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3'tsRNAs 被氨酰化:对其生物发生的影响。

The 3'tsRNAs are aminoacylated: Implications for their biogenesis.

机构信息

Department of Pediatrics, Stanford University, Stanford, California, United States of America.

Department of Genetics, Stanford University, Stanford, Califormia, United States of America.

出版信息

PLoS Genet. 2021 Jul 29;17(7):e1009675. doi: 10.1371/journal.pgen.1009675. eCollection 2021 Jul.

Abstract

Emerging evidence indicates that tRNA-derived small RNAs (tsRNAs) are involved in fine-tuning gene expression and become dysregulated in various cancers. We recently showed that the 22nt LeuCAG3´tsRNA from the 3´ end of tRNALeu is required for efficient translation of a ribosomal protein mRNA and ribosome biogenesis. Inactivation of this 3´tsRNA induced apoptosis in rapidly dividing cells and suppressed the growth of a patient-derived orthotopic hepatocellular carcinoma in mice. The mechanism involved in the generation of the 3´tsRNAs remains elusive and it is unclear if the 3´-ends of 3´tsRNAs are aminoacylated. Here we report an enzymatic method utilizing exonuclease T to determine the 3´charging status of tRNAs and tsRNAs. Our results showed that the LeuCAG3´tsRNA, and two other 3´tsRNAs are fully aminoacylated. When the leucyl-tRNA synthetase (LARS1) was inhibited, there was no change in the total tRNALeu concentration but a reduction in both the charged tRNALeu and LeuCAG3´tsRNA, suggesting the 3´tsRNAs are fully charged and originated solely from the charged mature tRNA. Altering LARS1 expression or the expression of various tRNALeu mutants were also shown to affect the generation of the LeuCAG3´tsRNA further suggesting they are created in a highly regulated process. The fact that the 3´tsRNAs are aminoacylated and their production is regulated provides additional insights into their importance in post-transcriptional gene regulation that includes coordinating the production of the protein synthetic machinery.

摘要

新出现的证据表明,tRNA 衍生的小 RNA(tsRNA)参与微调基因表达,并在各种癌症中失调。我们最近表明,来自 tRNALeu3'端的 22nt LeuCAG3' tsRNA 对于核糖体蛋白 mRNA 的有效翻译和核糖体生物发生是必需的。这种 3' tsRNA 的失活会诱导快速分裂细胞的凋亡,并抑制患者来源的原位肝癌在小鼠中的生长。产生 3' tsRNA 的机制仍不清楚,也不清楚 3' tsRNA 的 3'端是否被氨酰化。在这里,我们报告了一种利用核酸外切酶 T 的酶促方法来确定 tRNA 和 tsRNA 的 3'氨酰化状态。我们的结果表明,LeuCAG3' tsRNA 和另外两种 3' tsRNA 完全被氨酰化。当抑制亮氨酰-tRNA 合成酶(LARS1)时,总 tRNALeu 浓度没有变化,但带电荷的 tRNALeu 和 LeuCAG3' tsRNA 减少,这表明 3' tsRNA 完全被氨酰化,并且仅源自带电荷的成熟 tRNA。改变 LARS1 的表达或各种 tRNALeu 突变体的表达也会影响 LeuCAG3' tsRNA 的产生,这进一步表明它们是在高度调控的过程中产生的。3' tsRNA 被氨酰化及其产生受到调控的事实为它们在包括协调蛋白质合成机制产生的转录后基因调控中的重要性提供了更多的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6669/8354468/de0268454b9c/pgen.1009675.g001.jpg

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