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IgE regulation of mast cell survival and function

机译:肥大细胞生存和功能的IgE调节

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Traditionally, it is thought that IgE binding to mast cells via the high-affinity receptor (FcepsilonRI) is simply a passive 'sensitization' step prior to activation by receptor aggregation or cross-linking with multivalent antigen or other cross-linking agents. However, in addition to receptor up-regulation, recent studies have shown that monomeric IgE can induce survival and other activation events including increased histamine content, degranulation, leukotriene release, receptor internalization, adhesion, migration and DNA synthesis. Various IgE molecules exhibit a vast spectrum of heterogeneity: the highly cytokinergic (HC) group of IgEs at an extreme end of the spectrum can induce survival and other activation events very efficiently, whereas poorly cytokinergic (PC) IgEs at the other end can do so less efficiendy. All the IgEs tested appear to be capable of inducing receptor aggregation with HC IgEs having a higher capacity to do so than PC IgEs. HC IgEs can promote the production and secretion of various cytokines including the one(s) that can sustain survival in an autocrine and paracrine mechanism. Consistent with receptor aggregation induced by monomeric IgE, other means of receptor aggregation, e.g. IgE+antigen and IgE+anti-IgE, can also induce survival and other events in unique ranges of stimulation intensity.
机译:传统上,认为据思想通过高亲和力受体(Fcepsilonri)与肥大细胞的IgE结合是在通过受体聚集或与多价抗原或其他交联剂的交联之前的被动性的“敏化”步骤。然而,除了受体上调之外,最近的研究表明,单体IgE可以诱导存活和其他活化事件,包括增加的组胺含量,脱粒,白酮释放,受体内化,粘附,迁移和DNA合成。各种IgE分子表现出广泛的异质性:高度细胞石能(HC)IGES在光谱极端的IGES非常有效地诱发生存和其他激活事件,而另一端的细胞内能(PC)差异差异差效率较少。测试的所有IGE似乎能够用比PC IGES具有更高容量的HC IGE诱导受体聚集。 HC IGES可以促进各种细胞因子的生产和分泌,包括可以在自分泌和旁静脉机制中维持生存的一个细胞因子。与单体IgE诱导的受体聚集一致,其他受体聚集方法,例如, IgE +抗原和IgE +抗IgE,也可以在独特的刺激强度范围内诱发生存和其他事件。

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