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A novel signature for identification of upstream alternative translation initiation sites

机译:用于识别上游替代翻译起始位点的新颖签名

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Alternative translation initiation sites (aTIS) and the factors that determine an ideal mode of translation of mRNA in the eukaryotic system has been widely studied over the past several decades. Such studies demonstrate that single mRNA can yield multiple protein isoforms using the AUG and non-AUG start codons. While the conspicuous scanning model explains how the process of translation initiation begins when the pre-initiation complex encounters a start codon with optimal sequence context, referred to as “Kozak” consensus and the leaky scanning model explains the process of alternative translation downstream. Additionally, there are alternative translation initiation sites upstream and in-frame to the canonical AUG start site, which are present in the 5' UTR of the mRNA. This choice of aTIS results in a longer N-terminally expanded protein isoform. It is unclear as to what are the factors that determine the selection of a start codon to be a potential upstream aTIS. In this study we investigate if there exists a third element, besides the sequence context at a certain distance from canonical AUG start codon, in the 5' UTR of human mRNAs called the “complementary matching palindrome” that differentiates an upstream aTIS from any other codon. Our results show the presence of longest complementary matching palindrome around CUG codon, which may serve as an aTIS to translate proteins that are longer than their canonical isoforms.
机译:在过去的几十年中,替代翻译起始位点(aTIS)和确定真核系统中mRNA理想翻译模式的因素已得到广泛研究。此类研究表明,使用AUG和非AUG起始密码子,单个mRNA可以产生多种蛋白质同工型。显眼的扫描模型解释了当预启动复合体遇到具有最佳序列上下文的起始密码子时,翻译起始过程如何开始,这被称为“ Kozak”共识,而泄漏扫描模型解释了下游替代翻译的过程。另外,在规范的AUG起始位点的上游和框内还有替代的翻译起始位点,它们存在于mRNA的5'UTR中。选择aTIS会导致更长的N端扩展蛋白同工型。目前尚不清楚哪些因素决定了选择起始密码子作为潜在的上游aTIS。在这项研究中,我们研究了人类mRNA的5'UTR中距规范AUG起始密码子有一定距离的序列上下文之外是否存在第三种元素,称为“互补匹配回文”,该区别可将上游aTIS与任何其他密码子区分开。我们的结果表明,在CUG密码子附近存在最长的互补匹配回文,它可以作为aTIS来翻译比其规范同种型更长的蛋白质。

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