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受体结合的IgE交联形成大于二聚体的聚集体会导致快速固定。

Cross-linking of receptor-bound IgE to aggregates larger than dimers leads to rapid immobilization.

作者信息

Menon A K, Holowka D, Webb W W, Baird B

出版信息

J Cell Biol. 1986 Feb;102(2):541-50. doi: 10.1083/jcb.102.2.541.

Abstract

Controlled cross-linking of IgE-receptor complexes on the surface of rat basophilic leukemia cells and mast cells has allowed a comparison of the lateral mobility and cell triggering activity of monomers, dimers, and higher oligomers of receptors. Addition of a monoclonal anti-IgE(Fc) antibody to IgE-sensitized cells in stoichiometric amounts relative to IgE produces IgE-receptor dimers with high efficiency. These dimers are nearly as mobile as IgE-receptor monomers and trigger cellular degranulation poorly, but in the presence of 30% D2O, substantial immobilization of the dimers is seen and degranulation activity doubles. Addition of this monoclonal antibody in larger amounts results in the formation of larger oligomeric receptor clusters which are immobile and effectively trigger the cells. Thus, small receptor clusters that are active in stimulating degranulation are immobilized in a process that is not anticipated by simple hydrodynamic theories. Further experiments involving cross-linking of receptor-bound IgE by multivalent antigen demonstrate that immobilization of receptors occurs rapidly (less than 2 min) upon cross-linking and is fully and rapidly reversible by the addition of excess monovalent hapten. The rapidity and reversibility of the immobilization process are entirely consistent with the possibility that immobilization represents a recognition event between clustered receptors and cytoskeleton-associated components that plays an important role early in the cell triggering mechanism.

摘要

对大鼠嗜碱性白血病细胞和肥大细胞表面的IgE受体复合物进行可控交联,使得能够比较受体单体、二聚体及更高聚体的侧向流动性和细胞触发活性。相对于IgE,以化学计量的量向IgE致敏细胞中添加单克隆抗IgE(Fc)抗体,可高效产生IgE受体二聚体。这些二聚体的流动性与IgE受体单体几乎相同,且引发细胞脱颗粒的能力较差,但在30% D2O存在的情况下,可观察到二聚体大量固定,且脱颗粒活性加倍。添加大量这种单克隆抗体可导致形成更大的寡聚受体簇,这些簇不具有流动性且能有效触发细胞。因此,在刺激脱颗粒方面具有活性的小受体簇在一个简单流体动力学理论无法预测的过程中被固定。涉及通过多价抗原交联受体结合的IgE的进一步实验表明,交联后受体的固定迅速发生(不到2分钟),并且通过添加过量单价半抗原可完全且迅速逆转。固定过程的快速性和可逆性与以下可能性完全一致,即固定代表簇状受体与细胞骨架相关成分之间的识别事件,该事件在细胞触发机制的早期起着重要作用。

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