a Department of Oncology-Pathology , Science for Life Laboratory, Karolinska Institutet , Stockholm , Sweden.
b Lady Davis Institute, SMBD Jewish General Hospital , Montreal , Canada.
RNA Biol. 2017 Oct 3;14(10):1299-1305. doi: 10.1080/15476286.2017.1290041. Epub 2017 Feb 10.
Translation is fundamental for many biologic processes as it enables cells to rapidly respond to stimuli without requiring de novo mRNA synthesis. The mammalian/mechanistic target of rapamycin (mTOR) is a key regulator of translation. Although mTOR affects global protein synthesis, translation of a subset of mRNAs appears to be exceptionally sensitive to changes in mTOR activity. Recent efforts to catalog these mTOR-sensitive mRNAs resulted in conflicting results. Whereas ribosome-profiling almost exclusively identified 5'-terminal oligopyrimidine (TOP) mRNAs as mTOR-sensitive, polysome-profiling suggested that mTOR also regulates translation of non-TOP mRNAs. This inconsistency was explained by analytical and technical biases limiting the efficiency of ribosome-profiling in detecting mRNAs showing differential translation. Moreover, genome-wide characterization of 5'UTRs of non-TOP mTOR-sensitive mRNAs revealed 2 subsets of transcripts which differ in their requirement for translation initiation factors and biologic functions. We summarize these recent advances and their impact on the understanding of mTOR-sensitive translation.
翻译对于许多生物过程至关重要,因为它使细胞能够快速响应刺激,而无需新合成 mRNA。哺乳动物/雷帕霉素靶蛋白(mTOR)是翻译的关键调节剂。尽管 mTOR 影响整体蛋白质合成,但一组 mRNA 的翻译似乎对 mTOR 活性的变化特别敏感。最近对这些 mTOR 敏感的 mRNAs 进行编目的努力产生了相互矛盾的结果。尽管核糖体分析几乎只鉴定出 5'-末端寡嘧啶(TOP)mRNA 是 mTOR 敏感的,但多核糖体分析表明 mTOR 也调节非 TOP mRNAs 的翻译。这种不一致性可以通过分析和技术偏差来解释,这些偏差限制了核糖体分析检测显示差异翻译的 mRNAs 的效率。此外,对非 TOP mTOR 敏感 mRNAs 的 5'UTR 的全基因组特征分析揭示了 2 个转录本亚组,它们在翻译起始因子和生物学功能的需求上有所不同。我们总结了这些最新进展及其对理解 mTOR 敏感翻译的影响。
