地塞米松对人培养气道平滑肌中组胺H1受体偶联的调节作用
Regulation of histamine H1 receptor coupling by dexamethasone in human cultured airway smooth muscle.
作者信息
Hardy E, Farahani M, Hall I P
机构信息
Department of Therapeutics, University Hospital of Nottingham.
出版信息
Br J Pharmacol. 1996 Jun;118(4):1079-84. doi: 10.1111/j.1476-5381.1996.tb15509.x.
Abstract
- The regulation of histamine-induced [3H]-inositol phosphate and intracellular calcium responses in human cultured airway smooth muscle cells was studied. 2. Histamine induced concentration-dependent [3H]-inositol phosphate formation (EC50 4 microM). This response was inhibited by a range of selective H1 receptor antagonists but not by the H2-selective antagonist, tiotidone or the H3 receptor-selective antagonist, thioperamide, indicating that an H1 receptor is involved in this response in human cultured airway smooth muscle cells. 3. Preincubation of human cultured airway smooth muscle cells with concentrations of dexamethasone > 10 nM for 22 h produced concentration-dependent inhibition of histamine-induced inositol phosphate formation. The maximum inhibition observed was 45% of the response in control cells. The inhibitory effect of dexamethasone was itself reversed by prior exposure to the glucocorticoid receptor antagonist, RU38486 (10 microM). Preincubation for 22 h with 1 microM dexamethasone produced inhibition of the inositol phosphate response to histamine to all concentrations of histamine inducing significant inositol phosphate formation in these cells. In contrast, the response to the G protein activator, NaF (0.1-20 mM) was unaltered by preincubation with dexamethasone. 4. Preincubation of human airway smooth muscle cells with 1 microM dexamethasone for time periods of < 6 h failed to inhibit histamine-induced inositol phosphate formation in human airway smooth muscle cells. 5. Histamine also induced concentration-dependent elevation of intracellular calcium levels in Fura 2-loaded human airway smooth muscle cells. This response was inhibited by preincubation with 1 microM dexamethasone. 6. We conclude that signal transduction through the H1 receptor in human airway smooth muscle is subject to regulation by dexamethasone and that this may in part account for the protective effect of dexamethasone against spasmogen-induced contractile responses in the airways.
摘要
- 研究了组胺诱导人培养气道平滑肌细胞中[3H]-肌醇磷酸和细胞内钙反应的调节机制。2. 组胺诱导浓度依赖性的[3H]-肌醇磷酸形成(EC50为4 microM)。该反应受到一系列选择性H1受体拮抗剂的抑制,但不受H2选择性拮抗剂替奥地定或H3受体选择性拮抗剂硫代哌酰胺的抑制,表明H1受体参与了人培养气道平滑肌细胞的这一反应。3. 将人培养气道平滑肌细胞与浓度>10 nM的地塞米松预孵育22小时,可产生浓度依赖性抑制组胺诱导的肌醇磷酸形成。观察到的最大抑制率为对照细胞反应的45%。地塞米松的抑制作用可被预先暴露于糖皮质激素受体拮抗剂RU38486(10 microM)所逆转。用1 microM地塞米松预孵育22小时可抑制这些细胞中对所有诱导显著肌醇磷酸形成的组胺浓度的肌醇磷酸反应。相比之下,与地塞米松预孵育不会改变对G蛋白激活剂氟化钠(0.1 - 20 mM)的反应。4. 将人气道平滑肌细胞与1 microM地塞米松预孵育<6小时未能抑制人气道平滑肌细胞中组胺诱导的肌醇磷酸形成。5. 组胺还诱导Fura 2负载的人气道平滑肌细胞中细胞内钙水平的浓度依赖性升高。该反应可被1 microM地塞米松预孵育所抑制。6. 我们得出结论,人气道平滑肌中通过H1受体的信号转导受地塞米松调节,这可能部分解释了地塞米松对气道中致痉剂诱导的收缩反应的保护作用。
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