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VAR2CSA 蛋白的硫酸软骨素 A 结合位点涉及多个 N 端结构域。

The chondroitin sulfate A-binding site of the VAR2CSA protein involves multiple N-terminal domains.

机构信息

Department of International Health, Immunology, University of Copenhagen and the Department of Infectious Diseases, Copenhagen University Hospital (Rigshospitalet), Copenhagen K, Denmark.

出版信息

J Biol Chem. 2011 May 6;286(18):15908-17. doi: 10.1074/jbc.M110.191510. Epub 2011 Mar 11.

Abstract

Malaria during pregnancy is a major health problem for African women. The disease is caused by Plasmodium falciparum malaria parasites, which accumulate in the placenta by adhering to chondroitin sulfate A (CSA). The interaction between infected erythrocytes and the placental receptor is mediated by a parasite expressed protein named VAR2CSA. A vaccine protecting pregnant women against placental malaria should induce antibodies inhibiting the interaction between VAR2CSA and CSA. Much effort has been put into defining the part of the 350 kDa VAR2CSA protein that is responsible for binding. It has been shown that full-length recombinant VAR2CSA binds specifically to CSA with high affinity, however to date no sub-fragment of VAR2CSA has been shown to interact with CSA with similar affinity or specificity. In this study, we used a biosensor technology to examine the binding properties of a panel of truncated VAR2CSA proteins. The experiments indicate that the core of the CSA-binding site is situated in three domains, DBL2X-CIDR(PAM) and a flanking domain, located in the N-terminal part of VAR2CSA. Furthermore, recombinant VAR2CSA subfragments containing this region elicit antibodies with high parasite adhesion blocking activity in animal immunization experiments.

摘要

怀孕期间疟疾是非洲妇女面临的一个主要健康问题。这种疾病是由恶性疟原虫寄生虫引起的,寄生虫通过黏附硫酸软骨素 A(CSA)而在胎盘内积聚。受感染的红细胞与胎盘受体之间的相互作用是由一种名为 VAR2CSA 的寄生虫表达蛋白介导的。一种能保护孕妇免受胎盘疟疾的疫苗应该能诱导出抑制 VAR2CSA 与 CSA 相互作用的抗体。人们已经投入大量精力来确定负责结合的 350 kDa VAR2CSA 蛋白的部分。已经表明全长重组 VAR2CSA 与 CSA 特异性高亲和力结合,然而迄今为止,还没有显示出 VAR2CSA 的任何亚片段以类似的亲和力或特异性与 CSA 相互作用。在这项研究中,我们使用生物传感器技术来研究一组截断的 VAR2CSA 蛋白的结合特性。实验表明,CSA 结合位点的核心位于三个结构域、DBL2X-CIDR(PAM)和一个侧翼结构域,位于 VAR2CSA 的 N 端部分。此外,含有该区域的重组 VAR2CSA 亚片段在动物免疫实验中引发了具有高寄生虫黏附阻断活性的抗体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7185/3091200/dff6524f7c84/zbc0241161250001.jpg

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