Leoligin, the major lignan from Edelweiss, inhibits intimal hyperplasia of venous bypass grafts

Leoligin 是雪绒花的主要木脂素,可抑制静脉旁路移植物内膜增生

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作者:Ute Reisinger, Stefan Schwaiger, Iris Zeller, Barbara Messner, Robert Stigler, Dominik Wiedemann, Tobias Mayr, Christoph Seger, Thomas Schachner, Verena M Dirsch, Angelika M Vollmar, Johannes O Bonatti, Hermann Stuppner, Günther Laufer, David Bernhard

Aims

Despite the lower patency of venous compared with arterial coronary artery bypass grafts, approximately 50% of grafts used are saphenous vein conduits because of their easier accessibility. In a search for ways to increase venous graft patency, we applied the

Conclusion

Our data suggest that leoligin might represent a novel non-toxic, non-thrombogenic, endothelial integrity preserving candidate drug for the treatment of vein graft disease.

Results

We found that leoligin potently inhibits vascular smooth muscle cell (SMC) proliferation by inducing cell cycle arrest in the G1-phase. Leoligin induced cell death neither in SMCs nor, more importantly, in endothelial cells. In a human saphenous vein organ culture model for graft disease, leoligin potently inhibited intimal hyperplasia, and even reversed graft disease in pre-damaged vessels. Furthermore, in an in vivo mouse model for venous bypass graft disease, leoligin potently inhibited intimal hyperplasia.

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