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GLD-4介导的翻译激活调节成年秀丽隐杆线虫生殖系中增殖性生殖细胞池的大小。

GLD-4-mediated translational activation regulates the size of the proliferative germ cell pool in the adult C. elegans germ line.

作者信息

Millonigg Sophia, Minasaki Ryuji, Nousch Marco, Novak Jakub, Eckmann Christian R

机构信息

Max Planck Institute of Molecular Cell Biology and Genetics (MPI-CBG), Dresden, Germany.

出版信息

PLoS Genet. 2014 Sep 25;10(9):e1004647. doi: 10.1371/journal.pgen.1004647. eCollection 2014 Sep.

Abstract

To avoid organ dysfunction as a consequence of tissue diminution or tumorous growth, a tight balance between cell proliferation and differentiation is maintained in metazoans. However, cell-intrinsic gene expression mechanisms controlling adult tissue homeostasis remain poorly understood. By focusing on the adult Caenorhabditis elegans reproductive tissue, we show that translational activation of mRNAs is a fundamental mechanism to maintain tissue homeostasis. Our genetic experiments identified the Trf4/5-type cytoplasmic poly(A) polymerase (cytoPAP) GLD-4 and its enzymatic activator GLS-1 to perform a dual role in regulating the size of the proliferative zone. Consistent with a ubiquitous expression of GLD-4 cytoPAP in proliferative germ cells, its genetic activity is required to maintain a robust proliferative adult germ cell pool, presumably by regulating many mRNA targets encoding proliferation-promoting factors. Based on translational reporters and endogenous protein expression analyses, we found that gld-4 activity promotes GLP-1/Notch receptor expression, an essential factor of continued germ cell proliferation. RNA-protein interaction assays documented also a physical association of the GLD-4/GLS-1 cytoPAP complex with glp-1 mRNA, and ribosomal fractionation studies established that GLD-4 cytoPAP activity facilitates translational efficiency of glp-1 mRNA. Moreover, we found that in proliferative cells the differentiation-promoting factor, GLD-2 cytoPAP, is translationally repressed by the stem cell factor and PUF-type RNA-binding protein, FBF. This suggests that cytoPAP-mediated translational activation of proliferation-promoting factors, paired with PUF-mediated translational repression of differentiation factors, forms a translational control circuit that expands the proliferative germ cell pool. Our additional genetic experiments uncovered that the GLD-4/GLS-1 cytoPAP complex promotes also differentiation, forming a redundant translational circuit with GLD-2 cytoPAP and the translational repressor GLD-1 to restrict proliferation. Together with previous findings, our combined data reveals two interconnected translational activation/repression circuitries of broadly conserved RNA regulators that maintain the balance between adult germ cell proliferation and differentiation.

摘要

为避免因组织萎缩或肿瘤生长导致器官功能障碍,后生动物维持着细胞增殖与分化之间的严格平衡。然而,控制成体组织稳态的细胞内在基因表达机制仍知之甚少。通过聚焦于成年秀丽隐杆线虫的生殖组织,我们发现mRNA的翻译激活是维持组织稳态的一种基本机制。我们的遗传学实验确定了Trf4/5型细胞质聚腺苷酸聚合酶(cytoPAP)GLD-4及其酶激活剂GLS-1在调节增殖区大小方面发挥双重作用。鉴于GLD-4 cytoPAP在增殖性生殖细胞中普遍表达,其遗传活性对于维持强大的成体增殖性生殖细胞库是必需的,大概是通过调控许多编码促进增殖因子的mRNA靶点来实现的。基于翻译报告基因和内源性蛋白质表达分析,我们发现gld-4活性促进GLP-1/Notch受体表达,这是生殖细胞持续增殖的一个关键因素。RNA-蛋白质相互作用分析还证明了GLD-4/GLS-1 cytoPAP复合物与glp-1 mRNA存在物理关联,核糖体分级分离研究表明GLD-4 cytoPAP活性促进glp-1 mRNA的翻译效率。此外,我们发现,在增殖细胞中,促进分化的因子GLD-2 cytoPAP受到干细胞因子和PUF型RNA结合蛋白FBF的翻译抑制。这表明,cytoPAP介导的促进增殖因子的翻译激活,与PUF介导的分化因子的翻译抑制相结合,形成了一个翻译控制回路,扩大了增殖性生殖细胞库。我们进一步的遗传学实验发现,GLD-4/GLS-1 cytoPAP复合物也促进分化,与GLD-2 cytoPAP和翻译抑制因子GLD-1形成一个冗余的翻译回路来限制增殖。与之前的研究结果一起,我们的综合数据揭示了两个相互关联的翻译激活/抑制回路,这些回路由广泛保守的RNA调节因子组成,维持着成体生殖细胞增殖与分化之间的平衡。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6fa5/4177745/87a54b837383/pgen.1004647.g001.jpg

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