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首页> 外文期刊>Journal of bacteriology >Mosaic Structure and Molecular Evolution of the Leukotoxin Operon (lktCABD) in Mannheimia (Pasteurella) haemolytica, Mannheimia glucosida, and Pasteurella trehalosi
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Mosaic Structure and Molecular Evolution of the Leukotoxin Operon (lktCABD) in Mannheimia (Pasteurella) haemolytica, Mannheimia glucosida, and Pasteurella trehalosi

机译:溶血的曼海姆氏菌(Pasteurella),葡糖曼氏菌和海藻巴斯德氏菌中白细胞毒素操纵子(lktCABD)的马赛克结构和分子进化

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摘要

The mosaic structure and molecular evolution of the leukotoxin operon (lktCABD) was investigated by nucleotide sequence comparison of the lktC, lktB, and lktD genes in 23 Mannheimia (Pasteurella) haemolytica, 6 Mannheimia glucosida, and 4 Pasteurella trehalosi strains. Sequence variation in the lktA gene has been described previously (R. L. Davies et al., J. Bacteriol. 183:1394–1404, 2001). The leukotoxin operon of M. haemolytica has a complex mosaic structure and has been derived by extensive inter- and intraspecies horizontal DNA transfer and intragenic recombination events. However, the pattern of recombination varies throughout the operon and among the different evolutionary lineages of M. haemolytica. The lktA and lktB genes have the most complex mosaic structures with segments derived from up to four different sources, including M. glucosida and P. trehalosi. In contrast, the lktD gene is highly conserved in M. haemolytica. The lktC, lktA, and lktB genes of strains representing the major ovine lineages contain recombinant segments derived from bovine or bovine-like serotype A2 strains. These findings support the previous conclusion that host switching of bovine A2 strains from cattle to sheep has played a major role in the evolution of the leukotoxin operon in ovine strains of M. haemolytica. Homologous segments of donor and recipient alleles are identical, or nearly identical, indicating that the recombinational exchanges occurred relatively recent in evolutionary terms. The 5′ and 3′ ends of the operon are highly conserved in M. haemolytica, which suggests that multiple horizontal exchanges of the complete operon have occurred by a common mechanism such as transduction. Although the lktA and lktB genes both have complex mosaic structures and high nucleotide substitution rates, the amino acid diversity of LktB is significantly lower than that of LktA due to a higher degree of evolutionary constraint against amino acid replacement. The recombinational exchanges within the leukotoxin operon have had greatest effect on LktA and probably provide an adaptive advantage against the host antibody response by generating novel antigenic variation at surface-exposed sites.
机译:通过 lktC lktB 的核苷酸序列比较研究了白细胞毒素操纵子( lktCABD )的镶嵌结构和分子进化。 23个 Mannheimia Pasteurella haemolytica ,6个 Mannheimia glucosida 和4个的lktD 基因>海藻巴斯德氏菌菌株。 lktA基因的序列变异先前已有描述(R. L. Davies等人,J。Bacteriol。183:1394-1404,2001)。溶血支原体的白细胞毒素操纵子具有复杂的镶嵌结构,并已通过广泛的种间和种内水平DNA转移和基因内重组事件而衍生。但是,重组模式在整个操纵子中以及在 M的不同进化谱系中都不同。溶血性。 lktA和lktB基因具有最复杂的镶嵌结构,其片段来自多达四个不同的来源,包括 M。葡糖苷 P。海藻糖。相反, lktD 基因在 M中高度保守。溶血性。代表主要绵羊谱系的菌株的 lktC lktA lktB 基因包含源自牛或类牛血清型A2菌株的重组片段。这些发现支持了先前的结论,即牛A2菌株从牛到绵羊的宿主转换在 M绵羊品系中白细胞毒素操纵子的进化中起着重要作用。溶血性。供体和受体等位基因的同源部分相同,或几乎相同,这表明重组交流发生在进化方面是相对较新的。操纵子的5'和3'末端在 M中高度保守。 haemolytica ,这表明完整操纵子的多次水平交换是通过常见的机制(例如转导)发生的。尽管 lktA lktB 基因均具有复杂的镶嵌结构和较高的核苷酸取代率,但LktB的氨基酸多样性由于LkeB的较高程度而显着低于LktA。氨基酸替代的进化限制。白细胞毒素操纵子内的重组交换对LktA影响最大,并可能通过在表面暴露的位点产生新的抗原变异而对宿主抗体反应提供适应性优势。

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