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首页> 外文期刊>Antimicrobial agents and chemotherapy. >Sequence analyses of just four genes to detect extensively drug-resistant Mycobacterium tuberculosis strains in multidrug-resistant tuberculosis patients undergoing treatment.
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Sequence analyses of just four genes to detect extensively drug-resistant Mycobacterium tuberculosis strains in multidrug-resistant tuberculosis patients undergoing treatment.

机译:仅对四个基因进行序列分析,以检测正在接受治疗的耐多药结核病患者中广泛耐药的结核分枝杆菌菌株。

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The rapid detection of Mycobacterium tuberculosis isolates resistant to second-line drugs is crucial for the institution of appropriate treatment regimens as early as possible. Although molecular methods have successfully been used for the rapid detection of resistance to first-line drugs, there are limited data on mutations that confer resistance to second-line drugs. To address this question, we analyzed Mycobacterium tuberculosis strains resistant to ofloxacin (n = 26) and to capreomycin and/or amikacin (n = 48) from Uzbekistan for variations in target genes (gyrA, gyrB, rrs, and tlyA). Strains susceptible to ofloxacin (n = 49) and capreomycin and/or amikacin (n = 39) were included as controls. Mutations in gyrA or gyrB were found in 96% (25/26 strains) of the ofloxacin-resistant strains, while none of the susceptible strains displayed mutations in those two genes. The most common mutation occurred in gyrA at codon 94 (17/26 strains [65.4%]), followed by mutations at codons 90 and 91. Two strains showed a mutation in gyrB, at codons 485 and 543, respectively; both mutations have not been reported previously. The most frequent mutation in strains resistant to both amikacin and capreomycin was A1401G in rrs (34/40 strains [85.0%]). Three strains had mutations in tlyA, of which two (at codons 18 and 118) were associated with resistance to capreomycin alone. Overall, none of the 10 resistant strains (5 amikacin-resistant and capreomycin-susceptible strains) and none of the 39 susceptible control strains had mutations in the genes investigated. Our results clearly demonstrate the potential of sequence analyses of short regions of relatively few target genes for the rapid detection of resistance to second-line drugs among strains isolated from patients undergoing treatment for multidrug-resistant tuberculosis. The mechanisms that confer amikacin resistance in this setting remain unclear.
机译:对二线药物耐药的结核分枝杆菌分离物的快速检测对于尽早实施适当的治疗方案至关重要。尽管分子方法已成功用于快速检测对一线药物的耐药性,但有关赋予对二线药物耐药性的突变的数据有限。为了解决这个问题,我们分析了对氧氟沙星(n = 26)和对来自乌兹别克斯坦的红霉素和/或丁胺卡那霉素(n = 48)的结核分枝杆菌菌株靶基因(gyrA,gyrB,rrs和tlyA)的变异。包括对氧氟沙星(n = 49)和卡普霉素和/或丁胺卡那霉素(n = 39)敏感的菌株作为对照。在96%(25/26株)耐氧氟沙星的菌株中发现了gyrA或gyrB突变,而所有这两个易感菌株均未显示出突变。最常见的突变发生在gyrA的第94位密码子处(17/26株[65.4%]),随后发生在90和91号密码子处的突变。两种菌株显示gyrB发生了突变,分别位于485位和543位。两种突变以前都没有报道过。抗阿米卡星和卡普霉素的菌株中最常见的突变是rrs中的A1401G(34/40株[85.0%])。 3个菌株的tlyA突变,其中2个(第18和118位密码子)与仅对毛霉素的抗性有关。总体而言,10个耐药菌株(5个对阿米卡星耐药和对卡普霉素敏感的菌株)和39个易感对照菌株均未在所研究的基因中发生突变。我们的结果清楚地证明了从相对较少的靶基因的短区域进行序列分析的潜力,可用于快速检测从接受多药耐药性肺结核治疗的患者中分离出的菌株对二线药物的耐药性。在这种情况下赋予丁胺卡那霉素抗性的机制仍不清楚。

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