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克氏锥虫富谷氨酸/丙氨酸蛋白的结构特征和表位作图:定义寄生虫细胞表面的组装。

Structural characterization and epitope mapping of the glutamic acid/alanine-rich protein from Trypanosoma congolense: defining assembly on the parasite cell surface.

机构信息

Department of Biochemistry and Microbiology, University of Victoria, Victoria, British Columbia V8W 3P6, Canada.

出版信息

J Biol Chem. 2011 Jun 10;286(23):20658-65. doi: 10.1074/jbc.M111.218941. Epub 2011 Apr 6.

DOI:10.1074/jbc.M111.218941
PMID:21471223
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3121512/
Abstract

Trypanosoma congolense is an African trypanosome that causes serious disease in cattle in Sub-Saharan Africa. The four major life cycle stages of T. congolense can be grown in vitro, which has led to the identification of several cell-surface molecules expressed on the parasite during its transit through the tsetse vector. One of these, glutamic acid/alanine-rich protein (GARP), is the first expressed on procyclic forms in the tsetse midgut and is of particular interest because it replaces the major surface coat molecule of bloodstream forms, the variant surface glycoprotein (VSG) that protects the parasite membrane, and is involved in antigenic variation. Unlike VSG, however, the function of GARP is not known, which necessarily limits our understanding of parasite survival in the tsetse. Toward establishing the function of GARP, we report its three-dimensional structure solved by iodide phasing to a resolution of 1.65 Å. An extended helical bundle structure displays an unexpected and significant degree of homology to the core structure of VSG, the only other major surface molecule of trypanosomes to be structurally characterized. Immunofluorescence microscopy and immunoaffinity-tandem mass spectrometry were used in conjunction with monoclonal antibodies to map both non-surface-disposed and surface epitopes. Collectively, these studies enabled us to derive a model describing the orientation and assembly of GARP on the surface of trypanosomes. The data presented here suggest the possible structure-function relationships involved in replacement of the bloodstream form VSG by GARP as trypanosomes differentiate in the tsetse vector after a blood meal.

摘要

冈比亚锥虫是一种在撒哈拉以南非洲地区引起牛严重疾病的非洲锥虫。冈比亚锥虫的四个主要生命周期阶段可以在体外生长,这导致了在其通过采采蝇媒介传播过程中在寄生虫表面表达的几种细胞表面分子的鉴定。其中一种是谷氨酸/丙氨酸丰富蛋白(GARP),它是在采采蝇中肠中循环形式上最早表达的,特别有趣,因为它取代了血腔形式的主要表面被膜分子,即变异表面糖蛋白(VSG),保护寄生虫膜,并参与抗原变异。然而,与 VSG 不同,GARP 的功能尚不清楚,这必然限制了我们对寄生虫在采采蝇中生存的理解。为了确定 GARP 的功能,我们报告了其通过碘化物相测定到 1.65 Å分辨率的三维结构。扩展的螺旋束结构显示出与 VSG 的核心结构出乎意料的高度同源性,VSG 是唯一结构特征明确的其他主要表面分子的锥虫。免疫荧光显微镜和免疫亲和串联质谱联用单克隆抗体用于定位非表面暴露和表面表位。这些研究的综合结果使我们能够得出一个描述 GARP 在锥虫表面的取向和组装的模型。这里提出的数据表明,在采采蝇媒介中,当寄生虫在血液餐之后分化时,GARP 可能取代血腔形式的 VSG 的结构-功能关系。

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Tsetse EP protein protects the fly midgut from trypanosome establishment.采采蝇 EP 蛋白保护蝇的中肠免受锥虫的建立。
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