在人类阴茎镰状细胞病相关性阴茎异常勃起中勃起调节因子的分子分析。
Molecular analysis of erection regulatory factors in sickle cell disease associated priapism in the human penis.
机构信息
Department of Urology, Johns Hopkins Medical Institutions, Baltimore, Maryland, USA.
出版信息
J Urol. 2013 Feb;189(2):762-8. doi: 10.1016/j.juro.2012.08.198. Epub 2012 Oct 8.
PURPOSE
Priapism is a vasculopathy that occurs in approximately 40% of patients with sickle cell disease. Mouse models suggest that dysregulated nitric oxide synthase and RhoA/ROCK signaling as well as increased oxidative stress may contribute to the mechanisms of sickle cell disease associated priapism. We examined changes in the protein expression of nitric oxide synthase and ROCK signaling pathways, and a source of oxidative stress, NADPH oxidase, in penile erectile tissue from patients with a priapism history etiologically related and unrelated to sickle cell disease.
MATERIALS AND METHODS
Human penile erectile tissue was obtained from 5 patients with sickle cell disease associated priapism and from 6 with priapism of other etiologies during nonemergent penile prosthesis surgery for erectile dysfunction or priapism management and urethroplasty. Tissue was also obtained from 5 control patients without a priapism history during penectomy for penile cancer. Samples were collected, immediately placed in cold buffer and then frozen in liquid nitrogen. The expression of phosphodiesterase 5, endothelial nitric oxide synthase, neuronal nitric oxide synthase, inducible nitric oxide synthase, RhoA, ROCK1, ROCK2, p47(phox), p67(phox), gp91(phox) and β-actin were determined by Western blot analysis. Nitric oxide was measured using the Griess reaction.
RESULTS
In the sickle cell disease group phosphodiesterase 5 (p <0.05), endothelial nitric oxide synthase (p <0.01) and RhoA (p <0.01) expression was significantly decreased, while gp91(phox) expression (p <0.05) was significantly increased compared to control values. In the nonsickle cell disease group endothelial nitric oxide synthase, ROCK1 and p47(phox) expression (each p <0.05) was significantly decreased compared to control values. Total nitric oxide levels were not significantly different between the study groups.
CONCLUSIONS
Mechanisms of sickle cell disease associated priapism in the human penis may involve dysfunctional nitric oxide synthase and ROCK signaling, and increased oxidative stress associated with NADPH oxidase mediated signaling.
目的
阴茎异常勃起是一种血管疾病,约 40%的镰状细胞病患者会发生这种疾病。小鼠模型表明,一氧化氮合酶和 RhoA/ROCK 信号的失调以及氧化应激的增加可能是导致镰状细胞病相关阴茎异常勃起的机制。我们研究了与镰状细胞病相关的阴茎异常勃起患者和与镰状细胞病无关的其他病因引起的阴茎异常勃起患者的阴茎勃起组织中一氧化氮合酶和 ROCK 信号通路以及氧化应激的来源 NADPH 氧化酶的蛋白表达变化。
材料和方法
在非紧急阴茎假体手术治疗勃起功能障碍或阴茎异常勃起和尿道成形术期间,从 5 例镰状细胞病相关阴茎异常勃起患者和 6 例其他病因引起的阴茎异常勃起患者中获得了人类阴茎勃起组织。还从 5 例无阴茎异常勃起史的阴茎癌患者的阴茎切除术期间获得了组织。收集样本后,立即将其置于冷缓冲液中,然后在液氮中冷冻。通过 Western blot 分析测定磷酸二酯酶 5、内皮型一氧化氮合酶、神经元型一氧化氮合酶、诱导型一氧化氮合酶、RhoA、ROCK1、ROCK2、p47(phox)、p67(phox)、gp91(phox)和β-肌动蛋白的表达。使用格里斯反应测量一氧化氮。
结果
在镰状细胞病组中,磷酸二酯酶 5(p <0.05)、内皮型一氧化氮合酶(p <0.01)和 RhoA(p <0.01)的表达显著降低,而 gp91(phox)的表达(p <0.05)与对照组相比显著增加。在非镰状细胞病组中,内皮型一氧化氮合酶、ROCK1 和 p47(phox)的表达(p <0.05)与对照组相比显著降低。研究组之间的总一氧化氮水平无显著差异。
结论
人类阴茎镰状细胞病相关阴茎异常勃起的机制可能涉及一氧化氮合酶和 ROCK 信号的功能障碍,以及 NADPH 氧化酶介导的信号转导相关的氧化应激增加。
Zotero 插件