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首页> 外文期刊>Journal of bacteriology >Identification, Genomic Organization, and Analysis of the Group III Capsular Polysaccharide Genes kpsD, kpsM,kpsT, and kpsE from an Extraintestinal Isolate of Escherichia coli (CP9, O4/K54/H5)
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Identification, Genomic Organization, and Analysis of the Group III Capsular Polysaccharide Genes kpsD, kpsM,kpsT, and kpsE from an Extraintestinal Isolate of Escherichia coli (CP9, O4/K54/H5)

机译:从大肠杆菌肠外分离株(CP9,O4 / K54 / H5)中的III类荚膜多糖基因kpsD,kpsM,kpsT和kpsE的鉴定,基因组组织和分析

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Group III capsular polysaccharides (e.g., K54) of extraintestinal isolates of Escherichia coli, similar to group II capsules (e.g., K1), are important virulence traits that confer resistance to selected host defense components in vitro and potentiate systemic infection in vivo. The genomic organization of group II capsule gene clusters has been established as a serotype-specific region 2 flanked by regions 1 and 3, which contain transport genes that are highly homologous between serotypes. In contrast, the organization of group III capsule gene clusters is not well understood. However, they are defined in part by an absence of genes with significant nucleotide homology to group II capsule transport genes in regions 1 and 3. Evaluation of isogenic, TnphoA-generated, group III capsule-minus derivatives of a clinical blood isolate (CP9, O4/K54/H5) has led to the identification of homologs of the group II capsule transport genes kpsDMTE. These genes and their surrounding regions were sequenced and analyzed. The genomic organization of these genes is distinctly different from that of their group II counterparts. Although kps K54 DMTE are significantly divergent from their group II homologs at both the DNA and protein levels phoA fusions and computer-assisted analyses suggest that their structures and functions are similar. The putative proteins KpsK54M and KpsK54T appear to be the integral membrane component and the peripheral ATP-binding component of the ABC-2 transporter family, respectively. The putative KpsK54E possesses features similar to those of the membrane fusion protein family that facilitates the passage of large molecules across the periplasm. At one boundary of the capsule gene cluster, a truncated kpsM (kpsM truncated) and its 5′ noncoding regulatory sequence were identified. In contrast to the complete kps K54 M, this region was highly homologous to the group II kpsM. Fifty-three base pairs 3′ from the end of kpsM truncated was a sequence 75% homologous to the 39-bp inverted repeat in the IS110 insertion element from Streptomyces coelicolor. Southern analysis established that two copies of this element are present in CP9. These findings are consistent with the hypothesis that CP9 previously possessed group II capsule genes and acquired group III capsule genes via IS110-mediated horizontal transfer.
机译:大肠埃希菌的肠外分离物的III族荚膜多糖(例如K54),类似于II族胶囊(例如K1),是重要的毒力特性,可赋予体外选定的宿主防御成分抗性并增强其抗性体内全身感染。组II胶囊基因簇的基因组组织已被确定为血清型特异性区域2,其侧翼为区域1和3,区域1和区域3包含在血清型之间高度同源的转运基因。相比之下,III类胶囊基因簇的组织尚不十分清楚。但是,它们的部分定义是在区域1和3中不存在与II类胶囊转运基因具有显着核苷酸同源性的基因。评估同基因,Tn phoA 产生的III类胶囊-负衍生物临床血液分离物(CP9,O4 / K54 / H5)的分离已鉴定出II组胶囊转运基因 kpsDMTE 的同源物。对这些基因及其周围区域进行测序和分析。这些基因的基因组组织与第二类对应物明显不同。尽管 kps K54 DMTE 在DNA和蛋白质水平 phoA 融合和计算机辅助分析表明它们的结构和功能相似。推定的蛋白质Kps K54 M和Kps K54 T似乎分别是ABC-2转运蛋白家族的完整膜成分和外围ATP结合成分。推定的Kps K54 E具有类似于膜融合蛋白家族的特征,该特征有助于大分子穿过周质。在胶囊基因簇的一个边界处,鉴定出截短的 kpsM kpsM 截短的)及其5'非编码调控序列。与完整的 kps K54 M 相比,该区域与II kpsM 组高度同源。 kpsM 截短的末端的53个碱基对3'与IS 110 来自链霉菌的插入元素。 Southern分析确定CP9中存在该元素的两个副本。这些发现与以下假设相吻合:CP9以前具有II组荚膜基因并通过IS 110 介导的水平转移获得了III组荚膜基因。

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