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用于检测识别肠道贾第鞭毛虫和微小隐孢子虫抗原的免疫球蛋白G抗体的多重检测法。

Multiplex assay detection of immunoglobulin G antibodies that recognize Giardia intestinalis and Cryptosporidium parvum antigens.

作者信息

Priest Jeffrey W, Moss Delynn M, Visvesvara Govinda S, Jones Cara C, Li Anna, Isaac-Renton Judith L

机构信息

Division of Parasitic Diseases, Centers for Disease Control and Prevention, Atlanta, Georgia, USA.

出版信息

Clin Vaccine Immunol. 2010 Nov;17(11):1695-707. doi: 10.1128/CVI.00160-10. Epub 2010 Sep 28.

Abstract

Giardiasis and cryptosporidiosis are common enteric parasitic diseases that have similar routes of transmission. In this work, we have identified epitopes within the Giardia variant-specific surface protein (VSP) sequences that are recognized by IgG antibodies from 13 of 14 (93%) sera from patients with stool-confirmed giardiasis. The conserved epitopes are shared among VSPs from both of the assemblages that commonly infect humans, and they are likely to be structural, as both sodium dodecyl sulfate treatment and dithiothreitol reduction decrease antibody recognition. In a multiplex bead assay (MBA), we used three VSP fragments from an assemblage A Giardia strain, three VSP fragments from assemblage B strains, and the α-1 giardin structural antigen to detect IgG antibodies to Giardia and used the recombinant 17- and 27-kDa antigens to simultaneously detect IgG antibodies to Cryptosporidium. The MBA differentiated between sera from Giardia and Cryptosporidium outbreaks and also identified a giardiasis outbreak that may have included cryptosporidiosis cases. Approximately 40% of cryptosporidiosis outbreak samples had high MBA responses for both the 27- and 17-kDa antigens, while <10% of nonoutbreak and giardiasis outbreak samples had high responses. At least 60% of giardiasis outbreak samples were positive for antibodies to multiple Giardia antigens, while ≤12% of nonoutbreak samples and samples from U.S. and British Columbia cryptosporidiosis outbreaks met our definition for Giardia seropositivity. A MBA using multiple parasite antigens may prove useful in the epidemiologic analysis of future waterborne or food-borne outbreaks of diarrheal disease.

摘要

贾第虫病和隐孢子虫病是常见的肠道寄生虫病,传播途径相似。在本研究中,我们在贾第虫变异特异性表面蛋白(VSP)序列中鉴定出了表位,这些表位可被14例粪便确诊为贾第虫病患者血清中的13例(93%)IgG抗体识别。保守表位存在于通常感染人类的两个组合的VSP中,且可能具有结构特征,因为十二烷基硫酸钠处理和二硫苏糖醇还原都会降低抗体识别。在多重微珠分析(MBA)中,我们使用来自A组合贾第虫菌株的三个VSP片段、来自B组合菌株的三个VSP片段以及α-1贾第虫蛋白结构抗原检测贾第虫IgG抗体,并使用重组17 kDa和27 kDa抗原同时检测隐孢子虫IgG抗体。MBA能够区分贾第虫病和隐孢子虫病暴发的血清,还识别出一起可能包含隐孢子虫病病例的贾第虫病暴发。约40%的隐孢子虫病暴发样本对27 kDa和17 kDa抗原的MBA反应较高,而非暴发样本和贾第虫病暴发样本中该比例<10%。至少60%的贾第虫病暴发样本对多种贾第虫抗原的抗体呈阳性,而≤12%的非暴发样本以及来自美国和不列颠哥伦比亚隐孢子虫病暴发的样本符合我们对贾第虫血清阳性的定义。使用多种寄生虫抗原的MBA可能在未来水传播或食源性腹泻病暴发的流行病学分析中发挥作用。

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