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首页> 外文期刊>BMC Genomics >Capsular profiling of the Cronobacter genus and the association of specific Cronobacter sakazakii and C. malonaticus capsule types with neonatal meningitis and necrotizing enterocolitis
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Capsular profiling of the Cronobacter genus and the association of specific Cronobacter sakazakii and C. malonaticus capsule types with neonatal meningitis and necrotizing enterocolitis

机译:克罗诺杆菌属的荚膜轮廓分析以及阪崎肠杆菌和克氏丙酸杆菌特定囊型与新生儿脑膜炎和坏死性小肠结肠炎的关联

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Cronobacter sakazakii and C. malonaticus can cause serious diseases especially in infants where they are associated with rare but fatal neonatal infections such as meningitis and necrotising enterocolitis. This study used 104 whole genome sequenced strains, covering all seven species in the genus, to analyse capsule associated clusters of genes involved in the biosynthesis of the O-antigen, colanic acid, bacterial cellulose, enterobacterial common antigen (ECA), and a previously uncharacterised K-antigen. Phylogeny of the gnd and galF genes flanking the O-antigen region enabled the defining of 38 subgroups which are potential serotypes. Two variants of the colanic acid synthesis gene cluster (CA1 and CA2) were found which differed with the absence of galE in CA2. Cellulose (bcs genes) were present in all species, but were absent in C. sakazakii sequence type (ST) 13 and clonal complex (CC) 100 strains. The ECA locus was found in all strains. The K-antigen capsular polysaccharide Region 1 (kpsEDCS) and Region 3 (kpsMT) genes were found in all Cronobacter strains. The highly variable Region 2 genes were assigned to 2 homology groups (K1 and K2). C. sakazakii and C. malonaticus isolates with capsular type [K2:CA2:Cell+] were associated with neonatal meningitis and necrotizing enterocolitis. Other capsular types were less associated with clinical infections. This study proposes a new capsular typing scheme which identifies a possible important virulence trait associated with severe neonatal infections. The various capsular polysaccharide structures warrant further investigation as they could be relevant to macrophage survival, desiccation resistance, environmental survival, and biofilm formation in the hospital environment, including neonatal enteral feeding tubes.
机译:阪崎肠杆菌和丙酸杆菌可引起严重疾病,尤其是在婴儿中,它们与罕见但致命的新生儿感染有关,例如脑膜炎和坏死性小肠结肠炎。这项研究使用了104个全基因组测序菌株,覆盖了该属中的所有七个物种,以分析与O抗原,可乐酸,细菌纤维素,肠细菌共同抗原(ECA)和以前的生物合成有关的胶囊相关基因簇。未鉴定的K抗原。 O抗原区侧翼的gnd和galF基因的系统发生使得能够确定38个亚型,它们是潜在的血清型。发现了可乐酸合成基因簇的两个变体(CA1和CA2),它们与CA2中不存在galE的情况有所不同。纤维素(bcs基因)存在于所有物种中,但在阪崎肠梭菌序列类型(ST)13和克隆复合体(CC)100菌株中不存在。在所有菌株中均发现了ECA基因座。在所有克罗诺杆菌菌株中均发现了K抗原荚膜多糖区域1(kpsEDCS)和区域3(kpsMT)基因。将高度可变的区域2基因分配给2个同源性组(K1和K2)。荚膜类型为[K2:CA2:Cell +]的阪崎假丝酵母和丙酸假丝酵母与新生儿脑膜炎和坏死性小肠结肠炎有关。其他类型的荚膜较少与临床感染相关。这项研究提出了一种新的荚膜分型方案,该方案确定了可能与严重新生儿感染相关的重要毒力特征。各种荚膜多糖结构值得进一步研究,因为它们可能与巨噬细胞存活,抗干燥性,环境存活以及医院环境(包括新生儿肠内饲管)中的生物膜形成有关。

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