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Fluoroquinolone resistance and mutational profile of gyrA in pulmonary MDR tuberculosis patients

机译:肺癌肺癌患者氟喹醇抗性和突变谱

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Fluoroquinolones (FQs) are potential drugs that inhibit DNA synthesis and are used in the treatment of multidrug-resistant tuberculosis (TB) and short-term anti-TB regimens. In recent years, a high proportion of FQ resistance has been observed in Mycobacterium tuberculosis isolates. The development of FQ resistance in multidrug-resistant TB negatively impacts patient treatment outcome and is a serious threat to control of TB. The study included a total of 562 samples from patients with pulmonary TB that had been on anti-tuberculosis therapy. MTBDRsl assays were performed for the molecular detection of mutations. Sequence analysis was performed for the characterization and mutational profiling of FQ-resistant isolates. FQ resistance was observed in 104 samples (18.5%), most of which were previously treated and treatment failure cases. A total of 102 isolates had mutations in DNA gyrase subunit A (gyrA), while mutations in gyrB were observed in only two isolates. Mutational analysis revealed that the mutations mostly alter codons 94 (replacing aspartic acid with glycine, D94G) and 90 (replacing alanine with valine, A90V). In MDR and treatment failure cases, resistance to FQs was most commonly associated with the D94G mutation. In contract, a high proportion of A90V mutations were observed in isolates that were newly diagnosed. The findings suggest that genotypic assays for FQ resistance should be carried out at the time of initial diagnosis, before starting treatment, in order to rule out mutations that impact the potential use of FQs in treatment and to control drug resistance.
机译:氟代喹啉酮(FQS)是抑制DNA合成的潜在药物,用于治疗多药结核(TB)和短期抗TB方案。近年来,在结核分枝杆菌分离物中观察到高比例的FQ抗性。多药TB在多药TB中的抗性的发展对患者治疗结果产生负面影响,对控制TB的严重威胁。该研究包括来自肺结核患者的总共562个样本,肺结核患者一直是抗结核疗法。对突变的分子检测进行MTBDRSL测定。对FQ抗性分离物的表征和突变分析进行序列分析。在104个样品中观察到FQ抗性(18.5%),其中大部分是先前治疗的和治疗失败病例。总共102个分离物在DNA腺苷酸亚基A(Gyra)中具有突变,而仅在两个分离株中观察到陀螺蛋白中的突变。突变分析显示,突变大多数改变密码子94(用甘氨酸,D94g)和90(用缬氨酸替换丙氨酸,A90V)。在MDR和治疗失败病例中,对FQS的抗性最常与D94G突变相关。在合同中,在新诊断出的分离物中观察到高比例的A90V突变。研究结果表明,用于在开始处理之前的初步诊断时,应在初步诊断时进行基因型测定,以便排除影响FQs治疗和控制耐药性的突变和控制耐药性的突变。

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