4.1 Article

A comparative study of sildenafil, NCX-911 and BAY41-2272 on the anococcygeus muscle of diabetic rats

Journal

INTERNATIONAL JOURNAL OF IMPOTENCE RESEARCH
Volume 16, Issue 6, Pages 479-485

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/sj.ijir.3901224

Keywords

NCX-911; sildenafil; BAY41-2272; soluble guanylyl cyclase; nitric oxide; erectile dysfunction; PDE5 inhibitors; diabetes mellitus

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We compared the effects of a nitric oxide (NO)-releasing sildenafil (NCX-911), NO-independent soluble guanylate cyclase activator (BAY41-2272) and sildenafil on the anococcygeus muscle from streptozotocin-induced 16-weeks diabetic rats. NCX-911, BAY41-2272 and sildenafil reduced the phenylephrine-induced tone in the control group (EC50 = 1088.8 +/- 165.0, 151.6 +/- 9.3 and 827.1 +/- 167.3 nM, respectively). The potencies of NCX-911 and BAY41-2272 were not altered, but that of sildenafil was significantly reduced in the diabetic group. EC50 values for NCX-911, BAY41-2272 and sildenafil in the diabetic group were 1765.9 +/- 303.5, 209.7 +/- 27.3 and 2842.2 +/- 640.3 nM, respectively ( P<0.05 for sildenafil). Nitrergic relaxation responses were significantly decreased in the diabetic group. The remaining nitrergic relaxation responses were potentiated by BAY41-2272 but not by sildenafil or NCX-911. These results confirm that endogenous NO derived from nitrergic nerves is significantly decreased in diabetes, and suggest that NO-releasing PDE5 inhibitors and NO-independent soluble guanylate cyclase activators could be more useful than PDE5 inhibitors in the treatment of ED in long-term diabetes.

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