Nuwayhid Samer J, Werling Linda L
Department of Pharmacology, The George Washington University Medical Center, Washington, DC 20037, USA.
J Pharmacol Exp Ther. 2003 Jan;304(1):364-9. doi: 10.1124/jpet.102.043398.
We have previously shown that sigma1 receptor agonists inhibit N-methyl-D-aspartate (NMDA)-stimulated [3H]dopamine from slices of rat striatum in a concentration-related manner and that the inhibition is reversed by sigma1 receptor-selective and nonsubtype-selective sigma receptor antagonists. Based on previous evidence from our laboratory as well as other laboratories, we hypothesized that sigma1 receptors might use a protein kinase C (PKC) signaling pathway to modulate stimulated dopamine release. We tested several inhibitors of PKC isozymes, as well as a phospholipase C inhibitor for their effects on sigma1 receptor agonist-mediated regulation of [3H]dopamine release. Although none of the inhibitors tested affected the ability of NMDA to stimulate [3H]dopamine release, they all abolished regulation by the sigma1 receptor agonist (+)-pentazocine in a concentration-related manner. We also found that prior exposure to 1 microM phorbol 2-myristate 13-acetate for 30 min abolished regulation by (+)-pentazocine. We concluded that an intact PKC system was required for sigma1 agonist-mediated regulation of NMDA-stimulated [3H]dopamine release from rat striatal slices. Based on the pharmacological profile of the PKC inhibitors tested, as well as reports in the literature on PKC
我们之前已经表明,σ1受体激动剂以浓度相关的方式抑制大鼠纹状体切片中N-甲基-D-天冬氨酸(NMDA)刺激的[3H]多巴胺释放,并且该抑制作用可被σ1受体选择性和非亚型选择性的σ受体拮抗剂逆转。基于我们实验室以及其他实验室之前的证据,我们推测σ1受体可能利用蛋白激酶C(PKC)信号通路来调节刺激后的多巴胺释放。我们测试了几种PKC同工酶抑制剂以及一种磷脂酶C抑制剂对σ1受体激动剂介导的[3H]多巴胺释放调节的影响。尽管所测试的抑制剂均未影响NMDA刺激[3H]多巴胺释放的能力,但它们均以浓度相关的方式消除了σ1受体激动剂(+)-喷他佐辛的调节作用。我们还发现,预先暴露于1μM佛波醇2-肉豆蔻酸酯13-乙酸酯30分钟可消除(+)-喷他佐辛的调节作用。我们得出结论,完整的PKC系统是σ1激动剂介导的大鼠纹状体切片中NMDA刺激的[3H]多巴胺释放调节所必需的。基于所测试的PKC抑制剂的药理学特征以及文献中关于PKC的报道
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