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用溶组织内阿米巴表面金属蛋白酶EhMSP-1进行免疫可保护仓鼠免受阿米巴肝脓肿的侵害。

Immunization with the Entamoeba histolytica surface metalloprotease EhMSP-1 protects hamsters from amebic liver abscess.

作者信息

Roncolato Eduardo C, Teixeira José E, Barbosa José E, Zambelli Ramalho Leandra N, Huston Christopher D

机构信息

Department of Biochemistry and Immunology, Ribeirão Preto Medical School, University of São Paulo, Ribeirão Preto, Brazil.

Department of Medicine, University of Vermont, Burlington, Vermont, USA.

出版信息

Infect Immun. 2015 Feb;83(2):713-20. doi: 10.1128/IAI.02490-14. Epub 2014 Dec 1.

Abstract

Diarrhea and amebic liver abscesses due to invasive Entamoeba histolytica infections are an important cause of morbidity and mortality in the developing world. Entamoeba histolytica adherence and cell migration, two phenotypes linked to virulence, are both aberrant in trophozoites deficient in the metallosurface protease EhMSP-1, which is a homologue of the Leishmania vaccine candidate leishmanolysin (GP63). We examined the potential of EhMSP-1 for use as a vaccine antigen to protect against amebic liver abscesses. First, existing serum samples from South Africans naturally infected with E. histolytica were examined by enzyme-linked immunosorbent assay (ELISA) for the presence of EhMSP-1-specific IgG. Nine of 12 (75%) people with anti-E. histolytica IgG also had EhMSP-1-specific IgG antibodies. We next used a hamster model of amebic liver abscess to determine the effect of immunization with a mixture of four recombinant EhMSP-1 protein fragments. EhMSP-1 immunization stimulated a robust IgG antibody response. Furthermore, EhMSP-1 immunization of hamsters reduced development of severe amebic liver abscesses following intrahepatic injection of E. histolytica by a combined rate of 68% in two independent animal experiments. Purified IgG from immunized compared to control animals bound to the surface of E. histolytica trophozoites and accelerated amebic lysis via activation of the classical complement cascade. We concluded that EhMSP-1 is a promising antigen that warrants further study to determine its full potential as a target for therapy and/or prevention of invasive amebiasis.

摘要

侵袭性溶组织内阿米巴感染所致的腹泻和阿米巴肝脓肿是发展中国家发病和死亡的重要原因。溶组织内阿米巴的黏附及细胞迁移这两种与毒力相关的表型,在缺乏金属表面蛋白酶EhMSP-1的滋养体中均异常,EhMSP-1是利什曼原虫疫苗候选物利什曼溶素(GP63)的同源物。我们研究了EhMSP-1作为疫苗抗原来预防阿米巴肝脓肿的潜力。首先,通过酶联免疫吸附测定(ELISA)检测来自自然感染溶组织内阿米巴的南非人的现有血清样本中是否存在EhMSP-1特异性IgG。12名抗溶组织内阿米巴IgG的人中,有9人(75%)也有EhMSP-1特异性IgG抗体。接下来,我们使用阿米巴肝脓肿的仓鼠模型来确定用四种重组EhMSP-1蛋白片段的混合物进行免疫的效果。EhMSP-1免疫刺激了强烈的IgG抗体反应。此外,在两项独立的动物实验中,对仓鼠进行EhMSP-1免疫后,肝内注射溶组织内阿米巴后严重阿米巴肝脓肿的发生率综合降低了68%。与对照动物相比,免疫动物的纯化IgG与溶组织内阿米巴滋养体表面结合,并通过激活经典补体级联反应加速阿米巴溶解。我们得出结论,EhMSP-1是一种有前景的抗原,值得进一步研究以确定其作为侵袭性阿米巴病治疗和/或预防靶点的全部潜力。

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