选择性内皮素受体拮抗剂对糖尿病阴茎血管内皮生长因子信号系统的影响:糖尿病性勃起功能障碍的可能临床意义

A. Maqbool, S. Jesmin, Chishimba N Mowa, S. N. Sultana, N. Shimojo, Y. Matsuishi, Takeru Shima, N. Yamaguchi, T. Miyauchi, S. Kawano, M. Moroi
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摘要

由于糖尿病引起的血管和神经病变并发症,大约50%的男性糖尿病患者受到勃起功能障碍(ED)的影响。血管内皮生长因子(Vascular endothelial growth factor, VEGF)在各种糖尿病并发症中的致病相关性已被广泛研究,我们已经注意到,在II型糖尿病大鼠模型的阴茎胰岛素抵抗阶段,VEGF信号明显减少。本研究采用三周链脲佐菌素(STZ)诱导的糖尿病(DM)大鼠模型,通过NO机制测定VEGF在阴茎组织中的表达,并随后研究其内皮素拮抗剂对这些变化的影响。雄性Sprague-Dawley大鼠(体重453±23 g)经高血糖确诊为糖尿病后,给予柠檬酸盐溶液或STZ (65 mg/kg IP),在糖尿病1周后,将动物分为内皮素- a (ET-A)受体拮抗剂(TA-0201, 1 mg/kg)或生理盐水,经渗透小泵灌注2周后处死。糖尿病大鼠的血糖水平(405±103 mg/dL)明显高于非糖尿病大鼠(120±8 mg/dL),糖尿病大鼠阴茎局部ET-1水平升高20%。DM大鼠阴茎组织中VEGF表达下降30%,ET拮抗剂改善了这一现象。DM大鼠阴茎NO和eNOS水平下降,而ET-A受体拮抗剂显著增加。因此,我们推断ET拮抗似乎能够恢复下调的VEGF,并可能有效地恢复DM中下降的NO和eNOS水平。
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Effects of Selective Endothelin Receptor Antagonist on Vegf Signaling System in Diabetic Penis: A Possible Clinical Implication for Diabetes Induced Erectile Dysfunction
Erectile dysfunction (ED) affects around 50 percent of male diabetic patients due to vascular and neuropathic complications arising from diabetes. Vascular endothelial growth factor (VEGF) has been extensively investigated for its pathogenic relevance in various diabetes complications, and we have already noted that VEGF signaling is significantly reduced at the insulin-resistant stage in the penis of type II diabetic rat model. The present research used a three-week streptozotocin (STZ)-induced diabetic (DM) rat model to determine the expression of VEGF with NO mechanism in penile tissue and subsequently investigated its impact endothelin antagonism on these shifts. Citrate saline vehicle or STZ (65 mg/kg IP) was administered to male Sprague-Dawley rats (weight 453 ± 23 g). Hyperglycemia confirmed diabetes, and then after 1 week of diabetes, animals were divided into receiving endothelin-A (ET-A) receptor antagonists (TA-0201, 1 mg/kg) or saline by osmotic minipump for 2 weeks and then sacrificed. Significantly improved glucose levels in DM rats (405 ± 103 mg/dL) relative to non-DM rats (120 ± 8 mg/dL) and higher local ET-1 levels in DM penis by 20% are observed. A 30 percent decline in penile tissue expression of VEGF was observed in DM rats and improved by an antagonist with ET. Penile NO and eNOS levels in DM rats decreased, while ET-A receptor antagonist significantly increased. Therefore, we infer that ET antagonism seemed able to restore the down-regulated VEGF and was possibly efficient in restoring the decreased levels of NO and eNOS in DM.
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