Fungal pathogens threaten ecosystems and human health. Understanding the molecular basis of their virulence is key to develop new treatment strategies. Here, we characterize NCS2*, a point mutation identified in a clinical baker's yeast isolate. Ncs2 is essential for 2-thiolation of tRNA and the NCS2* mutation leads to increased thiolation at body temperature. NCS2* yeast exhibits enhanced fitness when grown at elevated temperatures or when exposed to oxidative stress, inhibition of nutrient signalling, and cell-wall stress. Importantly, Ncs2* alters the interaction and stability of the thiolase complex likely mediated by nucleotide binding. The absence of 2-thiolation abrogates the in vivo virulence of pathogenic baker's yeast in infected mice. Finally, hypomodification triggers changes in colony morphology and hyphae formation in the common commensal pathogen Candida albicans resulting in decreased virulence in a human cell culture model. These findings demonstrate that 2-thiolation of tRNA acts as a key mediator of fungal virulence and reveal new mechanistic insights into the function of the highly conserved tRNA-thiolase complex.
Ncs2* mediates in vivo virulence of pathogenic yeast through sulphur modification of cytoplasmic transfer RNA.
Ncs2*通过对细胞质转移RNA进行硫修饰来介导致病酵母的体内毒力
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作者:Alings Fiona, Scharmann Karin, Eggers Cristian, Böttcher Bettina, SokoÅowski MikoÅaj, Shvetsova Ekaterina, Sharma Puneet, Roth Joël, Rashiti Leon, Glatt Sebastian, Brunke Sascha, Leidel Sebastian A
| 期刊: | Nucleic Acids Research | 影响因子: | 13.100 |
| 时间: | 2023 | 起止号: | 2023 Aug 25; 51(15):8133-8149 |
| doi: | 10.1093/nar/gkad564 | 种属: | Yeast |
| 研究方向: | 细胞生物学 | ||
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