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In Search of Lost Small Peptides

机译:寻找失去的小肽

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摘要

A large body of evidence indicates that genome annotation pipelines have biased our view of coding sequences because they generally undersample small proteins and peptides. The recent development of genome-wide translation profiling reveals the prevalence of small/short open reading frames (smORFs or sORFs), which are scattered over all classes of transcripts, including both mRNAs and presumptive long noncodingRNAs. Proteomic approaches further confirm an unexpected variety of smORF-encoded peptides (SEPs), representing an overlooked reservoir of bioactive molecules. Indeed, functional studies in a broad range of species from yeast to humans demonstrate that SEPs can harbor key activities for the control of development, differentiation, and physiology. Here we summarize recent advances in the discovery and functional characterization of smORF/SEPs and discuss why these small players can no longer be ignored with regard to genome function.
机译:大量证据表明,基因组注释管道已经偏离了我们对编码序列的看法,因为它们通常是欠缺陷的小蛋白质和肽。 最近的基因组翻页的发展揭示了小/短开放阅读框架(Smorf或Sorfs)的患病率,它们分散在所有类别的转录物上,包括MRNA和推定长的非耦合rnas。 蛋白质组学方法进一步证实了一种意想不到的Smorf编码肽(SEP),代表了生物活性分子的被忽略的储存器。 实际上,在酵母到人类的广泛种类中的功能研究表明,SEPs可以涉及控制发展,分化和生理学的关键活动。 在这里,我们总结了最近在Smorf / Seps的发现和功能表征中的进展,并讨论了为什么在基因组功能方面不再忽略这些小玩家。

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