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睾酮和磷酸二酯酶 5 抑制剂:预防内科学和性医学中内皮损伤的新策略?

Testosterone and phosphodiesterase type-5 inhibitors: new strategy for preventing endothelial damage in internal and sexual medicine?

机构信息

Dip.to Fisiopatologia Medica, Room 37, Viale Policlinico 155, 00161 Rome Italy.

出版信息

Ther Adv Urol. 2009 Oct;1(4):179-97. doi: 10.1177/1756287209344992.

Abstract

Normal vascular endothelium is essential for the synthesis and release of substances affecting vascular tone (e.g. nitric oxide; NO), cell adhesion (e.g. endothelins, interleukins), and the homeostasis of clotting and fibrinolysis (e.g. plasminogen inhibitors, von Willebrand factor). The degeneration of endothelial integrity promotes adverse events (AEs) leading to increased atherogenesis and to the development of vascular systemic and penile end-organ disease. Testosterone (T) is an important player in the regulation of vascular tone through non-genomic actions exerted via blockade of extracellular-calcium entry or activation of potassium channels; also, adequate T concentrations are paramount for the regulation of phosphodiesterase type-5 (PDE5) expression and finally, for the actions exerted by hydrogen sulphide, a gas involved in the alternative pathway controlling vasodilator responses in penile tissue. It is known that an age-related decline of serum T is reported in approximately 20 to 30% of men whereas T deficiency is reported in up to 50% of men with metabolic syndrome or diabetes. A number of laboratory and human studies have shown the combination of T and other treatments for erectile dysfunction (ED), such as PDE5 inhibitors, to be more beneficial in patients with ED and hypogonadism, who fail monotherapy for sexual disturbances.The aim of this review is to show evidence on the role of T and PDE5 inhibitors, alone or in combination, as potential boosters of endothelial function in internal medicine diseases associated with reduced T or NO bioavailability, i.e. metabolic syndrome, obesity, diabetes, coronary artery disease, hyperhomocysteinemia, that share common risk factors with ED. Furthermore, the possibility of such a strategy to prevent endothelial dysfunction in men at increased cardiovascular risk is discussed.

摘要

正常的血管内皮对于影响血管张力的物质的合成和释放至关重要(例如一氧化氮;NO)、细胞黏附(例如内皮素、白细胞介素)以及凝血和纤维蛋白溶解的内稳态(例如纤溶酶原抑制剂、血管性血友病因子)。内皮完整性的退化会促进不良事件(AE)的发生,导致动脉粥样硬化的增加以及血管系统和阴茎终末器官疾病的发展。睾丸激素(T)是通过阻断细胞外钙内流或激活钾通道来调节血管张力的重要因素;此外,足够的 T 浓度对于调节磷酸二酯酶 5 型(PDE5)的表达以及最终调节参与控制阴茎组织中血管舒张反应的替代途径的硫化氢的作用至关重要。据报道,大约 20%至 30%的男性血清 T 水平会随着年龄的增长而下降,而在代谢综合征或糖尿病患者中,高达 50%的男性会出现 T 缺乏症。许多实验室和人体研究表明,T 与其他治疗勃起功能障碍(ED)的药物(如 PDE5 抑制剂)联合使用对 ED 和性腺功能减退症患者更有益,这些患者对单一药物治疗性障碍的反应不佳。本综述的目的是展示 T 和 PDE5 抑制剂单独或联合使用作为潜在的内皮功能增强剂的作用证据,这些药物可用于治疗与 T 或 NO 生物利用度降低相关的内科疾病,即代谢综合征、肥胖症、糖尿病、冠心病、高同型半胱氨酸血症,这些疾病与 ED 具有共同的危险因素。此外,还讨论了这种策略在增加心血管风险的男性中预防内皮功能障碍的可能性。

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