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Systemic and metabolic effects of PDE5-inhibitor drugs

机译:PDE5抑制剂药物的全身和代谢作用

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摘要

Phosphodiesterase type-5 inhibitor (PDE5-i) drugs were first marketed in 1998 (sildenafil) for 'ondemand' treatment of male erectile dysfunction (ED) of any origin. They selectively inhibit intrapenile PDE5 isoenzyme which in turn increases intracellular cyclic guanosine monophosphate levels, thus resulting in prolonged relaxation of cavernosum smooth muscle cells and facilitating the erectile process. Since 2003, two new molecules (tadalafil and vardenafil) have been introduced, resulting in greater interest in these compounds and leading patients to ask for more prescriptions from their doctors. The vast use of PDE5-i in diabetic and cardiovascular ED patients led researchers to investigate their possible extra sexual effects. Several studies investigating their effects on endothelium, coronary and pulmonary circulation, inferior oesophageal sphincter and kidney functions have appeared and, finally, sildenafil was approved for the treatment of pulmonary arterial hypertension. Recent animal studies highlighted a possible interaction between chronic PDE5 inhibition and glucose homeostasis which occurs through a marked improvement of high fat diet induced insulin resistance. If this data is extended to humans, a new scenario will be opened for the chronic use of PDE5-i for sexual rehabilitation along with cardiovascular and metabolic benefits.
机译:磷酸二酯酶5型抑制剂(PDE5-i)药物于1998年首次上市(西地那非),用于“按需”治疗任何来源的男性勃起功能障碍(ED)。它们选择性抑制阴茎内PDE5同工酶,进而增加细胞内环鸟苷单磷酸水平,从而导致海绵体平滑肌细胞长时间松弛并促进勃起过程。自2003年以来,引入了两个新分子(他达拉非和伐地那非),引起了人们对这些化合物的更大兴趣,并导致患者要求医生提供更多处方。 PDE5-i在糖尿病和心血管ED患者中的广泛使用促使研究人员研究其可能的额外性影响。已经出现了几项研究其对内皮,冠状动脉和肺循环,食道下括约肌和肾功能的影响的研究,最后,西地那非被批准用于治疗肺动脉高压。最近的动物研究强调了慢性PDE5抑制与葡萄糖稳态之间可能的相互作用,这是通过高脂饮食诱导的胰岛素抵抗的显着改善而发生的。如果将这些数据扩展到人类,将为长期使用PDE5-i进行性康复以及心血管和代谢益处开辟新局面。

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