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通过tRNA切割将tRNA同功受体重新用于非规范功能。

Repurposing tRNA isodecoders for non-canonical functions via tRNA cleavage.

作者信息

Bhatter Nupur, Advani Vivek M, Takenaka Yoshika, Lyons Shawn M, Akiyama Yasutoshi, Anderson Paul J, Ivanov Pavel

出版信息

bioRxiv. 2024 Sep 4:2024.09.04.611212. doi: 10.1101/2024.09.04.611212.

Abstract

UNLABELLED

Transfer RNAs (tRNAs) are the key adaptor molecules aiding protein synthesis. Hundreds of tRNA genes are found in the human genome but the biological significance of this genetic excess is still enigmatic. The tRNA repertoires are variable between tissues and cells as well as during development. Such variations can only be partially explained by the correlation to the physiological needs in protein production, e.g. by changes in the expression of tRNA isoacceptor sets (tRNAs charged with the same amino acid but bearing different anticodons). However, changes in the expression levels of individual isodecoders (tRNAs with the same anticodon) are less understood. Besides canonical functions in mRNA translation, tRNAs are implicated in non-canonical functions unrelated to protein synthesis. tRNAs are rich source of small non-protein coding RNAs called tRNA-derived RNAs (tDRs), which include tRNA-derived stress-induced RNAs (tiRNAs) formed in response to stress. Here, we show that tiRNAs derived from isodecoders different in a single nucleotide can also differ in their activities. Specifically, we show that isodecoder sets for tRNA , tRNA and tRNA are cleaved by ribonucleases to yield 5'-tiRNAs showing differential activity towards mRNA reporter translation. Our data propose a model where cleavage repurposes specific tRNA isodecoders for non-canonical functions.

SIGNIFICANCE STATEMENT

The human genome encodes hundreds of transfer RNA (tRNA) genes to decode 61 codons. The basis for such genetic redundancy is unclear but the increase in the number of tRNA genes goes in concert with the complexity of an organism. While changes in the expression of isoacceptor tRNA pools can reflect adaptation to demanding protein synthesis needs and/or codon usage, the variations in the expression of the individual tRNA isodecoders are documented but poorly understood. Such expression variations are hypothesized to contribute to non-canonical tRNA functions, yet physiological relevance remains ambiguous. We report here that specific tRNA isodecoders can be functionally repurposed through cleavage that produces tRNA-derived RNAs (tDRs). The repurposing employs nucleotide variations in isodecoders leading to the production of distinct sets of tDRs with variable bioactivities.

摘要

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转运RNA(tRNA)是辅助蛋白质合成的关键衔接分子。人类基因组中发现了数百个tRNA基因,但这种基因冗余的生物学意义仍然是个谜。tRNA库在组织和细胞之间以及发育过程中是可变的。这种变化只能部分地通过与蛋白质生产中的生理需求的相关性来解释,例如通过tRNA同工受体集(携带相同氨基酸但具有不同反密码子的tRNA)表达的变化。然而,对单个同型译码器(具有相同反密码子的tRNA)表达水平的变化了解较少。除了在mRNA翻译中的经典功能外,tRNA还涉及与蛋白质合成无关的非经典功能。tRNA是称为tRNA衍生RNA(tDR)的小非蛋白质编码RNA的丰富来源,其中包括响应压力形成的tRNA衍生应激诱导RNA(tiRNA)。在这里,我们表明源自单个核苷酸不同的同型译码器的tiRNA在其活性上也可能不同。具体而言,我们表明tRNA 、tRNA 和tRNA 的同型译码器集被核糖核酸酶切割以产生对mRNA报告基因翻译具有不同活性的5'-tiRNA。我们的数据提出了一个模型,其中切割将特定的tRNA同型译码器重新用于非经典功能。

意义声明

人类基因组编码数百个转运RNA(tRNA)基因以解码61个密码子。这种基因冗余的基础尚不清楚,但tRNA基因数量的增加与生物体的复杂性相一致。虽然同工受体tRNA库表达的变化可以反映对苛刻的蛋白质合成需求和/或密码子使用的适应,但单个tRNA同型译码器表达的变化已有记录但了解甚少。这种表达变化被假设有助于tRNA的非经典功能,但其生理相关性仍然不明确。我们在此报告,特定的tRNA同型译码器可以通过产生tRNA衍生RNA(tDR)的切割在功能上重新利用。这种重新利用利用了同型译码器中的核苷酸变异,导致产生具有可变生物活性的不同tDR集。

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