Department of Pharmacology, University of Pennsylvania School of Medicine, Philadelphia, PA 19104-6084, United States.
Prostaglandins Other Lipid Mediat. 2010 Sep;93(1-2):20-4. doi: 10.1016/j.prostaglandins.2010.04.004. Epub 2010 May 10.
Stents eluting anti-proliferative drugs limit restenosis, but drugs commonly used to date are relatively non-specific cytostatic agents which inhibit proliferation of intimal endothelial cells as well as medial smooth muscle cells and may thereby contribute to the clinical complications associated with angioplasty. In an effort to identify a more specific anti-proliferative agent, we compared the effects of rapamycin to those of cicaprost, a mimetic of the naturally occurring anti-mitogen, PGI(2). Rapamycin and cicaprost were both strongly anti-mitogenic in vascular smooth muscle cells (VSMCs). But unlike rapamycin, cicaprost did not inhibit mitogenesis in aortic endothelial cells even when used at concentrations >10-fold higher than its ED(50) for VSMCs. Similarly, both rapamycin and cicaprost have been reported to regulate levels of the cdk inhibitor, p27(kip1). But rapamycin remained anti-mitogenic in p27(kip1)-null VSMCs whereas the anti-mitogenic effect of cicaprost was completely dependent on p27(kip1). We conclude that stable PGI(2) mimetics may be highly specific inhibitors of p27(kip1)-dependent VSMC proliferation after vascular injury.
支架释放抗增殖药物可限制再狭窄,但迄今为止常用的药物通常是非特异性细胞抑制剂,可抑制内膜内皮细胞以及中膜平滑肌细胞的增殖,这可能导致与血管成形术相关的临床并发症。为了寻找更特异的抗增殖药物,我们比较了雷帕霉素与 cicaprost 的作用,cicaprost 是天然抗有丝分裂原 PGI(2)的类似物。雷帕霉素和 cicaprost 均对血管平滑肌细胞(VSMCs)有强烈的抗有丝分裂作用。但与雷帕霉素不同,cicaprost 即使在高于其对 VSMCs 的 ED(50)浓度 10 倍以上的浓度下,也不会抑制主动脉内皮细胞的有丝分裂。同样,雷帕霉素和 cicaprost 都被报道可调节细胞周期蛋白依赖性激酶抑制剂 p27(kip1)的水平。但雷帕霉素在 p27(kip1)缺失的 VSMCs 中仍具有抗有丝分裂作用,而 cicaprost 的抗有丝分裂作用则完全依赖于 p27(kip1)。我们的结论是,稳定的 PGI(2)类似物可能是血管损伤后 p27(kip1)依赖性 VSMC 增殖的高度特异抑制剂。
