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微小RNA(miRNA)通路内在地控制果蝇生殖系干细胞的自我更新。

The miRNA pathway intrinsically controls self-renewal of Drosophila germline stem cells.

作者信息

Park Joseph K, Liu Xiang, Strauss Tamara J, McKearin Dennis M, Liu Qinghua

机构信息

Department of Molecular Biology, University of Texas Southwestern Medical Center, Dallas, Texas 75390.

出版信息

Curr Biol. 2007 Mar 20;17(6):533-8. doi: 10.1016/j.cub.2007.01.060. Epub 2007 Feb 22.

Abstract

Stem cells uniquely self-renew and maintain tissue homoeostasis by differentiating into different cell types to replace aged or damaged cells [1]. During oogenesis of Drosophila melanogaster, self-renewal of germline stem cells (GSCs) requires both intrinsic signaling mechanisms and extrinsic signals from neighboring niche cells [2]. Emerging evidence suggests that microRNA (miRNA)-mediated translational regulation may also control Drosophila GSC self-renewal [3, 4]. It is unclear, however, whether the miRNA pathway functions within stem cells or niche cells to maintain GSCs. In Drosophila, Dicer-1 (Dcr-1) and the double-stranded RNA binding protein Loquacious (Loqs) catalyze miRNA biogenesis [3-5]. Here, we generate loqs knockout (loqs(KO)) flies by ends-out homologous recombination and show that loqs is essential for embryonic viability and ovarian GSC maintenance. Both developmental and miRNA processing defects are rescued by transgenic expression of Loqs-PB, but not Loqs-PA. Furthermore, mosaic germline analysis indicates that Loqs is required intrinsically for GSC maintenance. Consistently, GSCs are restored in loqs mutant ovaries by germline expression, but not somatic expression, of Loqs-PB. Together, these results demonstrate that Loqs-PB, but not Loqs-PA, is necessary and sufficient for Drosophila development and the miRNA pathway. Our study strongly suggests that miRNAs play an intrinsic, but not extrinsic, role in Drosophila female GSC self-renewal.

摘要

干细胞具有独特的自我更新能力,并通过分化为不同的细胞类型来维持组织稳态,以取代衰老或受损的细胞[1]。在黑腹果蝇的卵子发生过程中,生殖系干细胞(GSCs)的自我更新既需要内在信号机制,也需要来自邻近微环境细胞的外在信号[2]。新出现的证据表明,微小RNA(miRNA)介导的翻译调控也可能控制果蝇GSCs的自我更新[3,4]。然而,尚不清楚miRNA途径是在干细胞还是微环境细胞中发挥作用以维持GSCs。在果蝇中,Dicer-1(Dcr-1)和双链RNA结合蛋白Loquacious(Loqs)催化miRNA的生物合成[3-5]。在这里,我们通过末端外同源重组产生了loqs基因敲除(loqs(KO))果蝇,并表明loqs对于胚胎活力和卵巢GSCs的维持至关重要。Loqs-PB的转基因表达可以挽救发育和miRNA加工缺陷,但Loqs-PA则不能。此外,嵌合生殖系分析表明,Loqs对于GSCs的维持是内在必需的。一致地,通过生殖系表达Loqs-PB而非体细胞表达,可以在loqs突变体卵巢中恢复GSCs。总之,这些结果表明,Loqs-PB而非Loqs-PA对于果蝇发育和miRNA途径是必要且充分的。我们的研究强烈表明,miRNAs在果蝇雌性GSCs自我更新中发挥内在而非外在的作用。

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