表现出了作用,在那里其多SUMO结合活性是募集染色质所必需的。

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