Department of Immunology and Infectious Diseases, Harvard T. H. Chan School of Public Health, Boston, Massachusetts, USA.
Division of Infectious Diseases, Brigham and Women's Hospital, Boston, Massachusetts, USA.
mBio. 2023 Feb 28;14(1):e0346922. doi: 10.1128/mbio.03469-22. Epub 2023 Jan 25.
Enzymes involved in rescuing stalled ribosomes and recycling translation machinery are ubiquitous in bacteria and required for growth. Peptidyl tRNA drop-off is a type of abortive translation that results in the release of a truncated peptide that is still bound to tRNA (peptidyl tRNA) into the cytoplasm. Peptidyl tRNA hydrolase (Pth) recycles the released tRNA by cleaving off the unfinished peptide and is essential in most bacteria. We developed a sequencing-based strategy called copper sulfate-based tRNA sequencing (Cu-tRNAseq) to study the physiological role of Pth in Mycobacterium tuberculosis (Mtb). While most peptidyl tRNA species accumulated in a strain with impaired Pth expression, peptidyl prolyl-tRNA was particularly enriched, suggesting that Pth is required for robust peptidyl prolyl-tRNA turnover. Reducing Pth levels increased Mtb's susceptibility to tRNA synthetase inhibitors that are in development to treat tuberculosis (TB) and rendered this pathogen highly susceptible to macrolides, drugs that are ordinarily ineffective against Mtb. Collectively, our findings reveal the potency of Cu-tRNAseq for profiling peptidyl tRNAs and suggest that targeting Pth would open new therapeutic approaches for TB. Peptidyl tRNA hydrolase (Pth) is an enzyme that cuts unfinished peptides off tRNA that has been prematurely released from a stalled ribosome. Pth is essential in nearly all bacteria, including the pathogen Mycobacterium tuberculosis (Mtb), but it has not been clear why. We have used genetic and novel biochemical approaches to show that when Pth levels decline in Mtb, peptidyl tRNA accumulates to such an extent that usable tRNA pools drop. Thus, Pth is needed to maintain normal tRNA levels, most strikingly for prolyl-tRNAs. Many antibiotics act on protein synthesis and could be affected by altering the availability of tRNA. This is certainly true for tRNA synthetase inhibitors, several of which are drug candidates for tuberculosis. We find that their action is potentiated by Pth depletion. Furthermore, Pth depletion results in hypersensitivity to macrolides, drugs that are not active enough under ordinary circumstances to be useful for tuberculosis.
涉及救援停滞核糖体和回收翻译机制的酶在细菌中无处不在,是生长所必需的。肽酰 tRNA 脱落是一种翻译失败的类型,导致未完成的肽从 tRNA(肽酰 tRNA)释放到细胞质中。肽酰 tRNA 水解酶(Pth)通过切割未完成的肽来回收释放的 tRNA,在大多数细菌中是必不可少的。我们开发了一种基于测序的策略,称为基于硫酸铜的 tRNA 测序(Cu-tRNAseq),用于研究 Pth 在结核分枝杆菌(Mtb)中的生理作用。虽然在表达 Pth 受损的菌株中大多数肽酰 tRNA 积累,但肽酰脯氨酰-tRNA 特别丰富,表明 Pth 是肽酰脯氨酰-tRNA 有效周转所必需的。降低 Pth 水平会增加 Mtb 对正在开发用于治疗结核病(TB)的 tRNA 合成酶抑制剂的敏感性,并使这种病原体对大环内酯类药物高度敏感,大环内酯类药物通常对 Mtb 无效。总之,我们的研究结果揭示了 Cu-tRNAseq 对肽酰 tRNA 进行分析的潜力,并表明靶向 Pth 将为 TB 开辟新的治疗方法。肽酰 tRNA 水解酶(Pth)是一种从停滞的核糖体过早释放的 tRNA 上切割未完成肽的酶。Pth 在几乎所有细菌中都是必需的,包括病原体结核分枝杆菌(Mtb),但原因尚不清楚。我们使用遗传和新的生化方法表明,当 Mtb 中的 Pth 水平下降时,肽酰 tRNA 积累到一定程度,可用的 tRNA 池减少。因此,Pth 是维持正常 tRNA 水平所必需的,最明显的是脯氨酰-tRNA。许多抗生素作用于蛋白质合成,并且可以通过改变 tRNA 的可用性来影响。这对于 tRNA 合成酶抑制剂确实如此,其中几种是结核病的候选药物。我们发现它们的作用因 Pth 耗尽而增强。此外,Pth 耗尽会导致对大环内酯类药物的敏感性增加,在普通情况下,这些药物对结核病不够活跃,因此无法使用。
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