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Identification of IgE

机译:IgE的鉴定

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Progress in protein chemistry in the 1950s revealed that the biologic activities of proteins, such as hemoglobin and enzymes, are based on partial structures in the protein molecules. This principle suggested to us the possibility that the human antibodies responsible for induction of reaginic hypersensitivity reactions might have unique structures that are lacking in the antibody molecules involved in immunity and that the differences in the structures of human antibody molecules can be recognized by the immune systems of experimental animals. Our studies were based on the hypothesis that reaginic antibody activity is associated with a unique immunoglobulin isotype, which is now called IgE. As expected, identification of IgE facilitated the analysis of immunologic mechanisms of reaginic hypersensitivity. Subsequent studies revealed that IgE specifically bound to basophilic granulocytes and mast cells through the Fc portion of the molecules and that cross-linking of the cell-bound IgE antibody molecules by allergen induced the release of bioactive mediators, such as histamine and leukotrienes, which initiate allergic reactions. (J Allergy Clin Immunol 2016;137:1646-50.)
机译:1950年代蛋白质化学的进步表明,诸如血红蛋白和酶之类的蛋白质的生物学活性是基于蛋白质分子中的部分结构的。该原理向我们建议了一种可能性,即负责诱发尿素超敏反应的人抗体可能具有独特的结构,而这种结构缺乏参与免疫的抗体分子,而且人抗体分子的结构差异可以被免疫系统识别实验动物。我们的研究基于假说,即尿囊素抗体活性与独特的免疫球蛋白同种型(现称为IgE)相关。正如预期的那样,IgE的鉴定有助于对尿素超敏反应的免疫学机制进行分析。随后的研究表明,IgE通过分子的Fc部分与嗜碱性粒细胞和肥大细胞特异性结合,并且变应原与细胞结合的IgE抗体分子的交联诱导了生物活性介质(例如组胺和白三烯)的释放,这些介质可以启动过敏反应。 (《过敏临床免疫杂志》 2016年; 137:1646-50。)

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