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用纯化的突变型志贺毒素1免疫小鼠对志贺毒素1攻击的保护作用。

Protection against Shiga toxin 1 challenge by immunization of mice with purified mutant Shiga toxin 1.

作者信息

Ishikawa Satoshi, Kawahara Kazuyoshi, Kagami Yutaka, Isshiki Yasunori, Kaneko Aki, Matsui Hidenori, Okada Nobuhiko, Danbara Hirofumi

机构信息

Department of Microbiology, School of Pharmaceutical Sciences, Kitasato University, Tokyo 108-8641, Japan.

出版信息

Infect Immun. 2003 Jun;71(6):3235-9. doi: 10.1128/IAI.71.6.3235-3239.2003.

Abstract

Shiga toxin 1 (Stx1) of enterohemorrhagic Escherichia coli O157:H7 was cloned, and four mutant Stx1s were constructed by site-directed mutagenesis with PCR. The wild-type and mutant Stx1s with amino acid replacements at positions 167 and 170 of the A subunit were purified by one-step affinity chromatography with commercially available Globotriose Fractogel, and the mutant Stxs were used for the immunization of mice. The mutant toxins were nontoxic to Vero cells in vitro and to mice in vivo and induced the immunoglobulin G antibody against the wild-type Stx1, which neutralized the cytotoxicity of Stx1. The induced antibody titers depended on the mutation at position 170 of the A subunit. The mice immunized with the mutant Stx1s were protected against a challenge of approximately 100 times the 50% lethal dose of the wild-type Stx1, suggesting that the mutant toxins are good candidates for toxoid vaccines for infection by Stx1-producing E. coli.

摘要

对肠出血性大肠杆菌O157:H7的志贺毒素1(Stx1)进行了克隆,并通过PCR定点诱变构建了四种突变型Stx1。利用市售的Globotriose Fractogel通过一步亲和层析法纯化了A亚基第167和170位氨基酸发生置换的野生型和突变型Stx1,并将突变型Stx用于小鼠免疫。突变毒素在体外对Vero细胞无毒,在体内对小鼠无毒,并诱导产生针对野生型Stx1的免疫球蛋白G抗体,该抗体可中和Stx1的细胞毒性。诱导的抗体滴度取决于A亚基第170位的突变。用突变型Stx1免疫的小鼠受到约100倍于野生型Stx1 50%致死剂量的攻击时得到了保护,这表明突变毒素是用于预防产Stx1大肠杆菌感染的类毒素疫苗的良好候选物。

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