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蓝氏贾第鞭毛虫变异表面蛋白H7主要抗原区域的分子特征分析

Molecular characterisation of a predominant antigenic region of Giardia lamblia variant surface protein H7.

作者信息

Bienz M, Wittwer P, Zimmermann V, Müller N

机构信息

Institute of Parasitology, University of Berne, Länggass-Strasse 122, CH-3012 Berne, Switzerland.

出版信息

Int J Parasitol. 2001 Jun;31(8):827-32. doi: 10.1016/s0020-7519(01)00182-5.

Abstract

During infection, the intestinal protozoan parasite Giardia lamblia undergoes continuous antigenic variation which is determined by diversification of the parasite's major surface antigen, named VSP (variant surface protein). One member from this protein family, VSP H7, is expressed by G. lamblia clone GS/M-83-H7. In the present study, we characterised a highly antigenic portion of VSP H7 which is positioned inside a 130 amino acid C-terminal region of the protein. This region overlaps with a cysteine-rich motif that is rather conserved within the VSP family. Detailed molecular dissection of the antigenic portion monitored a 12 amino acid peptidyl structure which constitutes a non-conformational epitope of VSP H7. In the murine host, this epitope is recognised relatively early (before day 10 p.i.) during infection and stimulates a strong intestinal immunoglobulin A response. At late infective stages (after day 10 p.i.) this immune reaction is progressively complemented by reactions against 'late' antigenic epitopes which are also located inside the 130 amino acid antigenic portion but in closer proximity to the C-terminal end of VSP H7 than the 12 amino acid epitope. Both the high antigenicity and the conserved character suggest that the 12 amino acid epitope is a key factor within the immunological interplay between G. lamblia and the experimental murine host.

摘要

在感染过程中,肠道原生动物寄生虫蓝氏贾第鞭毛虫会持续发生抗原变异,这是由该寄生虫主要表面抗原(称为VSP,即变异表面蛋白)的多样化所决定的。这个蛋白家族的一个成员VSP H7由蓝氏贾第鞭毛虫克隆株GS/M - 83 - H7表达。在本研究中,我们对VSP H7的一个高度抗原性部分进行了表征,该部分位于该蛋白130个氨基酸的C末端区域内。这个区域与VSP家族中相当保守的富含半胱氨酸的基序重叠。对抗原性部分的详细分子剖析监测到一个由12个氨基酸组成的肽基结构,它构成了VSP H7的一个非构象表位。在鼠类宿主中,这个表位在感染期间相对较早(感染后第10天之前)被识别,并刺激强烈的肠道免疫球蛋白A反应。在感染后期(感染后第10天之后),这种免疫反应逐渐被针对“晚期”抗原表位的反应所补充,这些表位也位于130个氨基酸的抗原性部分内,但比12个氨基酸的表位更靠近VSP H7的C末端。高抗原性和保守性都表明,12个氨基酸的表位是蓝氏贾第鞭毛虫与实验性鼠类宿主之间免疫相互作用的关键因素。

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