3' UTRs通过在蛋白质合成过程中提供一个培育生态位来调节蛋白质功能。

Christine Mayr
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引用次数: 7

摘要

信使rna (mrna)是蛋白质合成的模板,因为编码区被翻译成氨基酸序列。mrna还含有3'非翻译区(3' utr),其中含有用于调节蛋白质功能的额外元件。如果一个蛋白质的氨基酸序列是其功能所必需和充分的,我们称之为3' utr独立的。相反,由需要特定3' UTR存在的蛋白质复合物完成的功能是3' UTR依赖的蛋白质功能。我们发现3' UTRs可以在不影响蛋白质丰度的情况下调节蛋白质活性,而替代的3' UTRs可以使蛋白质功能多样化。我们目前认为,蛋白质合成位点的局部环境促进了3' utr对蛋白质功能的调节,我们称之为新生蛋白质的培育生态位。这个生态位由mRNA和结合蛋白组成,结合蛋白由rna结合蛋白和募集蛋白组成。它能够形成特定的蛋白质复合物,如最近发现的细胞质无膜细胞器TIS颗粒所示。这一发现表明,改变新生蛋白质的生态位将改变蛋白质的活性和功能,这意味着细胞质无膜细胞器可以以一种独立于蛋白质丰度的方式调节蛋白质功能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

3' UTRs Regulate Protein Functions by Providing a Nurturing Niche during Protein Synthesis.

3' UTRs Regulate Protein Functions by Providing a Nurturing Niche during Protein Synthesis.

3' UTRs Regulate Protein Functions by Providing a Nurturing Niche during Protein Synthesis.

3' UTRs Regulate Protein Functions by Providing a Nurturing Niche during Protein Synthesis.

Messenger RNAs (mRNAs) are the templates for protein synthesis as the coding region is translated into the amino acid sequence. mRNAs also contain 3' untranslated regions (3' UTRs) that harbor additional elements for the regulation of protein function. If the amino acid sequence of a protein is necessary and sufficient for its function, we call it 3' UTR-independent. In contrast, functions that are accomplished by protein complexes whose formation requires the presence of a specific 3' UTR are 3' UTR-dependent protein functions. We showed that 3' UTRs can regulate protein activity without affecting protein abundance, and alternative 3' UTRs can diversify protein functions. We currently think that the regulation of protein function by 3' UTRs is facilitated by the local environment at the site of protein synthesis, which we call the nurturing niche for nascent proteins. This niche is composed of the mRNA and the bound proteins that consist of RNA-binding proteins and recruited proteins. It enables the formation of specific protein complexes, as was shown for TIS granules, a recently discovered cytoplasmic membraneless organelle. This finding suggests that changing the niche for nascent proteins will alter protein activity and function, implying that cytoplasmic membraneless organelles can regulate protein function in a manner that is independent of protein abundance.

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