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激活素信号传导平衡卵巢生态位前体细胞的增殖和分化,并能调节生态位数量。

Activin signaling balances proliferation and differentiation of ovarian niche precursors and enables adjustment of niche numbers.

作者信息

Lengil Tamar, Gancz Dana, Gilboa Lilach

机构信息

Department of Biological regulation, Weizmann Institute of Science, Rehovot 76100, Israel.

Department of Biological regulation, Weizmann Institute of Science, Rehovot 76100, Israel

出版信息

Development. 2015 Mar 1;142(5):883-92. doi: 10.1242/dev.113902. Epub 2015 Jan 29.

DOI:10.1242/dev.113902
PMID:25633355
Abstract

How the numbers of niches and resident stem cells within a particular organ are determined during development and how they may be modulated or corrected is a question with significant medical implications. In the larval ovary of Drosophila melanogaster, somatic precursors for niches, and germ cells that will become germline stem cells, co-develop. Somatic precursors proliferate during the first 3 days of larval development. By mid-third instar, adult terminal filament (TF) (part of the germline stem cell niche) cells first appear, and differentiation terminates 24 h later when 16-20 TFs fully form. The developmental sequence responsible for TF cell determination and final TF numbers is only partially understood. We show that TF formation proceeds through several, hitherto uncharacterized stages, which include an early exit from the cell cycle to form TF precursors and two steps of cell shape change to form the mature TF cells. The Activin receptor Baboon (Babo) is required for somatic precursor cell proliferation and therefore determines the pool of TF precursors available for TF differentiation. During the final differentiation stage, Babo facilitates TF and germ cell differentiation, and promotes the accumulation of Broad-Z1, which is also a target of the steroid hormone ecdysone. Epistasis analysis shows that Activin controls cell proliferation in an ecdysone-independent manner and TF differentiation by affecting ecdysone targets. We propose that this mode of function allows Activin to balance proliferation and differentiation, and to equilibrate niche numbers. These results suggest a novel model for how niche numbers are corrected during development.

摘要

在发育过程中,特定器官内小生境和驻留干细胞的数量是如何确定的,以及它们如何被调节或纠正,这是一个具有重大医学意义的问题。在黑腹果蝇的幼虫卵巢中,小生境的体细胞前体和将成为生殖系干细胞的生殖细胞共同发育。体细胞前体在幼虫发育的前3天增殖。到三龄中期,成年终丝(TF)(生殖系干细胞小生境的一部分)细胞首次出现,16 - 20根终丝完全形成后24小时,分化终止。负责终丝细胞确定和最终终丝数量的发育序列仅被部分理解。我们发现终丝形成经历了几个迄今未被描述的阶段,包括早期退出细胞周期以形成终丝前体,以及两步细胞形状变化以形成成熟的终丝细胞。激活素受体狒狒(Babo)是体细胞前体细胞增殖所必需的,因此决定了可用于终丝分化的终丝前体库。在最终分化阶段,Babo促进终丝和生殖细胞分化,并促进Broad-Z1的积累,Broad-Z1也是类固醇激素蜕皮激素的靶标。上位性分析表明,激活素以蜕皮激素非依赖的方式控制细胞增殖,并通过影响蜕皮激素靶标来控制终丝分化。我们提出这种功能模式使激活素能够平衡增殖和分化,并平衡小生境数量。这些结果提示了一个关于发育过程中小生境数量如何被纠正的新模型。

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