Pathogenic mycobacteria are a significant cause of morbidity and mortality worldwide. The conserved whiB7 stress response reduces the effectiveness of antibiotic therapy by activating several intrinsic antibiotic resistance mechanisms. Despite our comprehensive biochemical understanding of WhiB7, the complex set of signals that induce whiB7 expression remain less clear. We employed a reporter-based, genome-wide CRISPRi epistasis screen to identify a diverse set of 150 mycobacterial genes whose inhibition results in constitutive whiB7 expression. We show that whiB7 expression is determined by the amino acid composition of the 5' regulatory uORF, thereby allowing whiB7 to sense amino acid starvation. Although deprivation of many amino acids can induce whiB7, whiB7 specifically coordinates an adaptive response to alanine starvation by engaging in a feedback loop with the alanine biosynthetic enzyme, aspC. These findings describe a metabolic function for whiB7 and help explain its evolutionary conservation across mycobacterial species occupying diverse ecological niches.
Beyond antibiotic resistance: The whiB7 transcription factor coordinates an adaptive response to alanine starvation in mycobacteria.
除了抗生素耐药性之外:whiB7 转录因子协调分枝杆菌对丙氨酸饥饿的适应性反应
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作者:Poulton Nicholas C, DeJesus Michael A, Munsamy-Govender Vanisha, Kanai Mariko, Roberts Cameron G, Azadian Zachary A, Bosch Barbara, Lin Karl Matthew, Li Shuqi, Rock Jeremy M
| 期刊: | Cell Chemical Biology | 影响因子: | 7.200 |
| 时间: | 2024 | 起止号: | 2024 Apr 18; 31(4):669-682 |
| doi: | 10.1016/j.chembiol.2023.12.020 | 研究方向: | 其它 |
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