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嗜碱性粒细胞和肥大细胞表面诱导脱颗粒的免疫事件。

Immunological events at the surface of basophil granulocytes and mast cells which induce degranulation.

作者信息

Ishizaka T, Ishizaka K

出版信息

Scand J Respir Dis Suppl. 1977;98:13-22.

PMID:72408
Abstract

IgE molecules combine with basophil granulocytes and mast cells through the Fc portion and sensitize these cells for reaginic hypersensitivity reactions. The number of receptors for IgE per human basophil granulocyte is estimated to be 40,000 to 100,000 and those on rat mast cells is about 300,000. The binding of IgE with the receptor is reversible and does not involve covalent bonding. The affinity of IgE molecules for the receptors is high; the equilibrium constant of the reaction is in the order of 10(9)/mole for both human basophils and rat mast cell systems. Such a high affinity will explain why a minute amount of IgE antibody can sensitize the target cells and why sensitization with the antibody is so persistent. The initial step of the reaginic hypersensitivity reactions is probably bridging of cell-bound IgE molecules by antigen, which activates enzymatic sequences. The release of chemical mediators, however, is controlled by pharmacological factors which have most important rôles in transducing immunological signals into intracellular signals and subsequent biochemical processes.

摘要

IgE分子通过Fc部分与嗜碱性粒细胞和肥大细胞结合,使这些细胞对反应素性超敏反应敏感。据估计,每个人类嗜碱性粒细胞上IgE受体的数量为40,000至100,000个,而大鼠肥大细胞上的受体数量约为300,000个。IgE与受体的结合是可逆的,不涉及共价键。IgE分子与受体的亲和力很高;人类嗜碱性粒细胞和大鼠肥大细胞系统反应的平衡常数约为10(9)/摩尔。如此高的亲和力可以解释为什么微量的IgE抗体就能使靶细胞致敏,以及为什么抗体致敏如此持久。反应素性超敏反应的初始步骤可能是抗原使细胞结合的IgE分子桥联,从而激活酶促序列。然而,化学介质的释放受药理学因素控制,这些因素在将免疫信号转导为细胞内信号及随后的生化过程中起最重要作用。

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