抑制再狭窄形成而不影响再内皮化作为血管成形术后血栓形成的潜在解决方案?

Alexandra Theresia Fuchs, Andreas Kuehnl, Jaroslav Pelisek, Pierre Henri Rolland, Choukri Mekkaoui, Heinrich Netz, Sigrid Nikol
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引用次数: 14

摘要

不同类型的支架植入后,支架内血栓形成仍然是一个重要的问题。一个潜在的解决方案可能是对不同细胞类型具有双重作用的血管活性药物,如c型利钠肽(CNP)。因此,我们在猪再狭窄模型中研究了CNP的体内外作用。CNP基因在猪血管细胞培养中的转移表明,平滑肌细胞的生长减少了30% (p
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Inhibition of restenosis formation without compromising reendothelialization as a potential solution to thrombosis following angioplasty?

Stent thrombosis remains an important problem after the implantation of different stent types. A potential solution to this problem may be vasoactive agents with dual effects on different cell types like C-type natriuretic peptide (CNP). Therefore, in vitro and in vivo effects of CNP were investigated in a porcine restenotic model. Gene transfer of CNP in cultures of porcine vascular cells revealed up to 30% reduction of growth of smooth muscle cells (p<.05), but no suppression of endothelial growth using CNP. Applied in vivo, angiography revealed a trend of reduced restenosis formation in balloon-injured porcine arteries treated with CNP gene or beta-galactosidase (beta-Gal) control gene after three months (2.59 +/- 2.04-fold reduction, p = n.s.). Histologically, morphometry revealed significantly reduced neointima formation after treatment with CNP plasmid (7.26 +/- 1.44-fold reduction, p < .05). Evans blue staining demonstrated complete endothelial repair already 3 weeks after intervention using CNP. Transfer of CNP gene resulted in a significant inhibition of neointima formation without compromising endothelial repair. Therefore, use of the CNP gene may offer a solution to suppress restenosis formation while preventing subacute or late thrombosis.

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