Whatley R E, Fennell D F, Kurrus J A, Zimmerman G A, McIntyre T M, Prescott S M
Department of Medicine, University of Utah School of Medicine, Salt Lake City 84112.
J Biol Chem. 1990 Sep 15;265(26):15550-9.
Production of the potent lipid autacoid, platelet-activating factor (PAF), is a stimulated response of the endothelium which has important physiologic consequences including mediating adherence of inflammatory cells to the endothelium. Consequently, an understanding of the mechanisms that regulate PAF synthesis by the endothelium is important. To this end, we investigated the role of G proteins as a component of the signal transduction pathway that couples hormonal stimuli to PAF production. The addition of aluminum fluoride (AlF-4) to endothelial cells resulted in production of PAF with a maximal effect at 20 mM fluoride and within 20-60 min of exposure. Alf-4 also augmented the production of PAF which occurs in response to hormonal agonists. In addition, submaximal concentrations of AlF-4 converted an ineffective hormonal agonist (thrombin in bovine cells) to a maximally effective agonist. The adherence of neutrophils to endothelial cells that had been exposed previously to AlF-4 was increased in a manner that paralleled PAF production. PAF production in response to AlF-4 was not consistently affected by pertussis or cholera toxin. Introduction of guanosine 5'-O-(3-thiotriphosphate) (GTP gamma S) into permeabilized endothelial cells also resulted in PAF production, with reversal by guanosine 5'-O-(2-thiodiphosphate) (GDP beta S), consistent with an effect mediated by a G protein. G protein activation with AlF-4 or GTP gamma S resulted in entry of extracellular Ca2+ as determined using 45Ca2+ flux studies and Indo-1 spectrofluorometry. Our data are consistent with the hypothesis that G proteins couple hormone-receptor binding to opening of a membrane calcium channel, a key step in the initiation of PAF production in endothelial cells.
强效脂质自分泌运动因子血小板活化因子(PAF)的产生是内皮细胞的一种刺激反应,它具有重要的生理后果,包括介导炎症细胞与内皮细胞的黏附。因此,了解调节内皮细胞PAF合成的机制很重要。为此,我们研究了G蛋白作为将激素刺激与PAF产生相偶联的信号转导途径的一个组成部分所起的作用。向内皮细胞中添加氟化铝(AlF₄)会导致PAF的产生,在20 mM氟化物时效果最佳,且在暴露后20 - 60分钟内出现。AlF₄还增强了对激素激动剂产生反应时PAF的产生。此外,亚最大浓度的AlF₄将无效的激素激动剂(牛细胞中的凝血酶)转化为最大有效的激动剂。先前暴露于AlF₄的内皮细胞对中性粒细胞的黏附以与PAF产生平行的方式增加。百日咳毒素或霍乱毒素对AlF₄诱导的PAF产生没有持续影响。将鸟苷5'-O-(3-硫代三磷酸)(GTPγS)引入通透的内皮细胞也会导致PAF的产生,而鸟苷5'-O-(2-硫代二磷酸)(GDPβS)可使其逆转,这与G蛋白介导的效应一致。使用⁴⁵Ca²⁺通量研究和Indo-1荧光分光光度法测定,用AlF₄或GTPγS激活G蛋白会导致细胞外Ca²⁺内流。我们的数据与以下假设一致,即G蛋白将激素 - 受体结合与膜钙通道的开放相偶联,这是内皮细胞中PAF产生起始的关键步骤。
