勃起功能障碍
医学
内科学
内分泌学
腺相关病毒
血管生成
勃起组织
血管内皮生长因子
遗传增强
生物
基因
血管内皮生长因子受体
载体(分子生物学)
重组DNA
生物化学
作者
Zhe Yu,Yan Zhang,Zhe Tang,Jingyu Song,Xintao Gao,Taotao Sun,Yang Liu,Jun Yang,Tao Wang,Jihong Liu
标识
DOI:10.1016/j.jsxm.2019.06.011
摘要
ABSTRACT Introduction Novel therapeutic targets for diabetes-induced erectile dysfunction (DED) are urgently needed. Previous studies have proved that S100A1, a small Ca2+-binding protein, is a pluripotent regulator of cardiovascular pathophysiology. Its absence is associated with endothelial dysfunction, the central event linking cardiovascular changes in diabetes. However, the role of S100A1 in DED remains unknown. Aim To explore the effect and underlying mechanisms of S100A1 in restoring erectile function in type I diabetic rat model. Methods Diabetes was induced by intraperitoneal injection of streptozotocin and then screened by apomorphine (APO) to confirm erectile dysfunction. Rats that met the criteria of penile erection were marked as APO-positive; otherwise, the result was APO-negative. In experiment 1, S100A1 gene expression alterations in the corpus cavernosum in moderate and established stages of DED were analyzed. In experiment 2, S100A1 and control GFP gene were delivered into the corpus cavernosum in APO-negative rats by adeno-associated virus (AAV) serotype 9. Erectile function was assessed at 4 weeks after gene therapy. Main Outcome Measures Erectile response, histologic and molecular alterations. Results S100A1 protein was localized to the area surrounding the cavernosal sinusoids in the penis, and it was gradually downregulated synchronized with the progression of DED. Compared with an injection of AAV-GFP, a single injection of AAV-S100A1 significantly restored erectile function in diabetic rats. S100A1 overexpression significantly upregulated the expression of endogenous VEGF-A, promoted VEGFR2 internalization, and subsequently triggered the protein kinase B–endothelial nitric oxide synthase pathway in diabetic erectile tissues. Marked increases in nitric oxide and endothelial content were noted in AAV-S100A1-treated diabetic rats. Clinical Implications Local S100A1 overexpression may be an alternative therapy for DED and should be further investigated by future clinical studies. Strength & Limitations This is the first study demonstrating the angiogenic role of S100A1 in DED, but does not preclude the contribution of the effects of S100A1 in other tissues such as the neuronal tissue on the functional effects observed in erectile responses. Conclusion The decreased expression of S100A1 during hyperglycemia might be important in the development of erectile dysfunction. S100A1 may play a potential role in restoring erectile function in rats with DED through modulating cavernous angiogenesis.
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