Complete genome sequences and multidrug resistance genotypes of nontuberculous mycobacteria isolates from the Central Tuberculosis Reference Laboratory Muhimbili Tanzania

Q4 Medicine
Hortensia G Nondoli, R. Maghembe, W. Kidima, Victor A. Makene, Esther Ngadaya
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Abstract

Background: Nontuberculous mycobacteria (NTM) usually comprise a group of environmental bacteria, with emerging but elusive coinfection with tuberculous mycobacteria, causing pulmonary tuberculosis. Whole genome sequencing may give insight into potential antimicrobial resistance genotypes, giving clinicians and policymakers proper directions in clinical applications and management regimens. Methods: WGS was performed on twenty-four gDNA isolates from archival samples at the Central Tuberculosis Reference Laboratory using the MinION Oxford Nanopore Sequencing approach. Out of twenty-four, two were confirmed to belong to the NTM group. Further analysis was done to resolve the complete genomes of two nontuberculous mycobacteria strains isolated from tuberculosis patients. We then combined phylogenomics, reference-based scaffolding and average nucleotide identity (ANI) analysis to delineate each strain's taxonomic position and corresponding features. Results: Our findings reveal that the two strains fit into the genus Mycolicibacterium, and the closest relative is Mycolicibacterium novocastrense. Coupling BacAnt and CARD-based antibiotic resistance analyses revealed multidrug-resistant genotypes of diverse spectra and mechanisms. While the BC02 strain is genetically resistant to beta-lactams, macrolides and rifamycins, the BC05 strain portrays an extended drug resistance genotype encompassing beta-lactams, macrolides, polyamines, and aminoglycosides. Both strains possess a single nucleotide polymorphism (SNP) of the RNA polymerase beta-subunit (rpoB), representing resistance to the first-line rifampicin. Additionally, the BC05 strain genetically portrays resistance to ethambutol, isoniazid and fosfomycin through mechanisms involving target alteration through SNPs, drug inactivation and efflux. Conclusion: Our findings strongly suggest the potential implication of multidrug-resistant NTM clinical isolates in the pathogenesis of pulmonary tuberculosis.  
坦桑尼亚穆欣比利中央结核病参考实验室分离的非结核分枝杆菌的完整基因组序列和耐多药基因型
背景:非结核分枝杆菌(NTM)通常由一组环境细菌组成,它们与结核分枝杆菌合并感染,导致肺结核,虽然新出现但难以捉摸。全基因组测序可深入了解潜在的抗菌药耐药性基因型,为临床医生和政策制定者提供正确的临床应用和管理方案:采用 MinION 牛津纳米孔测序方法对中央结核病参考实验室档案样本中的 24 个 gDNA 分离物进行了 WGS 测序。在 24 个样本中,有 2 个样本被证实属于 NTM 组。通过进一步分析,我们解析了从结核病患者体内分离出的两株非结核分枝杆菌的完整基因组。然后,我们结合系统发生组学、基于参考的支架和平均核苷酸同一性(ANI)分析,确定了每株菌株的分类位置和相应特征:结果:我们的研究结果表明,这两株菌株均属于霉菌属,其中最亲缘的菌株是新产霉菌(Mycolicibacterium novocastrense)。结合 BacAnt 和基于 CARD 的抗生素耐药性分析,我们发现了具有不同光谱和机制的多重耐药基因型。BC02 菌株对 beta-内酰胺类、大环内酯类和利福霉素具有耐药性,而 BC05 菌株的耐药性基因型则扩展到了 beta-内酰胺类、大环内酯类、多胺类和氨基糖苷类。两株菌株都具有 RNA 聚合酶 beta 亚基(rpoB)的单核苷酸多态性(SNP),代表了对一线利福平的耐药性。此外,BC05菌株通过SNP、药物失活和外流等机制对乙胺丁醇、异烟肼和磷霉素产生耐药性:我们的研究结果有力地证明了耐多药非结核分枝杆菌临床分离株在肺结核发病机制中的潜在影响。
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来源期刊
Tanzania Journal of Health Research
Tanzania Journal of Health Research Medicine-Medicine (all)
CiteScore
0.20
自引率
0.00%
发文量
20
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