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Structures of heterodimeric POZ domains of Miz1/BCL6 and Miz1/NAC1

机译:Miz1 / BCL6和Miz1 / NAC1的异二聚POZ域的结构

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摘要

The POZ domain is an evolutionarily conserved protein–protein interaction domain that is found in approximately 40 mammalian transcription factors. POZ domains mediate both homodimerization and the heteromeric interactions of different POZ-domain transcription factors with each other. Miz1 is a POZ-domain transcription factor that regulates cell-cycle arrest and DNA-damage responses. The activities of Miz1 are altered by its interaction with the POZ-domain transcriptional repressors BCL6 and NAC1, and these interactions have been implicated in tumourigenesis in B-cell lymphomas and in ovarian serous carcinomas that overexpress BCL6 and NAC1, respectively. A strategy for the purification of tethered POZ domains that form forced heterodimers is described, and crystal structures of the heterodimeric POZ domains of Miz1/BCL6 and of Miz1/NAC1 are reported. These structures will be relevant for the design of therapeutics that target POZ-domain interaction interfaces.
机译:POZ域是一种进化保守的蛋白质-蛋白质相互作用域,存在于大约40个哺乳动物转录因子中。 POZ结构域介导同质二聚化和不同POZ结构域转录因子之间的异源相互作用。 Miz1是一个POZ域转录因子,可调节细胞周期停滞和DNA损伤反应。 Miz1的活性因其与POZ域转录阻遏物BCL6和NAC1的相互作用而改变,并且这些相互作用分别与B细胞淋巴瘤和过表达BCL6和NAC1的卵巢浆液性癌的肿瘤发生有关。描述了一种纯化形成强制异二聚体的拴系POZ域的策略,并报道了Miz1 / BCL6和Miz1 / NAC1的异二聚体POZ域的晶体结构。这些结构将与针对POZ域相互作用界面的治疗药物的设计有关。

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