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首页> 外文期刊>Nature reviews. Urology >Treatment of Peyronie's disease with PDE5 inhibitors: An antifibrotic strategy
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Treatment of Peyronie's disease with PDE5 inhibitors: An antifibrotic strategy

机译:PDE5抑制剂治疗Peyronie病:抗纤维化策略

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Peyronie's disease (PD) is a localized fibrotic condition of the tunica albuginea that is associated with risk factors for corpora cavernosa fibrosis (such as advanced age and diabetes) and Dupuytren contracture, another localized fibrotic process. Most of the current pharmacological treatments for PD are not based on antifibrotic approaches that have shown promising results in animal models and clinical efficacy in other fibrotic conditions, which may explain why they are generally unsuccessful. Evidence gathered in human specimens and animal models of PD have elucidated aspects of its etiology and histopathology, showing that overexpression of transforming growth factor Β1, plasminogen activator inhibitor 1, reactive oxygen species and other profibrotic factors, which are, in most cases, assumed to be induced by trauma to the tunica albuginea, leads to myofibroblast accumulation and excessive deposition of collagen. At the same time, a steady overexpression of inducible nitric oxide synthase, leading to increased nitric oxide and cGMP levels, seems to act as an endogenous antifibrotic mechanism. This process has also been reported in corporal and cardiovascular fibrosis, and has led to the demonstration that long-term continuous administration of phosphodiesterase type 5 inhibitors counteracts the development of a PD-like fibrotic plaque in a rat model, and later extended to the prevention of corporal fibrosis in animal models of erectile dysfunction.
机译:佩罗尼氏病(PD)是白膜上皮的局部纤维化病状,与海绵体纤维化(例如高龄和糖尿病)和Dupuytren挛缩症(另一种局部纤维化过程)的危险因素有关。当前用于PD的大多数药物治疗都不基于抗纤维化方法,该方法已在动物模型中显示出可喜的结果,并在其他纤维化条件下具有临床疗效,这可以解释为什么它们通常不成功。在PD的人类标本和动物模型中收集的证据阐明了其病因和组织病理学方面,表明转化生长因子factor1,纤溶酶原激活物抑制剂1,活性氧和其他纤维化因子的过表达在大多数情况下被认为是被白膜的外伤诱导,导致成肌纤维细胞积聚和胶原蛋白的过度沉积。同时,诱导型一氧化氮合酶的稳定过表达,导致一氧化氮和cGMP水平升高,似乎是一种内源性抗纤维化机制。在人体和心血管纤维化中也报告了该过程,并导致证明了长期连续施用5型磷酸二酯酶抑制剂可抵消大鼠模型中PD样纤维斑的形成,后来扩展到了预防纤维化在勃起功能障碍动物模型中的作用

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