了解并针对勃起功能障碍中的Rho激酶通路
Understanding and targeting the Rho kinase pathway in erectile dysfunction.
作者信息
Sopko Nikolai A, Hannan Johanna L, Bivalacqua Trinity J
机构信息
James Buchanan Brady Urological Institute, The Johns Hopkins School of Medicine, 1800 Orleans Street/Marburg 134, Baltimore, MD 21287, USA.
出版信息
Nat Rev Urol. 2014 Nov;11(11):622-8. doi: 10.1038/nrurol.2014.278. Epub 2014 Oct 14.
Abstract
Erectile dysfunction (ED) is a common disorder that affects a quarter of US men, and has many causes, including endothelial impairment, low testosterone levels, prior surgical manipulation, and/or psychogenic components. Penile erection is a complex process requiring neurally mediated relaxation of arteriolar smooth muscle and engorgement of cavernosal tissues, mediated by nitric oxide (NO). Current medical therapies for ED largely seek to maximize endogenous NO signalling. Certain aetiologies, including diabetes, are difficult to treat with current modalities, emphasizing the need for new molecular targets. Research has demonstrated the importance of RhoA-Rho-associated protein kinase (ROCK) signalling in maintaining a flaccid penile state, and inhibition of RhoA-ROCK signalling potentiates smooth-muscle relaxation in an NO-independent manner. The mechanisms and effects of RhoA-ROCK signalling and inhibition suggest that the RhoA-ROCK pathway could prove to be a new therapeutic target for the treatment of ED.
摘要
勃起功能障碍(ED)是一种常见疾病,影响着四分之一的美国男性,其病因众多,包括内皮功能损害、睾酮水平低下、既往手术操作和/或心理因素。阴茎勃起是一个复杂的过程,需要神经介导的小动脉平滑肌松弛以及海绵体组织充血,这一过程由一氧化氮(NO)介导。目前治疗ED的药物疗法主要致力于最大化内源性NO信号传导。某些病因,如糖尿病,目前的治疗方式难以有效治疗,这凸显了寻找新分子靶点的必要性。研究表明,RhoA- Rho相关蛋白激酶(ROCK)信号传导在维持阴茎疲软状态中起重要作用,抑制RhoA-ROCK信号传导可通过不依赖NO的方式增强平滑肌松弛。RhoA-ROCK信号传导及其抑制的机制和效果表明,RhoA-ROCK通路可能成为治疗ED的新治疗靶点。
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