George S J, Lloyd C T, Angelini G D, Newby A C, Baker A H
Bristol Heart Institute, University of Bristol, Bristol, UK.
Circulation. 2000 Jan 25;101(3):296-304. doi: 10.1161/01.cir.101.3.296.
Autologous saphenous vein coronary artery bypass graft surgery is complicated by late graft failure due to neointima formation and subsequent atherosclerosis. Growth factors and metalloproteinases (MMPs) act in concert to promote neointima formation. Tissue inhibitor of metalloproteinase-3 (TIMP-3), an extracellular matrix-associated MMP inhibitor, uniquely promotes apoptosis of isolated vascular smooth muscle cells. Here, we overexpressed TIMP-3 at the luminal surface of human saphenous veins before organ culture and in pig saphenous veins before interposition grafting into carotid arteries in vivo to assess neointima formation.
In both models, high TIMP-3 immunoreactivity occurred in the luminal and upper medial extracellular matrix after adenovirus delivery. MMP activity measured by in situ zymography was reduced throughout the veins, confirming a bystander effect. By use of 3 independent techniques, apoptosis levels in the neointima and medial layer were significantly elevated by TIMP-3 overexpression. Neointima formation was reduced by 84% in 14-day human organ cultures and by 58% in 28-day pig vein grafts (both P<0.05). In contrast, TIMP-2 overexpression had no effect on neointima formation in vivo.
Our results highlight the potential therapeutic benefit for TIMP-3 overexpression to reduce neointima formation associated with late vein graft failure.
自体大隐静脉冠状动脉旁路移植手术会因新生内膜形成及随后的动脉粥样硬化而出现晚期移植物功能衰竭。生长因子和金属蛋白酶(MMPs)协同作用以促进新生内膜形成。金属蛋白酶组织抑制剂-3(TIMP-3)是一种与细胞外基质相关的MMP抑制剂,能独特地促进分离的血管平滑肌细胞凋亡。在此,我们在器官培养前使人隐静脉的管腔表面过表达TIMP-3,并在将猪隐静脉体内移植到颈动脉前过表达TIMP-3,以评估新生内膜的形成。
在两种模型中,腺病毒递送后,管腔和内侧上部细胞外基质中均出现高TIMP-3免疫反应性。通过原位酶谱法测定的MMP活性在整个静脉中均降低,证实了旁观者效应。通过使用3种独立技术,TIMP-3过表达使新生内膜和中层的凋亡水平显著升高。在14天的人体器官培养中,新生内膜形成减少了84%,在28天的猪静脉移植物中减少了58%(两者P<0.05)。相比之下,TIMP-2过表达对体内新生内膜形成没有影响。
我们的结果突出了TIMP-3过表达在减少与晚期静脉移植物功能衰竭相关的新生内膜形成方面的潜在治疗益处。
