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多种机制协同作用以抑制果蝇卵巢和胚胎中的 nanos 翻译。

Multiple mechanisms collaborate to repress nanos translation in the Drosophila ovary and embryo.

机构信息

Department of Molecular Biology, Princeton University, Princeton, New Jersey 08544, USA.

出版信息

RNA. 2011 May;17(5):967-77. doi: 10.1261/rna.2478611. Epub 2011 Apr 1.

Abstract

Translational control of gene expression is essential for development in organisms that rely on maternal mRNAs. In Drosophila, translation of maternal nanos (nos) mRNA must be restricted to the posterior of the early embryo for proper patterning of the anterior-posterior axis. Spatial control of nos translation is coordinated through the localization of a small subset of nos mRNA to the posterior pole late in oogenesis, activation of this localized mRNA, and repression of the remaining unlocalized nos mRNA throughout the bulk cytoplasm. Translational repression is mediated by the interaction of a cis-acting element in the nos 3' untranslated region with two proteins, Glorund (Glo) and Smaug (Smg), that function in the oocyte and embryo, respectively. The mechanism of Glo-dependent repression is unknown. Previous work suggests that Smg represses translation initiation but this model is not easily reconciled with evidence for polysome association of repressed nos mRNA. Using an in vitro translation system, we have decoupled translational repression of nos imposed during oogenesis from repression during embryogenesis. Our results suggest that both Glo and Smg regulate translation initiation, but by different mechanisms. Furthermore, we show that, during late oogenesis, nos translation is also repressed post-initiation and provide evidence that Glo mediates this event. This post-initiation block is maintained into embryogenesis during the transition to Smg-dependent regulation. We propose that the use of multiple modes of repression ensures inactivation of nos RNA that is translated at earlier stages of oogenesis and maintenance of this inactivate state throughout late oogenesis into embryogenesis.

摘要

基因表达的翻译调控对于依赖母体 mRNA 的生物体的发育至关重要。在果蝇中,母体 nanos(nos)mRNA 的翻译必须限制在早期胚胎的后部,以正确构建前后轴的模式。nos 翻译的空间调控是通过一小部分 nos mRNA 在后生卵母细胞晚期定位于后极来协调的,这一小部分 nos mRNA 被激活,而其余未定位的 nos mRNA 在整个细胞质中被抑制。翻译抑制是由 nos 3'非翻译区中的顺式作用元件与两个蛋白质 Glorund(Glo)和 Smaug(Smg)相互作用介导的,这两个蛋白质分别在卵母细胞和胚胎中发挥作用。Glo 依赖性抑制的机制尚不清楚。先前的工作表明 Smg 抑制翻译起始,但这种模型与抑制物对未定位的 nos mRNA 的多核糖体结合的证据不太吻合。使用体外翻译系统,我们已经将母体期 nos 所施加的翻译抑制与胚胎期的抑制分离开来。我们的结果表明,Glo 和 Smg 都调节翻译起始,但机制不同。此外,我们表明,在后生卵母细胞晚期,nos 翻译也被起始后抑制,并提供了证据表明 Glo 介导了这一事件。这种起始后阻断在向 Smg 依赖调节的转变过程中一直维持到胚胎期。我们提出,使用多种抑制模式可确保在早期卵母细胞中翻译的 nos RNA 失活,并在整个后期卵母细胞到胚胎期维持这种失活状态。

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