Gonzalez-Iglesias Arturo E, Murano Takayo, Li Shuo, Tomić Melanija, Stojilkovic Stanko S
National Institute of Child Health and Human Development, 49 Convent Drive, Bethesda, MD 20892-4510, USA.
Endocrinology. 2008 Apr;149(4):1470-9. doi: 10.1210/en.2007-0980. Epub 2007 Dec 20.
Dopamine D2 receptors signal through the pertussis toxin (PTX)-sensitive G(i/o) and PTX-insensitive G(z) proteins, as well as through a G protein-independent, beta-arrestin/glycogen synthase kinase-3-dependent pathway. Activation of these receptors in pituitary lactotrophs leads to inhibition of prolactin (PRL) release. It has been suggested that this inhibition occurs through the G(i/o)-alpha protein-mediated inhibition of cAMP production and/or G(i/o)-betagamma dimer-mediated activation of inward rectifier K(+) channels and inhibition of voltage-gated Ca(2+) channels. Here we show that the dopamine agonist-induced inhibition of spontaneous Ca(2+) influx and release of prestored PRL was preserved when cAMP levels were elevated by forskolin treatment. We further observed that dopamine agonists inhibited both spontaneous and depolarization-induced Ca(2+) influx in untreated but not in PTX-treated cells. This inhibition was also observed in cells with blocked inward rectifier K(+) channels, suggesting that the dopamine effect on voltage-gated Ca(2+) channel gating is sufficient to inhibit spontaneous Ca(2+) influx. However, agonist-induced inhibition of PRL release was only partially relieved in PTX-treated cells, indicating that dopamine receptors also inhibit exocytosis downstream of voltage-gated Ca(2+) influx. The PTX-insensitive step in agonist-induced inhibition of PRL release was not affected by the addition of wortmannin, an inhibitor of phosphatidylinositol 3-kinase, and lithium, an inhibitor of glycogen synthase kinase-3, but was attenuated in the presence of phorbol 12-myristate 13-acetate, which inhibits G(z) signaling pathway in a protein kinase C-dependent manner. Thus, dopamine inhibits basal PRL release by blocking voltage-gated Ca(2+) influx through the PTX-sensitive signaling pathway and by desensitizing Ca(2+) secretion coupling through the PTX-insensitive and protein kinase C-sensitive signaling pathway.
多巴胺D2受体通过百日咳毒素(PTX)敏感的G(i/o)和PTX不敏感的G(z)蛋白进行信号传导,同时也通过一条不依赖G蛋白、β-抑制蛋白/糖原合酶激酶-3依赖的途径进行信号传导。这些受体在垂体催乳素细胞中的激活会导致催乳素(PRL)释放受到抑制。有人提出,这种抑制是通过G(i/o)-α蛋白介导的cAMP生成抑制和/或G(i/o)-βγ二聚体介导的内向整流钾通道激活以及电压门控钙通道抑制来实现的。在此我们表明,当通过福斯高林处理使cAMP水平升高时,多巴胺激动剂诱导的自发钙内流抑制和预存PRL释放得以保留。我们进一步观察到,多巴胺激动剂在未处理的细胞中抑制了自发的和去极化诱导的钙内流,但在PTX处理的细胞中未观察到这种抑制。在内向整流钾通道被阻断的细胞中也观察到了这种抑制,这表明多巴胺对电压门控钙通道门控的作用足以抑制自发钙内流。然而,激动剂诱导的PRL释放抑制在PTX处理的细胞中仅部分得到缓解,这表明多巴胺受体也在电压门控钙内流下游抑制胞吐作用。激动剂诱导的PRL释放抑制中PTX不敏感的步骤不受磷脂酰肌醇3激酶抑制剂渥曼青霉素和糖原合酶激酶-3抑制剂锂的添加影响,但在佛波醇12-肉豆蔻酸酯13-乙酸酯存在下会减弱,后者以蛋白激酶C依赖的方式抑制G(z)信号通路。因此,多巴胺通过PTX敏感的信号通路阻断电压门控钙内流,并通过PTX不敏感且蛋白激酶C敏感的信号通路使钙分泌偶联脱敏,从而抑制基础PRL释放。