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T-dependent B cell responses to Plasmodium induce antibodies that form a high-avidity multivalent complex with the circumsporozoite protein

机译:T依赖的B细胞对疟原虫的反应诱导抗体与环子孢子蛋白形成高亲和力的多价复合物

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摘要

The repeat region of the Plasmodium falciparum circumsporozoite protein (CSP) is a major vaccine antigen because it can be targeted by parasite neutralizing antibodies; however, little is known about this interaction. We used isothermal titration calorimetry, X-ray crystallography and mutagenesis-validated modeling to analyze the binding of a murine neutralizing antibody to Plasmodium falciparum CSP. Strikingly, we found that the repeat region of CSP is bound by multiple antibodies. This repeating pattern allows multiple weak interactions of single FAB domains to accumulate and yield a complex with a dissociation constant in the low nM range. Because the CSP protein can potentially cross-link multiple B cell receptors (BCRs) we hypothesized that the B cell response might be T cell independent. However, while there was a modest response in mice deficient in T cell help, the bulk of the response was T cell dependent. By sequencing the BCRs of CSP-repeat specific B cells in inbred mice we found that these cells underwent somatic hypermutation and affinity maturation indicative of a T-dependent response. Last, we found that the BCR repertoire of responding B cells was limited suggesting that the structural simplicity of the repeat may limit the breadth of the immune response.
机译:恶性疟原虫环子孢子蛋白(CSP)的重复区是主要的疫苗抗原,因为它可以被寄生虫中和抗体靶向。但是,对此交互作用知之甚少。我们使用等温滴定热法,X射线晶体学和诱变验证模型来分析鼠中和抗体与恶性疟原虫CSP的结合。令人惊讶地,我们发现CSP的重复区被多种抗体结合。这种重复模式允许单个FAB域的多次弱相互作用积累并产生具有低nM范围内解离常数的复合物。因为CSP蛋白可能潜在地交联多个B细胞受体(BCR),所以我们假设B细胞反应可能与T细胞无关。但是,尽管在缺乏T细胞帮助的小鼠中有适度的反应,但大部分反应是T细胞依赖性的。通过对近交小鼠中CSP重复特异性B细胞的BCR进行测序,我们发现这些细胞进行了体细胞超突变和亲和力成熟,表明存在T依赖性反应。最后,我们发现应答B细胞的BCR曲目有限,这表明重复序列的结构简单性可能会限制免疫应答的广度。

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