a Department of Medical Sciences and Institute of Biomedicine - iBiMED , University of Aveiro , Aveiro , Portugal.
b Expression Regulation in Cancer, Institute of Molecular Pathology and Immunology, University of Porto (IPATIMUP) , Porto , Portugal.
RNA Biol. 2018;15(6):773-786. doi: 10.1080/15476286.2018.1454244. Epub 2018 Jun 7.
Deregulation of tRNAs, aminoacyl-tRNA synthetases and tRNA modifying enzymes are common in cancer, raising the hypothesis that protein synthesis efficiency and accuracy (mistranslation) are compromised in tumors. We show here that human colon tumors and xenograft tumors produced in mice by two epithelial cancer cell lines mistranslate 2- to 4-fold more frequently than normal tissue. To clarify if protein mistranslation plays a role in tumor biology, we expressed mutant Ser-tRNAs that misincorporate Ser-at-Ala (frequent error) and Ser-at-Leu (infrequent error) in NIH3T3 cells and investigated how they responded to the proteome instability generated by the amino acid misincorporations. There was high tolerance to both misreading tRNAs, but the Ser-to-Ala misreading tRNA was a more potent inducer of cell transformation, stimulated angiogenesis and produced faster growing tumors in mice than the Ser-to-Leu misincorporating tRNA. Upregulation of the Akt pathway and the UPR were also observed. Most surprisingly, the relative expression of both misreading tRNAs increased during tumor growth, suggesting that protein mistranslation is advantageous in cancer contexts. These data highlight new features of protein synthesis deregulation in tumor biology.
tRNA、氨酰-tRNA 合成酶和 tRNA 修饰酶的失调在癌症中很常见,这就提出了一个假说,即在肿瘤中蛋白质合成的效率和准确性(错译)受到了损害。我们在这里表明,人类结肠肿瘤和由两种上皮癌细胞系在小鼠中产生的异种移植肿瘤的错译频率比正常组织高 2 到 4 倍。为了阐明蛋白质错译是否在肿瘤生物学中发挥作用,我们在 NIH3T3 细胞中表达了突变的 Ser-tRNA,这些 tRNA 会错误地将 Ser 掺入到 Ala(常见错误)和 Leu(罕见错误)中,并研究了它们如何对由氨基酸错配引起的蛋白质组不稳定性做出反应。这两种错读 tRNA 都有很高的耐受性,但 Ser-to-Ala 错读 tRNA 比 Ser-to-Leu 错读 tRNA 更能诱导细胞转化,刺激血管生成,并在小鼠中产生生长更快的肿瘤。还观察到 Akt 通路和 UPR 的上调。最令人惊讶的是,在肿瘤生长过程中,这两种错读 tRNA 的相对表达都增加了,这表明蛋白质错译在癌症环境中是有利的。这些数据突出了肿瘤生物学中蛋白质合成失调的新特征。
