Characteristic of the Mycobacterium tuberculosis genome of Beijing genotype of cluster 100-32 displaying pre-extended drug resistance

IF 0.1 Q4 MULTIDISCIPLINARY SCIENCES DOKLADY NATSIONALNOI AKADEMII NAUK BELARUSI Pub Date : 2023-07-06 DOI:10.29235/1561-8323-2023-67-3-231-241
V. Slizen, A. Akhremchuk, L. Surkova, G. L. Gurevich, L. Titov
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Abstract

A whole genome sequencing was performed of strain M. tuberculosis 11502 (NCBI biosamples database, access code SAMN17832565) that was assigned to the Beijing genotype subtype B0/W148 of cluster 100-32, based on the MIRU- VNTR loci (n = 24) structure, a nd t hat exhibited pre-extended d rug resistance. M. tuberculosis 11502 was resistant to isoniazid, rifampicin, ethambutol, levofloxacin, and ethionamide, which correlated with the presence of mutations in the genes: resistance to isoniazid – the mutations in the fabG1 promoter (p.-8T>C), the katG promoter (p.S315T), to ethionamide – the mutations in ethA (deletion of T at position 4 335 027 (gatgc-gagc)); to fluoroquinolones – in the gyrA gene (p.D94G); to ethambutol – in the embB gene (p.M306I); to streptomycin – in the rpsL gene (p.K43R). M. tuberculosis 11502 genome (Gen- Bank NCBI access code – CP070338) contained 4 420 561 base pairs, 4 104 genes, 4 053 CDSs (coding proteins – 3 874) and differed from reference strain M. tuberculosis H37Rv by the presence of 2 055 mutations. A slight drift of mutations towards the G+C accumulation was revealed, which indicates the importance of maintaining a high G+C content in the Mycobacterium spp.genome Strain M. tuberculosis 11502 has a higher number of mutations in comparison to previously sequenced M. tuberculosis 4860 (GenBank Access Code, NCBI: CP053092) belonging to the LAM genotype (2055 vs. 1577 mutations), which may be a consequence of a longer circulation of M. tuberculosis 11502, or some biological features providing the promutagenic effect.
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100-32簇北京基因型结核分枝杆菌基因组特征分析
基于MIRU-VNTR基因座(n=24)结构,对归属于100-32簇北京基因型B0/W148亚型的结核分枝杆菌11502菌株(NCBI生物样本数据库,访问代码SAMN17832565)进行了全基因组测序,该菌株表现出预扩展的抗药性。结核分枝杆菌11502对异烟肼、利福平、乙胺丁醇、左氧氟沙星和乙磺酰胺具有耐药性,这与基因突变的存在有关:对异烟酰胺的耐药性——fabG1启动子的突变(p.-8T>C)、katG启动子(p.S315T)、对乙磺酰胺的抗性——ethA的突变(4 335 027位T缺失(gatgc gagc));对氟喹诺酮类药物——在gyrA基因中(p.D94G);在embB基因中的乙胺丁醇(p.M306I);结核分枝杆菌11502基因组(Gen-Bank NCBI访问代码–CP070338)包含4 420 561个碱基对、4 104个基因、4 053个CDSs(编码蛋白–3 874),与参考菌株结核分枝杆菌H37Rv的差异在于存在2 055个突变。揭示了突变向G+C积累的轻微漂移,这表明在分枝杆菌基因组中保持高G+C含量的重要性。与先前测序的属于LAM基因型的结核分枝杆菌4860(GenBank Access Code,NCBI:CP053092)相比,结核分枝杆菌菌株11502具有更高数量的突变(2055对1577个突变),这可能是结核分枝杆菌11502的较长循环或提供促突变作用的一些生物学特征的结果。
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DOKLADY NATSIONALNOI AKADEMII NAUK BELARUSI
DOKLADY NATSIONALNOI AKADEMII NAUK BELARUSI MULTIDISCIPLINARY SCIENCES-
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