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Direct and indirect interactions in the recognition between a cross-neutralizing antibody and the four serotypes of dengue virus

机译:交叉中和抗体与四种血清型登革热病毒之间识别过程中的直接和间接相互作用

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摘要

Dengue fever is the most important vector-borne viral disease. Four serotypes of dengue virus, DENV1 to DENV4, coexist. Secondary infection by a different serotype is a risk factor for severe dengue. Monoclonal antibody mAb4E11 neutralizes the four serotypes of DENV with varying efficacies by recognizing an epitope located within domain-III (ED3) of the viral envelope (E) protein. To better understand the cross-reactivities between mAb4E11 and the four serotypes of DENV, we constructed mutations in both Fab4E11 fragment and ED3, and we searched for indirect interactions in the crystal structures of the four complexes. According to the serotype, 7 to 12 interactions aremediated by one watermolecule, 1 to 10 by two water molecules, and several of these interactions are conserved between serotypes. Most interfacial water molecules make hydrogen bonds with both antibody and antigen. Some residues or atomic groups are engaged in both direct and water-mediated interactions. The doubly-indirect interactions are more numerous in the complex of lowest affinity. The third complementarity determining region of the light chain (L-CDR3) of mAb4E11 does not contact ED3. The structures and double-mutant thermodynamic cycles showed that the effects of (hyper)-mutations in L-CDR3 on affinity were caused by conformational changes and indirect interactions with ED3 through other CDRs. Exchanges of residues between ED3 serotypes showed that their effects on affinity were context dependent. Thus, conformational changes, structural context, and indirect interactions should be included when studying cross-reactivity between antibodies and different serotypes of viral antigens for a better design of diagnostics, vaccine, and therapeutic tools against DENV and other Flaviviruses.
机译:登革热是最重要的媒介传播病毒病。登革病毒DENV1至DENV4共有四种血清型。不同血清型的继发感染是严重登革热的危险因素。单克隆抗体mAb4E11通过识别位于病毒包膜(E)蛋白结构域III(ED3)内的表位,以不同的效率中和DENV的四种血清型。为了更好地了解mAb4E11与DENV的四种血清型之间的交叉反应性,我们在Fab4E11片段和ED3中构建了突变,并在这四种复合物的晶体结构中搜索了间接相互作用。根据血清型,一个水分子介导7至12个相互作用,两个水分子介导1至10个相互作用,并且这些相互作用中的几种在血清型之间是保守的。大多数界面水分子都与抗体和抗原形成氢键。一些残基或原子团同时参与直接和水介导的相互作用。在最低亲和力的复合物中,双-间接相互作用更多。 mAb4E11的轻链(L-CDR3)的第三个互补决定区不接触ED3。结构和双突变热力学循环表明,L-CDR3中的(超)突变对亲和力的影响是由构象变化和通过其他CDR与ED3的间接相互作用引起的。 ED3血清型之间的残基交换表明它们对亲和力的影响取决于环境。因此,在研究抗体与病毒血清的不同血清型之间的交叉反应性时,应包括构象变化,结构背景和间接相互作用,以更好地设计针对DENV和其他黄病毒的诊断,疫苗和治疗工具。

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