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Characterizing the novel mutations associated with bedaquiline resistance in Mycobacterium tuberculosis

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NIAID Data Ecosystem2026-03-13 收录
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https://www.ncbi.nlm.nih.gov/sra/SRP340062
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Bedaquiline (BDQ), one of the new antitubercular agents, has been used to treat drug-resistant tuberculosis (TB). Although mutations in atpE, rv0678 and pepQ confer the major resistance to BDQ, the mechanism resistance to BDQ for a portion of isolates identified in vitro and in clinical remain unknown. Here, BDQ-resistant mutants were selected from 7H10 agar plates containing 0.5 mg/L BDQ (the critical concentration). Mutations associated with BDQ resistance were identified through whole genome sequence, PCR and Sanger sequencing analysis. A total of 1025 mutants were found to resistance to BDQ. We randomly picked 168 mutants for further analysis and discovered that 157/168 BDQ-resistant mutants harbored mutations in rv0678 encoding a transcriptional regulator repressing the expression of efflux pump MmpS5-MmpL5. Moreover, we found two mutations with high frequency in rv0678 gene, including nucleotide positions 286-287 (CG286-287 insertion; accounted for 26.8% (45/168)) and 198-199 (G198, G199 insertion, G198 deletion; accounted for 14.3 (24/168)). The remains were dispersed covering the entire rv0678 gene. Moreover, we found that one new gene, glpK harboring G572 insertion with high prevalence (85.7%, 144/168) in the isolated mutants and MIC assay demonstrated that G572 insertion mutation in glpK was closely associated with BDQ resistance. In summary, our study characterized 168/1025 mutants resistant to BDQ and found that mutations in rv0678 confer the primary mechanism of BDQ resistance. Moreover, we identified a new gene (glpK) involved in BDQ resistance. Our study offers new insights and valuable information that will contribute to the rapid identification of BDQ resistant isolates in the clinical setting.
创建时间:
2022-05-26
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