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From the * Department of Urology, St Joseph's
Health Care, Lawson Health Research Institute, and the
Department of Medical Biophysics, The
University of Western Ontario, London, Canada.
| Correspondence to: Dr Gerald Brock, Department of Urology, St Joseph's Health Care, London, Canada N6A 4V2 (e-mail: gebrock{at}sympatico.ca). |
-actin, nitrotyrosine, and endothelial cell
integrity. Urine nitrite and nitrate (NOx) concentration was
quantified, and electrolytes were tested by a serum biochemistry panel. A
significant decrease in ICP was recorded in the diabetic animals, with
improvement measured in the animals receiving PDE5 inhibitors either with or
without vitamin E; the controls had a pressure of 54.8 ± 5.3 cm
H2O, the vitamin E group had a pressure of 73.5 ± 6.6 cm
H2O, the sildenafil group had a pressure of 78.4 ± 10.77 cm
H2O, and the vitamin E plus sildenafil group had a pressure of 87.9
± 5.5 cm H2O (P < .05), compared with the normal cohorts
at 103.0 ± 4.8 cm H2O. Histoexaminations showed improved
nNOS, endothelial cell, and smooth muscle cell staining in the vitamin E plus
sildenafil group compared to the control animals. Urine NOx
increased significantly in all the diabetic groups but was blunted in the
vitamin E and vitamin E plus sildenafil groups. A significant increase in
positive staining for nitrotyrosine was observed in the vitamin E plus
sildenafil group. Vitamin E enhanced the therapeutic effect of the PDE5
inhibitor in this study, supporting the potential use of oxygen free radical
scavengers in salvaging erectile function in diabetic patients.
Key words: Impotence, vitamin E, sildenafil, nitric oxide, phosphodiesterase type 5
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