首页> 美国卫生研究院文献>Journal of Clinical Microbiology >Role of Large Sequence Polymorphisms (LSPs) in Generating Genomic Diversity among Clinical Isolates of Mycobacterium tuberculosis and the Utility of LSPs in Phylogenetic Analysis
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Role of Large Sequence Polymorphisms (LSPs) in Generating Genomic Diversity among Clinical Isolates of Mycobacterium tuberculosis and the Utility of LSPs in Phylogenetic Analysis

机译:大序列多态性(LSPs)在结核分枝杆菌临床分离株中产生基因组多样性中的作用以及LSPs在系统发生分析中的效用

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摘要

Mycobacterium tuberculosis strains contain different genomic insertions or deletions called large sequence polymorphisms (LSPs). Distinguishing between LSPs that occur one time versus ones that occur repeatedly in a genomic region may provide insights into the biological roles of LSPs and identify useful phylogenetic markers. We analyzed 163 clinical M. tuberculosis isolates for 17 LSPs identified in a genomic comparison of M. tuberculosis strains H37Rv and CDC1551. LSPs were mapped onto a single-nucleotide polymorphism (SNP)-based phylogenetic tree created using nine novel SNP markers that were found to reproduce a 212-SNP-based phylogeny. Four LSPs (group A) mapped to a single SNP tree segment. Two LSPs (group B) and 11 LSPs (group C) were inferred to have arisen independently in the same genomic region either two or more than two times, respectively. None of the group A LSPs but one group B LSP and five group C LSPs were flanked by IS6110 sequences in the references strains. Genes encoding members of the proline-glutamic acid or proline-proline-glutamic acid protein families were present only in group B or C LSPs. SNP- versus LSP-based phylogenies were also compared. We classified each isolate into 58 LSP types by using a separate LSP-based phylogenetic analysis and mapped the LSP types onto the SNP tree. LSPs often assigned isolates to the correct phylogenetic lineage; however, significant mistakes occurred for 6/58 (10%) of the LSP types. In conclusion, most LSPs occur in genomic regions that are prone to repeated insertion/deletion events and were responsible for an unexpectedly high degree of genomic variation in clinical M. tuberculosis. Group B and C LSPs may represent polymorphisms that occur due to selective pressure and affect the phenotype of the organism, while group A LSPs are preferable phylogenetic markers.
机译:结核分枝杆菌菌株含有不同的基因组插入或缺失,称为大序列多态性(LSPs)。区分一次发生的LSP与在基因组区域中反复发生的LSP可以提供对LSP生物学作用的认识,并确定有用的系统发生标记。我们分析了163株临床结核分枝杆菌的17 LSP,在结核分枝杆菌菌株H37Rv和CDC1551的基因组比较中鉴定出。将LSPs映射到使用九种新的SNP标记创建的基于单核苷酸多态性(SNP)的系统发育树上,发现它们可重现基于212-SNP的系统发育。四个LSP(A组)映射到单个SNP树段。推断两个LSP(B组)和11个LSP(C组)分别在同一基因组区域中独立出现两次或两次以上。在参考菌株中,A组LSP中没有一个,但一组B LSP和五个C组LSP的两侧是IS6110序列。编码脯氨酸-谷氨酸或脯氨酸-脯氨酸-谷氨酸蛋白家族成员的基因仅存在于B组或C组LSP中。还比较了基于SNP和LSP的系统发育。通过使用单独的基于LSP的系统发育分析,我们将每种分离物分为58种LSP类型,并将LSP类型映射到SNP树上。 LSP经常被分配到正确的系统进化谱系中。但是,有6/58(10%)的LSP类型发生了重大错误。总之,大多数LSPs发生在易于重复插入/缺失事件的基因组区域中,并导致临床上结核分枝杆菌出乎意料的高度基因组变异。 B和C组LSP可能代表由于选择性压力而发生的多态性,并影响生物体的表型,而A组LSP是优选的系统发育标记。

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