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Dead end1 is an essential partner of NANOS2 for selective binding of target RNAs in male germ cell development

机译:Dead end1是NANOS2在雄性生殖细胞发育中选择性结合靶RNA的重要伙伴。

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摘要

RNA‐binding proteins (RBPs) play important roles for generating various cell types in many developmental processes, including eggs and sperms. Nanos is widely known as an evolutionarily conserved RNA‐binding protein implicated in germ cell development. Mouse NANOS2 interacts directly with the CCR4‐NOT (CNOT) deadenylase complex, resulting in the suppression of specific RNAs. However, the mechanisms involved in target specificity remain elusive. We show that another RBP, Dead end1 (DND1), directly interacts with NANOS2 to load unique RNAs into the CNOT complex. This interaction is mediated by the zinc finger domain of NANOS2, which is essential for its association with target RNAs. In addition, the conditional deletion of DND1 causes the disruption of male germ cell differentiation similar to that observed in Nanos2‐ style="fixed-case">KO mice. Thus, style="fixed-case">DND1 is an essential partner for style="fixed-case">NANOS2 that leads to the degradation of specific style="fixed-case">RNAs. We also present the first evidence that the zinc finger domain of Nanos acts as a protein‐interacting domain for another style="fixed-case">RBP, providing a novel insight into Nanos‐mediated germ cell development.
机译:RNA结合蛋白(RBP)在许多发育过程中(包括卵和精子)在产生各种细胞类型中起着重要作用。 Nanos是众所周知的一种进化保守的RNA结合蛋白,与生殖细胞发育有关。小鼠NANOS2与CCR4-NOT(CNOT)腺苷酸酶复合物直接相互作用,从而抑制了特定的RNA。但是,涉及靶标特异性的机制仍然难以捉摸。我们显示了另一个RBP,Dead end1(DND1),直接与NANOS2交互以将独特的RNA加载到CNOT复合物中。这种相互作用是由NANOS2的锌指结构域介导的,这对于其与靶RNA的结合至关重要。此外,有条件的删除DND1会导致雄性生殖细胞分化的破坏,类似于在Nanos2- style =“ fixed-case”> KO 小鼠中观察到的破坏。因此, style =“ fixed-case”> DND 1是 style =“ fixed-case”> NANOS 2的重要合作伙伴,导致特定的 style = “ fixed-case”> RNA s。我们还提供了第一个证据,即Nanos的锌指结构域充当另一个 style =“ fixed-case”> RBP 的蛋白质相互作用域,从而为Nanos介导的生殖细胞发育提供了新颖的见解。

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