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炭疽芽孢杆菌S层蛋白的SLH基序与枯草芽孢杆菌果聚糖蔗糖酶之间功能性融合体的产生及细胞表面锚定

Production and cell surface anchoring of functional fusions between the SLH motifs of the Bacillus anthracis S-layer proteins and the Bacillus subtilis levansucrase.

作者信息

Mesnage S, Tosi-Couture E, Fouet A

机构信息

Toxines et Pathogénie Bactériennes (URA 1858, CNRS), Paris, France.

出版信息

Mol Microbiol. 1999 Feb;31(3):927-36. doi: 10.1046/j.1365-2958.1999.01232.x.

Abstract

Many surface proteins of Gram-positive bacteria contain motifs, about 50 amino acids long, called S-layer homology (SLH) motifs. Bacillus anthracis, the causal agent of anthrax, synthesizes two S-layer proteins, each with three SLH motifs towards the amino-terminus. We used biochemical and genetic approaches to investigate the involvement of these motifs in cell surface anchoring. Proteinase K digestion produced polypeptides lacking these motifs, and stable three-motif polypeptides were produced in Escherichia coli that were able to bind the B. anthracis cell walls in vitro, demonstrating that the three SLH motifs were organized into a cell surface anchoring domain. We also determined the function of these SLH domains by constructing chimeric genes encoding the SLH domains fused to the normally secreted levansucrase of Bacillus subtilis. Cell fractionation and electron microscopy studies showed that each three-motif domain was sufficient for the efficient anchoring of levansucrase onto the cell surface. Proteins consisting of truncated SLH domains fused to levansucrase were unstable and associated poorly with the cell surface. Surface-exposed levansucrase retained its enzymatic and antigenic properties.

摘要

许多革兰氏阳性菌的表面蛋白含有约50个氨基酸长的基序,称为S层同源性(SLH)基序。炭疽病的病原体炭疽芽孢杆菌合成两种S层蛋白,每种蛋白在氨基末端都有三个SLH基序。我们使用生化和遗传学方法来研究这些基序在细胞表面锚定中的作用。蛋白酶K消化产生了缺乏这些基序的多肽,并且在大肠杆菌中产生了稳定的三基序多肽,这些多肽能够在体外结合炭疽芽孢杆菌细胞壁,表明这三个SLH基序被组织成一个细胞表面锚定结构域。我们还通过构建编码与枯草芽孢杆菌正常分泌的蔗糖转化酶融合的SLH结构域的嵌合基因来确定这些SLH结构域的功能。细胞分级分离和电子显微镜研究表明,每个三基序结构域足以将蔗糖转化酶有效地锚定到细胞表面。由与蔗糖转化酶融合的截短SLH结构域组成的蛋白质不稳定,并且与细胞表面的结合较差。表面暴露的蔗糖转化酶保留了其酶活性和抗原特性。

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