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通过蛋白质印迹法分析不同形式恰加斯病患者血清中抗克氏锥虫抗体的同种型特异性。

Analysis of anti-Trypanosoma cruzi antibody isotype specificities by western blot in sera from patients with different forms of Chagas' disease.

作者信息

Morgan J, Colley D G, Pinto Dias J C, Gontijo E D, Bahia-Oliveira L, Correa-Oliveira R, Powell M R

机构信息

Immunology Branch, Division of Parasitic Diseases, National Center for Infectious Diseases, Centers for Disease Control and Prevention, U.S. Department of Health and Human Services, Atlanta, Georgia 30341-3724, USA.

出版信息

J Parasitol. 1998 Jun;84(3):641-3.

PMID:9645878
Abstract

Infection of humans with Trypanosoma cruzi leads to either a lifelong asymptomatic infection or to symptomatic presentations such as cardiomyopathy, mega-syndromes, or both. The reasons for the different clinical manifestations are not understood. We have previously studied a group of chronically infected individuals with different clinical forms of Chagas' disease and found that the levels of some anti-T. cruzi antibody isotypes, analyzed by enzyme-linked immunosorbent assay, differed among patients with different clinical presentations. We have expanded these studies to examine the antigen specificity of these patients' IgG1, 2, 3, IgM, and IgA by western blot. We observed that binding of particular antigens by some antibody isotypes were more prevalent in some clinical groups as compared to others. For example, IgG3 from 13 of 19 (68%) individuals with digestive manifestations bound a 68-kDa antigen, but only 3 of 31 (9%) individuals with cardiac involvement detected this same moiety. We also found that, regardless of the clinical group, the profiles of antigens recognized by each antibody isotype differs dramatically from the profiles recognized by each other isotype. Together with our previous observations demonstrating that the levels of anti-parasite antibody isotypes correlates with the clinical form, these data suggest that overall anti-T. cruzi antibody reactivities may indeed be skewed toward different antigens in individuals with different clinical presentations.

摘要

人类感染克氏锥虫会导致终身无症状感染或出现心肌病、巨型综合征等症状表现,或两者皆有。不同临床表现的原因尚不清楚。我们之前研究了一组患有不同临床形式恰加斯病的慢性感染个体,发现通过酶联免疫吸附测定分析,一些抗克氏锥虫抗体亚型的水平在不同临床表现的患者中存在差异。我们扩展了这些研究,通过蛋白质印迹法检测这些患者的IgG1、2、3、IgM和IgA的抗原特异性。我们观察到,与其他临床组相比,某些抗体亚型对特定抗原的结合在一些临床组中更为普遍。例如,19名有消化系统表现的个体中有13名(68%)的IgG3与一种68 kDa的抗原结合,但31名有心脏受累的个体中只有3名(9%)检测到相同的部分。我们还发现,无论临床组如何,每种抗体亚型识别的抗原谱与其他亚型识别的谱有很大差异。连同我们之前的观察结果表明抗寄生虫抗体亚型的水平与临床形式相关,这些数据表明,在不同临床表现的个体中,总体抗克氏锥虫抗体反应性可能确实偏向于不同的抗原。

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