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首页> 外文期刊>International journal of infectious diseases : >Rapid identification of a Mycobacterium tuberculosis full genetic drug resistance profile through whole genome sequencing directly from sputum
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Rapid identification of a Mycobacterium tuberculosis full genetic drug resistance profile through whole genome sequencing directly from sputum

机译:直接从痰液中通过全基因组测序快速鉴定结核分枝杆菌全基因药物耐药性

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Introduction: Resistance to second-line tuberculosis drugs is common, but slow to diagnose with phenotypic drug sensitivity testing. Rapid molecular tests speed up diagnosis, but can only detect limited mutations. Whole genome sequencing (WGS) of culture isolates can generate a complete genetic drug resistance profile, but is delayed by the initial culture step. In the case presented here, successful WGS directly from sputum was achieved using targeted enrichment. Case report: A 29-year-old Nigerian woman was diagnosed with tuberculosis. Xpert MTB/RIF and Hain line probe assays identified rpoB and inhA mutations consistent with rifampicin and intermediate isoniazid resistance, and a further possible mutation conferring fluoroquinolone resistance. WGS directly from sputum identified a further inhA mutation consistent with high-level isoniazid resistance and confirmed the absence of fluoroquinolone resistance. Isoniazid was stopped, and the patient has completed 18 months of a fluoroquinolone-based regimen without relapse. Discussion: Compared to rapid molecular tests (which can only examine a limited number of mutations) and WGS of culture isolates (which requires a culture step), WGS directly from sputum can quickly generate a complete genetic drug resistance profile. In this case, WGS altered the clinical management of drug-resistant tuberculosis and demonstrated potential for guiding individualized drug treatment where second-line drug resistance is common.
机译:简介:对二线结核药物的耐药性很普遍,但通过表型药物敏感性测试难以诊断。快速的分子检测可加快诊断速度,但只能检测出有限的突变。培养分离株的全基因组测序(WGS)可以产生完整的遗传药物抗药性,但会因最初的培养步骤而延迟。在这里介绍的情况下,使用靶向富集技术可直接从痰液中成功获得WGS。病例报告:一名29岁的尼日利亚妇女被诊断出患有肺结核。 Xpert MTB / RIF和Hain线探针测定法鉴定出与利福平和中间异烟肼耐药性相符的rpoB和inhA突变,以及可能导致氟喹诺酮耐药性的进一步突变。直接从痰液中提取的WGS鉴定出进一步的inhA突变,与高水平的异烟肼耐药性相符,并证实不存在氟喹诺酮耐药性。停止使用异烟肼,患者已完成18个月基于氟喹诺酮的治疗方案,且未复发。讨论:与快速分子检测(只能检查有限数量的突变)和培养分离株的WGS(需要培养步骤)相比,直接来自痰液的WGS可以快速生成完整的遗传耐药性。在这种情况下,WGS改变了耐药结核病的临床管理,并证明了指导二线耐药的个性化药物治疗的潜力。

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