首页> 美国卫生研究院文献>The EMBO Journal >EDEN and EDEN-BP a cis element and an associated factor that mediate sequence-specific mRNA deadenylation in Xenopus embryos.
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EDEN and EDEN-BP a cis element and an associated factor that mediate sequence-specific mRNA deadenylation in Xenopus embryos.

机译:EDEN和EDEN-BP一种介导爪蟾胚胎中序列特异性mRNA腺苷酸化的顺式元件和相关因子。

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摘要

During Xenopus early development, gene expression is regulated mainly at the translational level by the length of the poly(A) tail of mRNAs. The Eg family and c-mos maternal mRNAs are deadenylated rapidly and translationally repressed after fertilization. Here, we characterize a short sequence element (EDEN) responsible for the rapid deadenylation of Eg5 mRNA. Determining the core EDEN sequence permitted us to localize the c-mos EDEN sequence. The c-mos EDEN confered a rapid deadenylation to a reporter gene. The EDEN-specific RNA-binding protein (EDEN-BP) was purified and a cDNA obtained. EDEN-BP is highly homologous to a human protein possibly involved in myotonic dystrophy. Immunodepleting EDEN-BP from an egg extract totally abolished the EDEN-mediated deadenylation activity, but did not affect the default deadenylation activity. Therefore, EDEN-BP constitutes the first trans-acting factor for which an essential role in the specificity of mRNA deadenylation has been directly demonstrated.
机译:在非洲爪蟾的早期发育过程中,基因表达主要在翻译水平受到mRNA的poly(A)尾巴长度的调节。 Eg家族和c-mos母体mRNA迅速去甲腺苷酸化,受精后被翻译抑制。在这里,我们表征了负责Eg5 mRNA快速去甲腺苷酸化的短序列元件(EDEN)。确定核心EDEN序列使我们能够定位c-mos EDEN序列。 c-mos EDEN赋予报告基因快速的去烯基化作用。纯化EDEN特异性RNA结合蛋白(EDEN-BP)并获得cDNA。 EDEN-BP与可能与强直性营养不良有关的人类蛋白质高度同源。从蛋提取物中对EDEN-BP进行不饱和处理完全消除了EDEN介导的去烯基化活性,但没有影响默认的去烯基化活性。因此,EDEN-BP构成了第一个反式作用因子,已直接证明了其在mRNA腺苷酸化特异性中的重要作用。

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