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Actions of Calcium Channel Blockers on Vascular Proteoglycan Synthesis: Relationship to Atherosclerosis

机译:钙通道阻滞剂对血管蛋白聚糖合成的作用:与动脉粥样硬化的关系。

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摘要

Calcium channel blockers (CCBs) are a widely used group of antihypertensive agents. CCBs are efficacious in the reduction of blood pressure but the extent to which they manifest beneficial effects on cardiovascular disease is variable. Clinical studies indicate that pleiotropic actions make significant contributions to the efficacy of agents aimed at preventing atherosclerosis. The “response to retention” hypothesis implicates the binding and retention of lipoproteins by glycosaminoglycan chains on proteoglycans as an initiating step in atherogenesis. Atherogenic factors act as agonists and several classes of drugs including peroxisome proliferating-activated receptor (PPAR)-α and -γ ligands act as antagonists in this model. Initial data have demonstrated that high concentrations of CCBs inhibit proteoglycan synthesis. Newer preliminary data show that the action is very modest at reasonable concentrations and appears to be independent of calcium channel blocking activity. We have reviewed the role of cardiovascular drugs acting on vascular smooth muscle proteoglycan synthesis and considered the potential action of CCBs in this model. We conclude that the inhibition of proteoglycan synthesis by CCBs does not play a role in the attenuation of atherosclerosis; however, the antihypertensive efficacy and alternative beneficial actions provide support for the use of CCBs in the therapy of cardiovascular disease.
机译:钙通道阻滞剂(CCB)是一组广泛使用的降压药。 CCB在降低血压方面有效,但是它们对心血管疾病表现出有益作用的程度是可变的。临床研究表明,多效作用对旨在预防动脉粥样硬化的药物的功效做出了重大贡献。 “对保留的反应”假说暗示了蛋白聚糖上糖胺聚糖链对脂蛋白的结合和保留是动脉粥样硬化形成的起始步骤。致动脉粥样硬化因子充当激动剂,包括过氧化物酶体增殖激活受体(PPAR)-α和-γ配体在内的几类药物在该模型中充当拮抗剂。初步数据表明,高浓度的CCB会抑制蛋白聚糖的合成。最新的初步数据表明,在合理的浓度下该作用非常适中,并且似乎与钙通道阻滞活性无关。我们已经综述了心血管药物在血管平滑肌蛋白聚糖合成中的作用,并考虑了CCB在该模型中的潜在作用。我们得出的结论是,CCBs对蛋白聚糖合成的抑制作用在动脉粥样硬化的减轻中不起作用。但是,降压功效和替代有益作用为CCB在心血管疾病治疗中的使用提供了支持。

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