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首页> 外文期刊>Gene expression >Genetic analysis of the basis of translation in the -1 frame of an unusual non-ORF sequence isolated from phage display.
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Genetic analysis of the basis of translation in the -1 frame of an unusual non-ORF sequence isolated from phage display.

机译:从噬菌体展示中分离出来的异常非ORF序列-1帧中翻译基础的遗传分析。

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摘要

An unusual peptide-encoding sequence, called H10, and several derivatives of this sequence were previously isolated from a random peptide library screened by phage display during drug discovery protocols. The H10 family of sequences had the unusual property of being expressed despite the absence of an open reading frame. When these sequences were fused to a reporter lacZ gene in all three frames, beta-galactosidase was expressed not only from the parental non-open reading frame, consistent with the original isolations, but also from the frame -1 to the parental. This unexpected translation in a second reading frame could result from either a recoding event or from an internal translation initiation event. In order to elucidate which type of event, a genetic approach was selected to eliminate a potential downstream initiator site within the H10 sequence. This report provides strong evidence that translation in the -1 frame in this family of sequences is indeed originating from a downstream translation initiation event. Unexpectedly, the mutation eliminating the downstream initiation event in the -1 frame simultaneously elevated expression in the original non-open reading frame.
机译:先前从药物发现方案期间通过噬菌体展示筛选的随机肽库中分离出了一个异常的肽编码序列,称为H10,以及该序列的几种衍生物。尽管没有开放阅读框,H10家族序列仍具有表达的异常特性。当在所有三个框架中将这些序列与报告基因lacZ基因融合时,不仅从亲本的非开放阅读框表达了β-半乳糖苷酶,与最初的分离相符,而且从框架-1到亲本表达了β-半乳糖苷酶。第二个阅读框中的这种意外翻译可能是由于重新编码事件或内部翻译启动事件引起的。为了阐明事件的类型,选择了一种遗传方法来消除H10序列中潜在的下游启动子位点。该报告提供了有力的证据,表明该序列家族中-1框内的翻译确实来自下游翻译起始事件。出乎意料的是,该突变消除了-1帧中的下游启动事件,同时提高了原始非开放阅读框中的表达。

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