在大鼠嗜碱性白血病细胞中,交联IgE受体与膜骨架的关联是独立于已知的信号机制的。

J R Apgar
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引用次数: 12

摘要

大鼠嗜碱性白血病(RBL)细胞表面的IgE受体通过多价抗原交联诱导这些受体与洗涤剂不溶性膜骨架的关联。通过使用IgE低聚物或IgE单体加多价抗原,也可以在从RBL细胞分离的纯化质膜上诱导受体的洗涤剂不溶性。受体与膜骨架相互作用的关键是受体的交联。这种关联是迅速的,当由多价抗原触发时,通过添加过量的单价抗原迅速逆转。使用纯化质膜时发生这种关联的事实表明,这种相互作用所需的所有成分都存在于质膜中,而细胞内成分则不需要。虽然受体的交联激活磷脂酶C和磷脂酶A2,导致几个第二信使的产生,但这些信号机制似乎都不参与IgE受体与膜骨架的相互作用。这种相互作用不能由phorbol 12-肉豆蔻酸13-乙酸酯(PMA)、离子霉素或这两种试剂的组合诱导,尽管这将导致脱粒。此外,当多价抗原触发时,受体洗涤剂不溶性与温度无关,因此表明酶催化反应并不重要。事实证明,多种阻断磷脂酰肌醇代谢、花生四烯酸代谢、Ca2+内流和蛋白激酶C (PKC)激活的抑制剂对抗原诱导的受体与膜骨架的关联没有影响。这些结果表明,导致脱颗粒反应的信号机制与交联受体与膜骨架的关联无关。
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Association of the crosslinked IgE receptor with the membrane skeleton is independent of the known signaling mechanisms in rat basophilic leukemia cells.

Crosslinking of the IgE receptor on the surface of rat basophilic leukemia (RBL) cells by multivalent antigen induces an association of these receptors with the detergent-insoluble membrane skeleton. Detergent insolubility of the receptor can also be induced on purified plasma membranes isolated from RBL cells by the use of either IgE oligomers or IgE monomers plus multivalent antigen. The critical event in initiating this interaction between the receptor and the membrane skeleton is cross-linking of the receptor. This association is rapid, and, when triggered by multivalent antigen, it is quickly reversed by the addition of excess monovalent antigen. The fact that this association occurs with the use of purified plasma membranes indicates that all of the components necessary for this interaction are present in the plasma membrane and that intracellular components are not required. Although crosslinking of the receptor activates phospholipase C and phospholipase A2 leading to the generation of several second messengers, none of these signaling mechanisms appears to be involved in IgE receptor interaction with the membrane skeleton. This interaction cannot be induced by phorbol 12-myristate 13-acetate (PMA), ionomycin, or a combination of these two reagents, although this will result in degranulation. Furthermore, receptor detergent insolubility is temperature independent when triggered by multivalent antigen, thus indicating that enzyme-catalyzed reactions are not important. This was verified by the fact that a variety of inhibitors that block phosphatidylinositol metabolism, arachidonic acid metabolism, Ca2+ influx, and protein kinase C (PKC) activation had no effect on antigen-induced association of the receptor with the membrane skeleton. These results indicate that the signaling mechanisms leading to the degranulation response are not involved in the association of the crosslinked receptor with the membrane skeleton.

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