Introduction
Traditional
beta-blockers have sometimes been associated with erectile dysfunction (ED).
Nebivolol is a cardioselective β1-adrenoceptor
antagonist that promotes vasodilation through a nitric oxide (NO)-dependent
mechanism.
Aim
We
evaluated the effects of nebivolol on the NO/cyclic guanosine monophosphate
(cGMP) signaling pathway, on erectile function and dysfunction, and in human
penile vascular tissues.
Methods
Erectile
response to cavernosal nerve electrical stimulation in control and
diabetes-induced ED rats were evaluated, along with serum nitrite/nitrate (NOx)
concentration and plasma/tissue cGMP levels. Endothelium-dependent and
sildenafil-induced relaxation of isolated human corpus cavernosum (HCC) and
human penile resistance arteries (HPRA) were also determined.
Main Outcome Measures
Main Outcome Measures
The effects of nebivolol on erectile function and
dysfunction and on NO/cGMP-mediated responses.
Results
Results
Treatment
with nebivolol significantly potentiated erectile response in control rats,
regardless of its effects on blood pressure. Nebivolol increased NOx and plasma
cGMP by 3-fold and 2.75-fold, respectively, and significantly augmented the
elevation of plasma cGMP produced by sildenafil. Nebivolol enhanced
endothelium-dependent and sildenafil-induced relaxations of HCC tissue, and
produced endothelium-dependent vasodilation of HPRA. Nebivolol, but not
atenolol, significantly improved erectile response in diabetic rats (51.6%,
53.2%, and 87.1% of response at 3 Hz in nondiabetic rats, for
vehicle-treated, atenolol-treated, and nebivolol-treated diabetic rats,
respectively); after sildenafil administration, ED was completely reversed in
nebivolol-treated diabetic rats (69.6% and 112% for diabetic rats treated with
sildenafil and nebivolol plus sildenafil, respectively). Accordingly, nebivolol
restored systemic NOx levels and cGMP content in penile tissue from these
animals.
Conclusions
Conclusions
Nebivolol
in vivo activated the NO/cGMP pathway, enhanced erectile response and reversed
ED in diabetic rats. Moreover, nebivolol in vitro potentiated NO/cGMP-mediated
relaxation of human erectile tissues. These effects may account for the low
incidence of ED in nebivolol-treated hypertensive patients. Nebivolol therefore
may have utility in the treatment of ED, particularly ED associated with
diabetes.
Reference:
Angulo J, Wright HM, Cuevas P,
González-Corrochano R, Fernández A, Cuevas B, La Fuente JM, Gupta S, and de
Tejada IS. Nebivolol dilates human penile arteries and reverses erectile
dysfunction in diabetic rats through enhancement of nitric oxide signaling. J
Sex Med 2010;7:2681–2697.
