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蛋白质中抗原决定簇的结构。

The structure of an antigenic determinant in a protein.

作者信息

Wilson I A, Niman H L, Houghten R A, Cherenson A R, Connolly M L, Lerner R A

出版信息

Cell. 1984 Jul;37(3):767-78. doi: 10.1016/0092-8674(84)90412-4.

Abstract

The immunogenic and antigenic determinants of a synthetic peptide and the corresponding antigenic determinants in the parent protein have been elucidated. Four determinants have been defined by reactivity of a large panel of antipeptide monoclonal antibodies with short, overlapping peptides (7-28 amino acids), the immunizing peptide (36 amino acids), and the intact parent protein (the influenza virus hemagglutinin, HA). The majority of the antipeptide antibodies that also react strongly with the intact protein recognize one specific nine amino acid sequence. This immunodominant peptide determinant is located in the subunit interface in the HA trimeric structure. The relative inaccessibility of this site implies that antibody binding to the protein is to a more unfolded HA conformation. This antigenic determinant differs from those previously described for the hemagglutinin and clearly demonstrates the ability of synthetic peptides to generate antibodies that interact with regions of the protein not immunogenic or generally accessible when the protein is the immunogen.

摘要

一种合成肽的免疫原性和抗原决定簇以及亲本蛋白中的相应抗原决定簇已得到阐明。通过大量抗肽单克隆抗体与短的重叠肽(7 - 28个氨基酸)、免疫肽(36个氨基酸)以及完整的亲本蛋白(流感病毒血凝素,HA)的反应性,确定了四个决定簇。大多数也能与完整蛋白强烈反应的抗肽抗体识别一个特定的九氨基酸序列。这个免疫显性肽决定簇位于HA三聚体结构的亚基界面。该位点相对难以接近,这意味着抗体与蛋白的结合是针对更未折叠的HA构象。这个抗原决定簇与先前描述的血凝素的抗原决定簇不同,并且清楚地证明了合成肽产生与当蛋白作为免疫原时无免疫原性或通常无法接近的蛋白区域相互作用的抗体的能力。

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