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葡萄球菌与生物膜。

Staphylococcus and biofilms.

作者信息

Götz Friedrich

机构信息

Department of Microbial Genetics, Universität Tübingen, Waldhäuser Str. 70/8, D-72076 Tübingen, Germany.

出版信息

Mol Microbiol. 2002 Mar;43(6):1367-78. doi: 10.1046/j.1365-2958.2002.02827.x.

DOI:10.1046/j.1365-2958.2002.02827.x
PMID:11952892
Abstract

The genetic and molecular basis of biofilm formation in staphylococci is multifaceted. The ability to form a biofilm affords at least two properties: the adherence of cells to a surface and accumulation to form multilayered cell clusters. A trademark is the production of the slime substance PIA, a polysaccharide composed of beta-1,6-linked N-acetylglucosamines with partly deacetylated residues, in which the cells are embedded and protected against the host's immune defence and antibiotic treatment. Mutations in the corresponding biosynthesis genes (ica operon) lead to a pleiotropic phenotype; the cells are biofilm and haemagglutination negative, less virulent and less adhesive on hydrophilic surfaces. ica expression is modulated by various environmental conditions, appears to be controlled by SigB and can be turned on and off by insertion sequence (IS) elements. A number of biofilm-negative mutants have been isolated in which polysaccharide intercellular adhesin (PIA) production appears to be unaffected. Two of the characterized mutants are affected in the major autolysin (atlE) and in D-alanine esterification of teichoic acids (dltA). Proteins have been identified that are also involved in biofilm formation, such as the accumulation-associated protein (AAP), the clumping factor A (ClfA), the staphylococcal surface protein (SSP1) and the biofilm-associated protein (Bap). Concepts for the prevention of obstinate polymer-associated infections include the search for new anti-infectives active in biofilms and new biocompatible materials that complicate biofilm formation and the development of vaccines.

摘要

葡萄球菌生物膜形成的遗传和分子基础是多方面的。形成生物膜的能力至少赋予两种特性:细胞粘附于表面并聚集形成多层细胞簇。一个标志性特征是产生黏液物质PIA,它是一种由β-1,6-连接的N-乙酰葡糖胺与部分脱乙酰化残基组成的多糖,细胞嵌入其中并受到保护,免受宿主免疫防御和抗生素治疗的影响。相应生物合成基因(ica操纵子)的突变导致多效性表型;细胞生物膜和血凝反应呈阴性,毒力较低,在亲水性表面上的粘附性也较低。ica的表达受多种环境条件调节,似乎受SigB控制,并可被插入序列(IS)元件开启和关闭。已经分离出许多生物膜阴性突变体,其中多糖细胞间粘附素(PIA)的产生似乎未受影响。两个已鉴定的突变体在主要自溶素(atlE)和磷壁酸的D-丙氨酸酯化(dltA)方面受到影响。已经鉴定出一些也参与生物膜形成的蛋白质,例如积累相关蛋白(AAP)、聚集因子A(ClfA)、葡萄球菌表面蛋白(SSP1)和生物膜相关蛋白(Bap)。预防顽固性聚合物相关感染的概念包括寻找对生物膜有活性的新型抗感染药物、使生物膜形成复杂化的新型生物相容性材料以及疫苗的研发。

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