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从结构明确的配体深入了解免疫球蛋白E受体信号传导。

Insights into immunoglobulin E receptor signaling from structurally defined ligands.

作者信息

Holowka David, Sil Dwaipayan, Torigoe Chikako, Baird Barbara

机构信息

Department of Chemistry and Chemical Biology, Cornell University, Ithaca, NY 14853-1301, USA.

出版信息

Immunol Rev. 2007 Jun;217:269-79. doi: 10.1111/j.1600-065X.2007.00517.x.

DOI:10.1111/j.1600-065X.2007.00517.x
PMID:17498065
Abstract

The asymmetrical structure of bent immunoglobulin E (IgE) bound to its high-affinity receptor, Fc epsilon RI, suggests a possible role for this configuration in the regulation of signaling mediated by cross-linking of Fc epsilon RI on the surface of mast cells and basophils. Indeed, the presence of bound IgE strongly influences the capacity of cross-linked Fc epsilon RI dimers to trigger mast cell degranulation, implicating orientational constraints by bound IgE. Bivalent ligands that cross-link by binding to bivalent IgE can form linear and cyclic chains of IgE/Fc epsilon RI complexes, and these exhibit only limited capacity to stimulate downstream signaling and degranulation, whereas structurally analogous trivalent ligands, which can form branched networks of cross-linked IgE/Fc epsilon RI complexes, are more effective at cell activation. Long bivalent ligands with flexible spacers can form intramolecular cross-links with IgE, and these stable 1:1 complexes are very potent inhibitors of mast cell degranulation stimulated by multivalent antigen. In contrast, trivalent ligands with rigid double-stranded DNA spacers effectively stimulate degranulation responses in a length-dependent manner, providing direct evidence for receptor transphosphorylation as a key step in the mechanism of signaling by Fc epsilon RI. Thus, studies with chemically defined oligovalent ligands show important features of IgE receptor cross-linking that regulate signaling, leading to mast cell activation.

摘要

弯曲的免疫球蛋白E(IgE)与其高亲和力受体FcεRI结合的不对称结构表明,这种构象可能在调节肥大细胞和嗜碱性粒细胞表面FcεRI交联介导的信号传导中发挥作用。实际上,结合的IgE的存在强烈影响交联的FcεRI二聚体触发肥大细胞脱颗粒的能力,这暗示了结合的IgE产生的取向限制。通过与二价IgE结合而交联的二价配体可以形成IgE/FcεRI复合物的线性和环状链,并且这些复合物在刺激下游信号传导和脱颗粒方面仅表现出有限的能力,而结构类似的三价配体可以形成交联的IgE/FcεRI复合物的分支网络,在细胞活化方面更有效。具有柔性间隔区的长二价配体可以与IgE形成分子内交联,并且这些稳定的1:1复合物是多价抗原刺激的肥大细胞脱颗粒的非常有效的抑制剂。相比之下,具有刚性双链DNA间隔区的三价配体以长度依赖性方式有效刺激脱颗粒反应,为受体转磷酸化作为FcεRI信号传导机制中的关键步骤提供了直接证据。因此,使用化学定义的多价配体进行的研究显示了IgE受体交联调节信号传导从而导致肥大细胞活化的重要特征。

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