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基质金属蛋白酶抑制治疗血管疾病。

Matrix metalloproteinase inhibition therapy for vascular diseases.

机构信息

Bristol Heart Institute, University of Bristol, UK.

出版信息

Vascul Pharmacol. 2012 May-Jun;56(5-6):232-44. doi: 10.1016/j.vph.2012.01.007. Epub 2012 Feb 1.

DOI:10.1016/j.vph.2012.01.007
PMID:22326338
Abstract

The matrix metalloproteinases (MMPs) are 23 secreted or cell surface proteases that act together and with other protease classes to turn over the extracellular matrix, cleave cell surface proteins and alter the function of many secreted bioactive molecules. In the vasculature MMPs influence the migration proliferation and apoptosis of vascular smooth muscle, endothelial cells and inflammatory cells, thereby affecting intima formation, atherosclerosis and aneurysms, as substantiated in clinical and mouse knockout and transgenic studies. Prominent counterbalancing roles for MMPs in tissue destruction and repair emerge from these experiments. Naturally occurring tissue inhibitors of MMPs (TIMPs), pleiotropic mediators such as tetracyclines, chemically-synthesised small molecular weight MMP inhibitors (MMPis) and inhibitory antibodies have all shown effects in animal models of vascular disease but only doxycycline has been evaluated extensively in patients. A limitation of broad specificity MMPis is that they prevent both matrix degradation and tissue repair functions of different MMPs. Hence MMPis with more restricted specificity have been developed and recent studies in models of atherosclerosis accurately replicate the phenotypes of the corresponding gene knockouts. This review documents the established actions of MMPs and their inhibitors in vascular pathologies and considers the prospects for translating these findings into new treatments.

摘要

基质金属蛋白酶(MMPs)是 23 种分泌或细胞表面蛋白酶,它们协同作用并与其他蛋白酶家族一起,使细胞外基质降解,切割细胞表面蛋白,并改变许多分泌的生物活性分子的功能。在血管系统中,MMPs 影响血管平滑肌、内皮细胞和炎症细胞的迁移、增殖和凋亡,从而影响内膜形成、动脉粥样硬化和动脉瘤,这在临床和小鼠基因敲除和转基因研究中得到了证实。这些实验揭示了 MMPs 在组织破坏和修复方面的显著平衡作用。天然存在的 MMP 组织抑制剂(TIMPs)、多效性介质(如四环素)、化学合成的小分子 MMP 抑制剂(MMPis)和抑制性抗体,在血管疾病的动物模型中都显示出了效果,但只有强力霉素在患者中进行了广泛评估。广泛特异性 MMPis 的局限性在于,它们既阻止基质降解,也阻止不同 MMPs 的组织修复功能。因此,已经开发出具有更特异性的 MMPis,并且最近在动脉粥样硬化模型中的研究准确地复制了相应基因敲除的表型。这篇综述记录了 MMPs 及其抑制剂在血管病理学中的作用,并考虑了将这些发现转化为新的治疗方法的前景。

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Matrix metalloproteinase inhibition therapy for vascular diseases.基质金属蛋白酶抑制治疗血管疾病。
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