首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Protection against Invasive Amebiasis by a Single Monoclonal Antibody Directed against a Lipophosphoglycan Antigen Localized on the Surface of Entamoeba histolytica
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Protection against Invasive Amebiasis by a Single Monoclonal Antibody Directed against a Lipophosphoglycan Antigen Localized on the Surface of Entamoeba histolytica

机译:针对针对脂解糖蛋白表面溶脂阿米巴表面上的脂磷酸聚糖抗原的单克隆抗体的侵袭性阿米巴病的保护。

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摘要

A panel of monoclonal antibodies was raised from mice immunized with a membrane preparation from Entamoeba histolytica, the pathogenic species causing invasive amebiasis in humans. Antibody EH5 gave a polydisperse band in immunoblots from membrane preparations from different E. histolytica strains, and a much weaker signal from two strains of the nonpathogenic species Entamoeba dispar. Although the exact chemical structure of the EH5 antigen is not yet known, the ability of the antigen to be metabolically radiolabeled with [32P]phosphate or [3H]glucose, its sensitivity to digestion by mild acid and phosphatidylinositol-specific phospholipase C, and its specific extraction from E. histolytica trophozoites by a method used to prepare lipophosphoglycans from Leishmania showed that it could be classified as an amebal lipophosphoglycan. Confocal immunofluorescence and immunogold labeling of trophozoites localized the antigen on the outer face of the plasma membrane and on the inner face of internal vesicle membranes. Antibody EH5 strongly agglutinated amebas in a similar way to concanavalin A (Con A), and Con A bound to immunoaffinity-purified EH5 antigen. Therefore, surface lipophosphoglycans may play an important role in the preferential agglutination of pathogenic amebas by Con A. The protective ability of antibody EH5 was tested in a passive immunization experiment in a severe combined immunodeficient (SCID) mouse model. Intrahepatic challenge of animals after administration of an isotype-matched control antibody or without treatment led to the development of a liver abscess in all cases, whereas 11 out of 12 animals immunized with the EH5 antibody developed no liver abscess. Our results demonstrate the importance and, for the first time, the protective capacity of glycan antigens on the surface of the amebas.
机译:从用溶组织性变形杆菌(Entamoeba histolytica)的膜制剂免疫的小鼠中产生一组单克隆抗体,所述致病性物种引起人的侵袭性阿米巴病。抗体EH5在来自不同溶组织性大肠杆菌菌株的膜制剂的免疫印迹中产生了一条多分散带,而来自两种非致病性物种Entamoeba dispar的菌株的信号弱得多。尽管EH5抗原的确切化学结构尚不清楚,但是抗原可以通过[ 32 P]磷酸或[ 3 H]葡萄糖进行放射性标记,其对弱酸和磷脂酰肌醇特异性磷脂酶C消化的敏感性,以及通过用于从利什曼原虫中制备脂磷酸聚糖的方法从组织溶埃希氏菌滋养体中特异性提取的结果表明,它可以被归类为阿米巴脂磷酸聚糖。共焦免疫荧光和滋养体的免疫金标记将抗原定位在质膜的外表面和内囊膜的内表面。抗体EH5以与伴刀豆球蛋白A(Con A)类似的方式强烈凝集阿米巴,而Con A则与免疫亲和纯化的EH5抗原结合。因此,表面脂质磷酸聚糖可能在Con A致病性阿米巴的优先凝集中起重要作用。在严重的联合免疫缺陷(SCID)小鼠模型的被动免疫实验中测试了抗体EH5的保护能力。在所有情况下,给予同种型匹配的对照抗体或未经治疗的动物肝内攻击均会导致肝脓肿的形成,而用EH5抗体免疫的12只动物中有11只没有肝脓肿。我们的结果首次证明了阿米巴斯表面上聚糖抗原的重要性和保护能力。

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