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Evidence that tRNA modifying enzymes are important in vivo targets for 5-fluorouracil in yeast.

机译:tRNA修饰酶是酵母中5-氟尿嘧啶的重要体内靶标的证据。

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摘要

We have screened a collection of haploid yeast knockout strains for increased sensitivity to 5-fluorouracil (5-FU). A total of 138 5-FU sensitive strains were found. Mutants affecting rRNA and tRNA maturation were particularly sensitive to 5-FU, with the tRNA methylation mutant trm10 being the most sensitive mutant. This is intriguing since trm10, like many other tRNA modification mutants, lacks a phenotype under normal conditions. However, double mutants for nonessential tRNA modification enzymes are frequently temperature sensitive, due to destabilization of hypomodified tRNAs. We therefore tested if the sensitivity of our mutants to 5-FU is affected by the temperature. We found that the cytotoxic effect of 5-FU is strongly enhanced at 38 degrees C for tRNA modification mutants. Furthermore, tRNA modification mutants show similar synthetic interactions for temperature sensitivity and sensitivity to 5-FU. A model is proposed for how 5-FU kills these mutants by reducing the number of tRNA modifications, thus destabilizing tRNA. Finally, we found that also wild-type cells are temperature sensitive at higher concentrations of 5-FU. This suggests that tRNA destabilization contributes to 5-FU cytotoxicity in wild-type cells and provides a possible explanation why hyperthermia can enhance the effect of 5-FU in cancer therapy.
机译:我们筛选了单倍体酵母基因敲除菌株集合,以提高对5-氟尿嘧啶(5-FU)的敏感性。共发现138株5-FU敏感菌株。影响rRNA和tRNA成熟的突变体对5-FU特别敏感,其中tRNA甲基化突变体trm10是最敏感的突变体。有趣的是,与许多其他tRNA修饰突变体一样,trm10在正常条件下也缺乏表型。但是,非必需的tRNA修饰酶的双突变体通常对温度敏感,这是因为低修饰的tRNA不稳定。因此,我们测试了突变体对5-FU的敏感性是否受温度影响。我们发现,对于tRNA修饰突变体,在38°C时5-FU的细胞毒性作用被大大增强。此外,tRNA修饰突变体在温度敏感性和对5-FU敏感性方面显示出相似的合成相互作用。针对5-FU如何通过减少tRNA修饰数量从而破坏tRNA的稳定性来杀死这些突变体提出了一个模型。最后,我们发现野生型细胞在更高浓度的5-FU下也对温度敏感。这表明tRNA去稳定化导致野生型细胞中5-FU的细胞毒性,并为热疗为何能增强5-FU在癌症治疗中的作用提供了可能的解释。

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