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利用单克隆抗体鉴定磷脂酶C为霍乱弧菌O139双功能溶血素-磷脂酶C分子的肠毒素因子。

Use of monoclonal antibodies to identify phospholipase C as the enterotoxic factor of the bifunctional hemolysin-phospholipase C molecule of Vibrio cholerae O139.

作者信息

Pal S, Datta A, Nair G B, Guhathakurta B

机构信息

National Institute of Cholera and Enteric Diseases, Calcutta, India.

出版信息

Infect Immun. 1998 Aug;66(8):3974-7. doi: 10.1128/IAI.66.8.3974-3977.1998.

Abstract

Two hybrid clones producing monoclonal antibodies (MAbs) raised against the purified enterotoxic hemolysin-phospholipase C (HlyPC) bifunctional molecule of a Vibrio cholerae O139 strain were used to study its enterotoxicity in relation to its hemolytic and enzymatic activities. Fab fragments of MAbs from ascites produced by the two hybrids neutralized the hemolytic activity of HlyPC, leaving the enzymatic activity unaffected. In ligated rabbit ileal loop and infant mouse intestine, the Fab fragments of the MAbs were not able to neutralize the enterotoxicity of HlyPC, suggesting that PC rather than Hly is the enterotoxic moiety of the molecule. The enterotoxicity of the purified PC molecule isolated from an Hly- spontaneous mutant of the HlyPC-producing parent strain further confirms this contention. The Hly molecule isolated from a PC- mutant was not diarrheagenic.

摘要

使用两个杂交克隆产生的单克隆抗体(MAb)来研究霍乱弧菌O139菌株纯化的肠毒素溶血素-磷脂酶C(HlyPC)双功能分子的肠毒性与其溶血和酶活性的关系,这些单克隆抗体是针对该双功能分子产生的。这两个杂交瘤产生的腹水单克隆抗体的Fab片段中和了HlyPC的溶血活性,而酶活性未受影响。在结扎的兔回肠袢和幼鼠肠道中,单克隆抗体的Fab片段无法中和HlyPC的肠毒性,这表明该分子的肠毒性部分是磷脂酶C(PC)而非溶血素(Hly)。从产生HlyPC的亲本菌株的Hly自发突变体中分离出的纯化PC分子的肠毒性进一步证实了这一观点。从PC突变体中分离出的Hly分子不具有致腹泻性。

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本文引用的文献

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Purification and characterisation of a hemolysin with phospholipase C activity from Vibrio cholerae O139.
FEMS Microbiol Lett. 1997 Feb 1;147(1):115-20. doi: 10.1111/j.1574-6968.1997.tb10229.x.
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Bacterial phospholipases C.细菌磷脂酶C
Microbiol Rev. 1993 Jun;57(2):347-66. doi: 10.1128/mr.57.2.347-366.1993.
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Cloning and sequencing of a novel hemolysis gene of Vibrio cholerae.霍乱弧菌一种新型溶血基因的克隆与测序
FEMS Microbiol Lett. 1995 May 15;128(3):265-9. doi: 10.1111/j.1574-6968.1995.tb07534.x.
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