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首页> 外文期刊>Infection, Genetics and Evolution: Journal of Molecular Epidemiology and Evolutionary Genetics in Infectious Diseases >Large genomics datasets shed light on the evolution of the Mycobacterium tuberculosis complex
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Large genomics datasets shed light on the evolution of the Mycobacterium tuberculosis complex

机译:大型基因组学数据集在结核分枝杆菌复合体的演变上闪光

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摘要

Two strains of Mycobacterium tuberculosis complex can be separated as much as 2500 single nucleotide differences (Coscolla and Gagneux, 2014). In that limited amount of diversity, we find an astonishing range of clinical, epidemiological and biological phenotypes. The most striking is the strong host preferences depending on the infecting strain while more subtle differences can be found looking at different human tuberculosis isolates. Those subtle differences are the most difficult to spot given that analysis methods for so little diversity are limited and phenotypes like virulence are difficult to define and measure. Recent genomics advances allow to study the pathogen diversity at a resolution not available before from comparative species level, to global diversity to transmission in local settings. Here, we will review some of these recent results to highlight how population genomics approaches can aid not only to understand how MTBC evolved but also to identify relevant biomedical targets.
机译:两种分枝杆菌复合物的菌株可以分离多达2500个单核苷酸差异(Coscolla和Gagneux,2014)。在这种有限的多样性中,我们发现令人惊讶的临床,流行病学和生物表型。最引人注目的是,取决于感染菌株的强烈宿主偏好,而可以发现更细微的差异,看看不同的人结核病分离株。对于如此小的多样性的分析方法有限,那些微妙的差异是最难以发现的,并且难以定义和测量等毒力的表型。最近的基因组学进步允许在比较物种级别之前的分辨率下验到病原体多样性,以在本地设置中传输的全球多样性。在这里,我们将审查一些最近的结果,突出群体基因组学方法可以帮助了解MTBC如何发展,而且还要识别相关的生物医学目标。

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