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翻译起始因子 eIF3h 在胚胎发生过程中将特定的转录本靶向多核糖体。

Translation initiation factor eIF3h targets specific transcripts to polysomes during embryogenesis.

机构信息

Department of Developmental and Molecular Biology, Albert Einstein College of Medicine of Yeshiva University, Bronx, NY 10461, USA.

出版信息

Proc Natl Acad Sci U S A. 2013 Jun 11;110(24):9818-23. doi: 10.1073/pnas.1302934110. Epub 2013 May 28.

Abstract

Eukaryotic translation initiation factor 3 (eIF3) plays a central role in translation initiation and consists of five core (conserved) subunits present in both budding yeast and higher eukaryotes. Higher eukaryotic eIF3 contains additional (noncore or nonconserved) subunits of poorly defined function, including sub-unit h (eIF3h), which in zebrafish is encoded by two distinct genes (eif3ha and eif3hb). Previously we showed that eif3ha encodes the predominant isoform during zebrafish embryogenesis and that depletion of this factor causes defects in the development of the brain and eyes. To investigate the molecular mechanism governing this regulation, we developed a genome-wide polysome-profiling strategy using stage-matched WT and eif3ha morphant zebrafish embryos. This strategy identified a large set of predominantly neural-associated translationally regulated mRNAs. A striking finding was a cohort of lens-associated crystallin isoform mRNAs lost from the eif3ha morphant polysomes, revealing a mechanism by which lens development is translationally controlled. We show that both UTR sequences of a targeted crystallin transcript are necessary but not sufficient for translational regulation by eif3ha. Therefore, our study reveals the role of a noncore eIF3 subunit in modulating a specific developmental program by regulating translation of defined transcripts and highlights the potential of the zebrafish system to identify translational regulatory mechanisms controlling vertebrate development.

摘要

真核翻译起始因子 3(eIF3)在翻译起始中发挥核心作用,由在芽殖酵母和高等真核生物中都存在的五个核心(保守)亚基组成。高等真核生物的 eIF3 含有功能尚未明确的额外(非核心或非保守)亚基,包括亚基 h(eIF3h),在斑马鱼中由两个不同的基因(eif3ha 和 eif3hb)编码。之前我们表明,eif3ha 在斑马鱼胚胎发生期间编码主要的同工型,并且该因子的耗竭导致大脑和眼睛发育缺陷。为了研究调控这种调控的分子机制,我们使用匹配阶段的 WT 和 eif3ha 突变体斑马鱼胚胎开发了一种全基因组多核糖体谱分析策略。该策略鉴定了一组主要与神经相关的翻译调节 mRNA。一个显著的发现是,从 eif3ha 突变体多核糖体中丢失了一组与晶状体相关的晶体蛋白同工型 mRNA,揭示了晶状体发育的翻译控制机制。我们表明,靶向晶体转录物的 UTR 序列对于 eif3ha 的翻译调控是必需的但不是充分的。因此,我们的研究揭示了非核心 eIF3 亚基通过调节特定转录物的翻译来调节特定发育程序的作用,并强调了斑马鱼系统在鉴定控制脊椎动物发育的翻译调节机制方面的潜力。

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