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DEAD-box RNA helicase Belle/DDX3 and the RNA interference pathway promote mitotic chromosome segregation

机译:DEAD-box RNA解旋酶Belle / DDX3和RNA干扰途径促进有丝分裂染色体分离

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摘要

During mitosis, faithful inheritance of genetic material is achieved by chromosome segregation, as mediated by the condensin I and II complexes. Failed chromosome segregation can result in neoplasm formation, infertility, and birth defects. Recently, the germ-line–specific DEAD-box RNA helicase Vasa was demonstrated to promote mitotic chromosome segregation in Drosophila by facilitating robust chromosomal localization of Barren (Barr), a condensin I component. This mitotic function of Vasa is mediated by Aubergine and Spindle-E, which are two germ-line components of the Piwi-interacting RNA pathway. Faithful segregation of chromosomes should be executed both in germ-line and somatic cells. However, whether a similar mechanism also functions in promoting chromosome segregation in somatic cells has not been elucidated. Here, we present evidence that belle (vasa paralog) and the RNA interference pathway regulate chromosome segregation in Drosophila somatic cells. During mitosis, belle promotes robust Barr chromosomal localization and chromosome segregation. Belle's localization to condensing chromosomes depends on dicer-2 and argonaute2. Coimmunoprecipitation experiments indicated that Belle interacts with Barr and Argonaute2 and is enriched at endogenous siRNA (endo-siRNA)-generating loci. Our results suggest that Belle functions in promoting chromosome segregation in Drosophila somatic cells via the endo-siRNA pathway. DDX3 (human homolog of belle) and DICER function in promoting chromosome segregation and hCAP-H (human homolog of Barr) localization in HeLa cells, indicating a conserved function for those proteins in human cells. Our results suggest that the RNA helicase Belle/DDX3 and the RNA interference pathway perform a common role in regulating chromosome segregation in Drosophila and human somatic cells.
机译:在有丝分裂过程中,通过染色体分离实现了对遗传物质的忠实遗传,这是由凝聚素I和II复合体介导的。染色体分离失败会导致肿瘤形成,不育和出生缺陷。最近,已证明种系特异性DEAD-box RNA解旋酶Vasa通过促进Barden(Barr)(凝缩蛋白I成分)的稳健染色体定位来促进果蝇中的有丝分裂染色体分离。 Vasa的这种有丝分裂功能是由茄子和Spindle-E介导的,这是Piwi相互作用RNA途径的两个种系组成部分。染色体的忠实分离应该在种系和体细胞中进行。然而,尚未阐明类似的机制是否也能促进体细胞中的染色体分离。在这里,我们提供的证据表明,美女(vasa旁系同源物)和RNA干扰途径调节果蝇体细胞中的染色体分离。在有丝分裂期间,美女会促进鲁棒的Barr染色体定位和染色体分离。美女的缩合染色体定位取决于dicer-2和argonaute2。免疫共沉淀实验表明,Belle与Barr和Argonaute2相互作用,并在产生内源性siRNA(endo-siRNA)的位点富集。我们的结果表明,美女通过内在siRNA途径促进果蝇体细胞染色体分离。 DDX3(美女的人类同源物)和DICER在促进HeLa细胞中的染色体分离和hCAP-H(Barr的人类同源物)定位中起作用,表明这些蛋白质在人类细胞中具有保守的功能。我们的结果表明,RNA解旋酶Belle / DDX3和RNA干扰途径在调节果蝇和人类体细胞的染色体分离中起着共同的作用。

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    Pek, Jun Wei; Kai, Toshie;

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  • 年度 2011
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