盐酸雷洛昔芬对心血管的影响。

A. Saitta, Nunziate Morabito, Nicola Frisina, Domenico Cucinotte, Francesco Corrado, R. D’Anna, D. Altavilla, G. Squadrito, L. Minutoli, Vincenzo Arcoraci, Francesco Cancellieri, F. Squadrito
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引用次数: 46

摘要

盐酸雷洛昔芬与雌激素受体结合并表现出组织选择性效应;因此,它属于一类最近被描述为选择性雌激素受体调节剂(SERMs)的药物。雷洛昔芬的组织选择性可能通过以下几种机制实现:配体结构、配体与不同组织中不同受体亚型的相互作用以及配体结合后的细胞内事件。雷洛昔芬对骨骼和脂质有雌激素激动作用,对乳房和子宫有雌激素拮抗剂作用。除了对骨质疏松症的疗效外,最近的临床前和临床研究结果表明,雷洛昔芬对心血管系统也有有益的作用。这些发现表明,雷洛昔芬可能具有保护心脏的特性,而不会增加患癌症的风险或产生其他副作用。雷洛昔芬已被证明可以降低血浆中总脂蛋白和低密度脂蛋白胆固醇的浓度,其效果与雌激素相似。然而,与雌激素不同,雷洛昔芬不会增加血浆中的高密度脂蛋白胆固醇和甘油三酯水平。内皮被认为在动脉粥样硬化的发生中起重要作用。一些证据表明,干预内皮功能可能影响冠状动脉疾病的进展和心血管事件的发生率。雷洛昔芬增加一氧化氮/内皮素-1比值,改善绝经后妇女内皮依赖性血管舒缩的程度与雌激素相同。此外,在两项针对绝经后妇女的随机试验中,雷洛昔芬降低了同型半胱氨酸水平,这是心血管疾病发展的另一个独立危险因素。虽然雌激素仍然是大多数绝经后妇女激素治疗的首选药物,但雷洛昔芬可能是有冠状动脉疾病风险的妇女的替代药物。
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Cardiovascular effects of raloxifene hydrochloride.
Raloxifene hydrochloride binds to the estrogen receptor and shows tissue-selective effects; thus, it belongs to a class of drugs recently described as selective estrogen receptor modulators (SERMs). Tissue selectivity of raloxifene may be achieved through several mechanisms: the ligand structure, interaction of the ligand with different receptor subtypes in various tissues, and intracellular events after ligand binding. Raloxifene has estrogen-agonist effects on bone and lipids and estrogen antagonist effects on the breast and uterus. In addition to its well established effects on osteoporosis, recent preclinical and clinical findings suggest that raloxifene also possesses beneficial effects on the cardiovascular system. These findings indicated that raloxifene may have cardioprotective properties without an increased risk of cancer or other side effects. Raloxifene has been shown to reduce total and low-density lipoprotein cholesterol concentrations in plasma, an effect similar to that produced by estrogens. Unlike estrogens, however, raloxifene does not increase high-density lipoprotein cholesterol and triglyceride levels in plasma. Endothelium is thought to play an important role in the genesis of atherosclerosis. Several lines of evidence suggest that an intervention with endothelial function might influence the progression of coronary disease and the incidence of cardiovascular events. Raloxifene increases the nitric oxide/endothelin-1 ratio, and improves endothelium-dependent vasomotion in post-menopausal women to the same extent as estrogens. Furthermore, in two randomized trials on post-menopausal women raloxifene reduced homocysteine levels, another independent risk factor for the development of cardiovascular disease. Although estrogens remain the drugs of choice in the hormonal therapy of most postmenopausal women, raloxifene may represent and alternative in women who are at risk of coronary artery disease.
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