【摘要】 实验旨在研究糖皮质激素快速、非基因组作用的细胞内信号传导机制。Western分析研究结果表明 ,皮质酮可快速激活PC12细胞中p38丝列原激活的蛋白激酶 (mitogen activatedproteinkinase ,MAPK) ,时间、浓度曲线均为钟形 ,最大激活为 10 -9mol/L和 15min。糖皮质激素受体阻断剂RU38486不能阻断此作用 ,而小牛血清白蛋白耦联的皮质酮也能快速激活p38。受体酪氨酸激酶阻断剂genistein对此作用无影响 ,表明此快速作用不涉及受体酪氨酸激酶活性。此作用能被蛋白激酶C (proteinkinaseC ,PKC)激动剂PMA模拟 ,而被PKC阻断剂G 6 976所阻断。结果表明 ,皮质酮可能通过推测的膜受体以PKC依赖的方式快速激活p38MAPK。更多还原

【Abstract】 The present study using immunoblot showed that corticosterone (B) could induce a rapid activation of p38 in PC12 cells. The dose- and time-response curves were bell-shaped with a maximal activation at 10 -9 mol/L and 15 min respectively. The activation was not affected by steroid nuclear receptor antagonist RU38486. Bovine serum albumin coupled B (B-BSA) could induce phosphorylation of p38. Tyrosine kinase inhibitor genistein failed to block the phosphorylation, a fact suggesting that the tyrosine kinase activity is not involved in the pathway. On the other hand, phorbol 12-myristate 13-acetate (PMA), a protein kinase C (PKC) activator, could mimic the actions of B, while G*i6976, a PKC inhibitor, could completely abolish the phosphorylation induced by B. These results clearly demonstrate that B activates p38 MAPK readily via a putative membrane receptor through a PKC-dependent pathway.更多还原