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Mitochondrial protein BmPAPI modulates the length of mature piRNAs

机译:线粒体蛋白BmPAPI调节成熟piRNA的长度

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PIWI proteins and their associated PIWI-interacting RNAs (piRNAs) protect genome integrity by silencing transposons in animal germlines. The molecular mechanisms and components responsible for piRNA biogenesis remain elusive. PIWI proteins contain conserved symmetrical dimethylarginines (sDMAs) that are specifically targeted by TUDOR domain-containing proteins. Here we report that the sDMAs of PIWI proteins play crucial roles in PIWI localization and piRNA biogenesis in Bombyx mori-derived BmN4 cells, which harbor fully functional piRNA biogenesis machinery. Moreover, RNAi screenings for Bombyx genes encoding TUDOR domain-containing proteins identified BmPAPI, a Bombyx homolog of Drosophila PAPI, as a factor modulating the length of mature piRNAs. BmPAPI specifically recognized sDMAs and interacted with PIWI proteins at the surface of the mitochondrial outer membrane. BmPAPI depletion resulted in 3? -terminal extensions of mature piRNAs without affecting the piRNA quantity. These results reveal the BmPAPI-involved piRNA precursor processing mechanism on mitochondrial outer membrane scaffolds.
机译:PIWI蛋白及其相关的PIWI相互作用RNA(piRNA)通过沉默动物种系中的转座子来保护基因组完整性。负责piRNA生物发生的分子机制和组件仍然难以捉摸。 PIWI蛋白包含保守对称的二甲基精氨酸(sDMA),这些蛋白被含TUDOR域的蛋白特异性靶向。在这里,我们报告PIWI蛋白的sDMAs在家蚕衍生的BmN4细胞中具有PIWI生物发生机制的PIWI定位和piRNA生物发生中起关键作用。此外,对编码含有TUDOR域的蛋白质的Bombyx基因进行RNAi筛选后,将果蝇PAPI的Bombyx同源物BmPAPI鉴定为调节成熟piRNA长度的因素。 BmPAPI特异性识别sDMA,并与线粒体外膜表面的PIWI蛋白相互作用。 BmPAPI耗尽导致3? piRNA的末端延伸而不影响piRNA的数量。这些结果揭示了线粒体外膜支架上的BmPAPI参与的piRNA前体加工机制。

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