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Epitope mapping of Ebola virus dominant and subdominant glycoprotein epitopes facilitates construction of an epitope-based DNA vaccine able to focus the antibody response in mice

机译:埃博拉病毒占优势和亚下芽糖蛋白表位的表位测绘促进了能够将抗体反应聚焦小鼠的表位的DNA疫苗的构建

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We performed epitope mapping studies on the major surface glycoprotein (GP) of Ebola virus (EBOV) using Chemically Linked Peptides on Scaffolds (CLIPS), which form linear and potential conformational epitopes. This method identified monoclonal antibody epitopes and predicted additional epitopes recognized by antibodies in polyclonal sera from animals experimentally vaccinated against or infected with EBOV. Using the information obtained along with structural modeling to predict epitope accessibility, we then constructed 2 DNA vaccines encoding immunodominant and subdominant epitopes predicted to be accessible on EBOV GP. Although a construct designed to produce a membrane-bound oligopeptide was poorly immunogenic, a construct generating a secreted oligopeptide elicited strong antibody responses in mice. When this construct was administered as a boost to a DNA vaccine expressing the complete EBOV GP gene, the resultant antibody response was focused largely toward the less immunodominant epitopes in the oligopeptide. Taken together, the results of this work suggest a utility for this method for immune focusing of antibody responses elicited by vaccination.
机译:我们在支架(夹子)上使用化学连接的肽对埃博拉病毒(EBOV)的主要表面糖蛋白(GP)进行表位映射研究,其形成线性和潜在的构象表位。该方法鉴定了单克隆抗体表位和预测来自多克隆血清中的抗体的额外表位,该抗体来自实验疫苗或用EBOV的动物进行了实验疫苗的动物。使用与结构建模一起获得的信息以预测表位可接近性,然后构建编码的2DNA疫苗编码免疫肿瘤,预测可在EBOV GP上访问。尽管设计用于产生膜结合的寡肽的构造是免疫原性差的,但是产生的构建体产生分泌的寡肽在小鼠中引起的强抗体应答。当将该构建体作为增压施用到表达完全EBOV GP基因的DNA疫苗时,所得抗体反应的主要掺入寡肽中的较低免疫素表位。结合在一起,这项工作的结果表明这种方法用于这种通过疫苗引起的抗体反应的免疫聚焦方法。

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