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首页> 外文期刊>Journal of Clinical Microbiology >Molecular Epidemiologic Evaluation of Transmissibility and Virulence of Mycobacterium tuberculosis
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Molecular Epidemiologic Evaluation of Transmissibility and Virulence of Mycobacterium tuberculosis

机译:分子流行病学评估结核分枝杆菌的传播和毒力

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Discovery of genotypic markers associated with increased transmissibility in Mycobacterium tuberculosis would represent an important step in advancing mycobacterial virulence studies. M. tuberculosis strains may be classified into one of three genotypes on the basis of the presence of specific nucleotide substitutions in codon 463 of the katG gene (katG-463) and codon 95 of the gyrA gene (gyrA-95). It has previously been reported that two of these three genotypes are associated with increased IS6110-based clustering, a potential proxy of virulence. We designed a case-control analysis of U.S.-born patients with tuberculosis in San Francisco, Calif., between 1991 and 1997 to investigate associations between katG-463 andgyrA-95 genotypes and epidemiologically determined measures of strain-specific infectivity and pathogenicity and IS6110-based clustering status. We used a new class of molecular probes called molecular beacons to genotype the isolates rapidly. Infectivity was defined as the propensity of isolates to cause tuberculin skin test conversions among named contacts, and pathogenicity was defined as their propensity to cause active disease among named contacts. The molecular beacon assay was a simple and reproducible method for the detection of known single nucleotide polymorphisms in large numbers of clinical M. tuberculosisisolates. The results showed that no genotype of thekatG-463- and gyrA-95-based classification system was associated with increased infectivity and pathogenicity or with increased IS6110-based clustering in San Francisco during the study period. We speculate that molecular epidemiologic studies investigating clinically relevant outcomes may contribute to the knowledge of the significance of laboratory-derived virulence factors in the propagation of tuberculosis in human communities.
机译:发现与结核分枝杆菌的增加的可传播性相关的基因型标记将是推进分枝杆菌毒力研究的重要一步。 M。根据 katG 基因( katG -463)密码子463中特定核苷酸取代的存在,可以将结核病菌株分为三种基因型之一。和 gyrA 基因( gyrA -95)的密码子95。以前曾有报道说,这三种基因型中的两种与基于IS 6110 的聚类增加有关,这是一种潜在的毒力代理。我们设计了1991年至1997年在美国加利福尼亚州旧金山市出生的美国结核病患者的病例对照分析,以研究 katG -463和 gyrA -95之间的关联菌株特异性传染性和致病性的基因型和流行病学测定方法以及基于IS 6110 的聚类状态。我们使用了一类称为分子信标的新型分子探针对分离株进行快速基因分型。传染性被定义为在命名的接触者中引起结核菌素皮肤试验转化的分离物的倾向,而致病性被定义为在命名的接触者中引起活动性疾病的倾向。分子信标测定法是一种简单且可重现的方法,用于检测大量临床M中的已知单核苷酸多态性。结核病隔离株。结果表明,基于 katG -463-和 gyrA -95的分类系统的基因型与感染性和致病性增加或与IS 6110 <研究期间在旧金山基于/ em>的集群。我们推测,调查临床相关结果的分子流行病学研究可能有助于了解实验室衍生的毒力因子在结核病在人类社区中的传播的重要性。

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