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J Bacteriol. 1995 Jul;177(13):3680-6. doi: 10.1128/jb.177.13.3680-3686.1995.
2
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本文引用的文献

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Non-flagellar appendages of bacteria.细菌的非鞭毛附属物。
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2
Non-flagellar filamentous appendages (fimbriae) and haemagglutinating activity in Bacterium coli.大肠杆菌中的非鞭毛丝状附属物(菌毛)和血凝活性。
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3
Bacterial adhesins and host factors: role in the development and outcome of Escherichia coli bacteremia.细菌黏附素与宿主因素:在大肠杆菌菌血症发生发展及转归中的作用
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4
Escherichia coli F-18 phase locked 'on' for expression of type 1 fimbriae is a poor colonizer of the streptomycin-treated mouse large intestine.用于表达1型菌毛的大肠杆菌F-18在链霉素处理的小鼠大肠中是一种定植能力较差的菌株。
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5
Neutrophil activation by nascent FimH subunits of type 1 fimbriae purified from the periplasm of Escherichia coli.从大肠杆菌周质中纯化的1型菌毛新生FimH亚基对中性粒细胞的激活作用。
J Biol Chem. 1993 Feb 5;268(4):3009-15.
6
Reciprocal exchange of minor components of type 1 and F1C fimbriae results in hybrid organelles with changed receptor specificities.1型菌毛和F1C菌毛的次要成分相互交换,产生了具有改变的受体特异性的杂交细胞器。
J Bacteriol. 1994 Apr;176(8):2227-34. doi: 10.1128/jb.176.8.2227-2234.1994.
7
Type 1 fimbrial shafts of Escherichia coli and Klebsiella pneumoniae influence sugar-binding specificities of their FimH adhesins.大肠杆菌和肺炎克雷伯菌的1型菌毛杆影响其FimH黏附素的糖结合特异性。
Infect Immun. 1994 Mar;62(3):843-8. doi: 10.1128/iai.62.3.843-848.1994.
8
FimH family of type 1 fimbrial adhesins: functional heterogeneity due to minor sequence variations among fimH genes.1型菌毛粘附素的FimH家族:fimH基因间微小序列变异导致的功能异质性
J Bacteriol. 1994 Feb;176(3):748-55. doi: 10.1128/jb.176.3.748-755.1994.
9
Bacterial adhesion measured by growth of adherent organisms.通过粘附微生物的生长来测量细菌粘附。
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10
Bacterial adherence: adhesin-receptor interactions mediating the attachment of bacteria to mucosal surface.细菌黏附:介导细菌附着于黏膜表面的黏附素-受体相互作用。
J Infect Dis. 1981 Mar;143(3):325-45. doi: 10.1093/infdis/143.3.325.

由于fimH基因结构差异导致的1型菌毛大肠杆菌黏附性的定量差异。

Quantitative differences in adhesiveness of type 1 fimbriated Escherichia coli due to structural differences in fimH genes.

作者信息

Sokurenko E V, Courtney H S, Maslow J, Siitonen A, Hasty D L

机构信息

Department of Anatomy and Neurobiology, University of Tennessee, Memphis 38163, USA.

出版信息

J Bacteriol. 1995 Jul;177(13):3680-6. doi: 10.1128/jb.177.13.3680-3686.1995.

DOI:10.1128/jb.177.13.3680-3686.1995
PMID:7601831
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC177083/
Abstract

Type 1 fimbriae are heteropolymeric surface organelles responsible for the D-mannose-sensitive (MS) adhesion of Escherichia coli. We recently reported that variation of receptor specificity of type 1 fimbriae can result solely from minor alterations in the structure of the gene for the FimH adhesin subunit. To further study the relationship between allelic variation of the fimH gene and adhesive properties of type 1 fimbriae, the fimH genes from five additional strains were cloned and used to complement the FimH deletion in E. coli KB18. When the parental and recombinant strains were tested for adhesion to immobilized mannan, a wide quantitative range in the ability of bacteria to adhere was noted. The differences in adhesion do not appear to be due to differences in the levels of fimbriation or relative levels of incorporation of FimH, because these parameters were similar in low-adhesion and high-adhesion strains. The nucleotide sequence for each of the fimH genes was determined. Analysis of deduced FimH sequences allowed identification of two sequence homology groups, based on the presence of Asn-70 and Ser-78 or Ser-70 and Asn-78 residues. The consensus sequences for each group conferred very low adhesion activity, and this low-adhesion phenotype predominated among a group of 43 fecal isolates. Strains isolated from a different host niche, the urinary tract, expressed type 1 fimbriae that conferred an increased level of adhesion. The results presented here strongly suggest that the quantitative variations in MS adhesion are due primarily to structural differences in the FimH adhesin. The observed differences in MS adhesion among populations of E. coli isolated from different host niches call attention to the possibility that phenotypic variants of FimH may play a functional role in populations dynamics.

摘要

1型菌毛是一种异聚体表面细胞器,负责大肠杆菌对D - 甘露糖敏感(MS)的黏附。我们最近报道,1型菌毛受体特异性的变化可能仅源于FimH黏附素亚基基因结构的微小改变。为了进一步研究fimH基因的等位基因变异与1型菌毛黏附特性之间的关系,我们克隆了另外五个菌株的fimH基因,并用于补充大肠杆菌KB18中的FimH缺失。当对亲本菌株和重组菌株进行对固定化甘露聚糖的黏附测试时,发现细菌黏附能力存在广泛的定量差异。黏附差异似乎不是由于菌毛形成水平或FimH掺入相对水平的差异,因为这些参数在低黏附菌株和高黏附菌株中相似。测定了每个fimH基因的核苷酸序列。基于Asn - 70和Ser - 78或Ser - 70和Asn - 78残基的存在,对推导的FimH序列进行分析,确定了两个序列同源组。每组的共有序列赋予非常低的黏附活性,并且这种低黏附表型在一组43个粪便分离株中占主导。从不同宿主生态位(泌尿道)分离的菌株表达的1型菌毛具有更高的黏附水平。此处呈现的结果强烈表明,MS黏附的定量变化主要是由于FimH黏附素的结构差异。在从不同宿主生态位分离的大肠杆菌群体中观察到的MS黏附差异,引起了人们对FimH表型变异体可能在群体动态中发挥功能作用的可能性的关注。