RNA 结合调控级联控制果蝇雄性生殖系干细胞系从增殖到分化的转换

Devon E Harris, Jongmin J Kim, Sarah R Stern, Hannah M Vicars, Neuza R Matias, Lorenzo Gallicchio, Catherine C Baker, Margaret T Fuller
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摘要

成体干细胞系从前体细胞增殖到开始分化的转换必须经过仔细调节,以产生足够的后代来维持和修复组织,同时防止过度增殖,以免导致肿瘤发生。在果蝇雄性生殖细胞系中,由生殖系干细胞产生的精原细胞在转入精母细胞程序之前,要经历有限次数的有丝分裂中转放大分裂,以启动减数分裂和最终的精子分化。有丝分裂的次数由大理石袋(Bam)蛋白积累到临界阈值决定。在 Bam 突变体中,精原细胞通过几轮额外的有丝分裂增殖,然后在没有成为精母细胞的情况下死亡。在这里,我们发现 Bam 在有丝分裂到分化的转换过程中的关键作用是抑制哺乳动物 Quaking 的同源物 Held Out Wings(how)的表达。敲除生殖细胞中的how足以使bam突变的精原细胞或其伴侣良性绒毛膜细胞瘤(bgcn)分化,而在bam野生型精原细胞中强制表达核靶向How蛋白则会导致精原细胞继续增殖而牺牲分化。我们的研究结果表明,Bam通过结合CCR4-NOT的亚基Caf40,作为适配器招募CCR4-NOT去淀粉化复合物,从而靶向降解how RNA。由于How本身是一种RNA结合蛋白,在RNA加工中发挥作用,我们的研究结果揭示了果蝇雄性生殖系成体干细胞系中从增殖到减数分裂和分化的转换是由一连串RNA结合蛋白调控的。
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An RNA binding regulatory cascade controls the switch from proliferation to differentiation in the Drosophila male germ line stem cell lineage
The switch from precursor cell proliferation to onset of differentiation in adult stem cell lineages must be carefully regulated to produce sufficient progeny to maintain and repair tissues, yet prevent overproliferation that may enable oncogenesis. In the Drosophila male germ cell lineage, spermatogonia produced by germ line stem cells undergo a limited number of transit amplifying mitotic divisions before switching to the spermatocyte program that sets up meiosis and eventual spermatid differentiation. The number of transit amplifying divisions is set by accumulation of the bag-of-marbles (Bam) protein to a critical threshold. In bam mutants, spermatogonia proliferate through several extra rounds of mitosis then die without becoming spermatocytes. Here we show that the key role of Bam for the mitosis to differentiation switch is repressing expression of Held Out Wings (how), homolog of mammalian Quaking. Knock down of how in germ cells was sufficient to allow spermatogonia mutant for bam or its partner benign gonial cell neoplasm (bgcn) to differentiate, while forced expression of nuclear-targeted How protein in spermatogonia wild-type for bam resulted in continued proliferation at the expense of differentiation. Our findings suggest that Bam targets how RNA for degradation by acting as an adapter to recruit the CCR4-NOT deadenylation complex via binding its subunit, Caf40. As How is itself an RNA binding protein with roles in RNA processing, our findings reveal that the switch from proliferation to meiosis and differentiation in the Drosophila male germ line adult stem cell lineage is regulated by a cascade of RNA-binding proteins.
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