Isoprenoid pathway activity is required for IgE receptor-mediated, tyrosine kinase-coupled transmembrane signaling in permeabilized RBL-2H3 rat basophilic leukemia cells.

G G Deanin, J R Pfeiffer, J L Cutts, M L Fore, J M Oliver
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引用次数: 17

Abstract

Previously, we reported that the isoprenoid pathway inhibitor, lovastatin, blocks the activation by IgE receptor cross-linking of 45Ca2+ influx, 1,4,5-inositol trisphosphate production, secretion, and membrane changes (ruffling, spreading) in intact RBL-2H3 rat basophilic leukemia cells. These results indicated that an isoprenoid pathway intermediate, very likely an isoprenylated protein, is importantly involved in the control of IgE receptor-mediated signal transduction. Here, we show that 20 h of pretreatment with lovastatin also inhibits antigen-induced secretion and membrane responses in streptolysin O-(SLO)-permeabilized cells. However, lovastatin does not inhibit secretion stimulated by the nonhydrolyzable GTP analog, GTP gamma S. Furthermore, the membrane responses to GTP gamma S persist, although in an attenuated form, in lovastatin-treated permeabilized cells. The relative insensitivity of GTP gamma S-induced responses to lovastatin was one of several indications that antigen and GTP gamma S may activate separate pathways leading to transmembrane responses in permeabilized cells. Further experiments showed that the beta-thio derivative of GDP, GDPBAS, inhibits the secretory and membrane responses to GTP gamma S, as expected for a GTP-binding protein-dependent signaling pathway, while having little effect on antigen-induced responses. Conversely, genistein blocks the secretory and membrane responses to antigen, as expected for a tyrosine kinase-dependent pathway, without altering the GTP gamma S-induced responses. From these results, and from additional data from cells treated with tyrphostins and sodium orthovanadate, we propose that IgE receptor-mediated secretion from permeabilized RBL-2H3 cells occurs by a tyrosine kinase-dependent pathway that requires isoprenoid pathway activity for function. We propose further that RBL-2H3 cells contain a separate GTP-binding protein-mediated signaling pathway whose direct activation by GTP gamma S is either independent of isoprenoid pathway activity or depends on the activity of an isoprenylated protein that is not significantly depleted after 20 h of lovastatin treatment.

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在通透性RBL-2H3大鼠嗜碱性白血病细胞中,IgE受体介导的酪氨酸激酶偶联的跨膜信号通路需要类异戊二烯途径活性。
先前,我们报道了类异戊二烯途径抑制剂洛伐他汀阻断了完整RBL-2H3大鼠嗜碱性白血病细胞中45Ca2+内流、1,4,5-肌醇三磷酸的产生、分泌和膜变化(皱缩、扩散)的IgE受体交联激活。这些结果表明,类异戊二烯途径中间体,很可能是一种异戊二烯化蛋白,在控制IgE受体介导的信号转导中起重要作用。在这里,我们发现洛伐他汀预处理20小时也抑制了抗原诱导的链溶素O-(SLO)渗透细胞的分泌和膜反应。然而,洛伐他汀不会抑制非水解GTP类似物GTP γ S刺激的分泌。此外,在洛伐他汀处理的通透性细胞中,膜对GTP γ S的反应持续存在,尽管以减弱的形式存在。GTP γ S诱导的对洛伐他汀反应的相对不敏感是抗原和GTP γ S可能激活导致通透性细胞跨膜反应的不同途径的几个迹象之一。进一步的实验表明,GDP的β -硫代衍生物GDPBAS抑制GTP γ S的分泌和膜反应,正如预期的GTP结合蛋白依赖的信号通路,而对抗原诱导的反应几乎没有影响。相反,染料木素阻断了对抗原的分泌和膜反应,正如酪氨酸激酶依赖途径所期望的那样,而不会改变GTP γ s诱导的反应。根据这些结果,以及通过暴发磷素和正钒酸钠处理的细胞的其他数据,我们提出IgE受体介导的RBL-2H3细胞的分泌通过酪氨酸激酶依赖途径发生,该途径需要类异戊二烯途径的活性才能发挥作用。我们进一步提出,rbr - 2h3细胞含有单独的GTP结合蛋白介导的信号通路,其GTP γ S的直接激活要么独立于类异戊二烯途径活性,要么依赖于异戊二烯化蛋白的活性,该蛋白在洛伐他汀治疗20小时后未显着耗尽。
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