摘要
目的探讨精氨酸血管加压素(AVP)对缺氧血管平滑肌细胞(VSMC)中PKC—α、δ和ε亚型蛋白表达的调节作用及其可能机制。方法取50只Wistar大鼠的血管进行原代VSMC培养,观察AVP对缺氧VSMC胞质和胞膜成分中PKC-α、δ和ε亚型蛋白表达的影响,同时检测缺氧VSMC中3种磷脂酶(PLC、PLD、PLA,)的活性变化及AVP和PKC亚型抑制剂对其的作用。结果缺氧后VSMC胞膜成分中PKC—α和ε亚型的表达分别升高为正常组的1.5和2.0倍,而胞质成分中表达降低,AVP处理进一步升高胞膜PKC—α和ε亚型的表达(分别为正常组的2.4和2.6倍,P〈0.05);而胞质和胞膜PKC-δ亚型有相似的变化趋势,但差异无统计学意义。同时,缺氧后PLC和PLD活性升高,AVP处理使PLC和PLD的活性进一步升高为正常组的1.6和2.1倍;PKC—α抑制剂G66976预处理可拮抗AVP诱导PLD活性升高的作用(PLD活性降低为AVP组的40.8%),而PKC-δ和ε抑制剂无明显作用;各组PLA2活性差异无统计学意义。结论AVP可通过促进VSMC胞质中的PKC-α和ε亚型向胞膜转位而激活,进而调节休克后血管反应性;PLC和PLD可能参与了AVP介导的PKC激活过程。
Objective To observe the effect of arginine vasopressin (AVP) on the expression of PKC-α, δ and ε isoforms of vascular smooth muscle cell ( VSMC ) after hypoxia and its mechanisms. Methods With cultured VSMC from 50 Wistar rats,the effect of AVP on the expression of PKC-α,δ and ε isoforms in the cytosol and particulate fractions of VSMC after hypoxia were observed. At the same time, the activity of phospholipase C ( PLC ), phospholipase D ( PLD ), phospholipase A2 ( PLA2 ) and the effects of AVP and PKC isoform inhibitors were also observed. Results The expression of particulate PKC-α and increased about 1.5 and 2.0 folds, respectively after 90-min hypoxia, with a concomitant decrease in cytosolic fractions. AVP treatment further increased expression of PKC-α and e in the particulate fractions to 2.4 and 2.6 folds ( P 〈 0.05 ). While PKC-δ showed a similar changes in the particulate and cytosolic fractions during the process, but there were no statistical differences among the groups. At the same time, treatment with hypoxia for 1.5 h caused a significant increase in PLC and PLD activity, AVP further increased of PLC and PLD activity to 1.6 and 2.1 folds, PKC-α inhibitor Go 6976 antagonized AVP-induced increased in PLD activity,which reduced to 40.8% as compared to AVP alone group. The PLA2 activity had no significant changes among the groups. Conclusion AVP improved vascular reactivity following shock through translocating PKC-α and e isoforms from a cytosol to a particulate and activation. And PLC and PLD may participate in the signal transduction pathway induced by AVP.
出处
《中华实验外科杂志》
CAS
CSCD
北大核心
2009年第5期570-572,共3页
Chinese Journal of Experimental Surgery
基金
国家杰出青年科学基金资助项目(30625037)
国家重点基础发展计划资助项目(973)(2005CB522601)
教育部创新团队资助计划资助项目(IRT0712)
