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Am J Physiol Renal Physiol (October 28, 2009). doi:10.1152/ajprenal.00281.2009
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Submitted on May 22, 2009
Revised on October 14, 2009
Accepted on October 27, 2009

Differential vulnerabilities of urethral afferents in diabetes and discovery of a novel urethra-to-urethra reflex

Zhongguang Yang1, Paul C Dolber1, and Matthew O Fraser1*

1 Duke University Medical Center

* To whom correspondence should be addressed. E-mail: matthew.fraser{at}duke.edu.

Urethral reflexes are important regulators of micturition, and impairment of urethral afferent neuronal function may disrupt coordinated bladder and urethral activity, thereby contributing to voiding dysfunction in lower urinary tract disorders. Chemical stimulation by intraurethral perfusion with irritant solutions was used to determine whether urethral afferent neuronal function is altered in diabetes mellitus (DM). Sprague-Dawley rats were studied 10 weeks after streptozotocin injection to induce DM or vehicle alone. Escalating doses of capsaicin (0.1-30 μM) or AA (0.01-1%) in saline were perfused intraurethrally while recording isovolumetric bladder activity, urethral perfusion pressure, and electromyography of the external urethral sphincter (EUS-EMG). Some rats were additionally treated with {alpha}-bungarotoxin, hexamethonium, or bilateral transection of the sensory branches of the pudendal nerves (PudSNx). Intraurethral capsaicin inhibited bladder contractions in 6/7 control rats but not in any of 6 DM rats. Low frequency oscillations (LFOs) of intraurethral pressure were observed in 5/6 control rats with capsaicin-induced bladder inhibition. In contrast, intraurethral AA inhibited bladder contractions and enhanced tonic EUS-EMG activity in 6/6 control and 5/6 DM rats. LFOs occurred in 4/6 control and 3/5 DM rats with bladder inhibition. Chemically induced bladder inhibition and LFOs were not prevented by {alpha}-bungarotoxin, but were eliminated by PudSNx and hexamethonium. Finally, LFOs were followed by phasic EUS activity. These findings show that DM affects urethral afferent neurons differentially, compromising those expressing TRPV1 receptors. Urethral smooth muscle LFOs are neurogenically mediated and induce EUS activity, revealing the existence of a hitherto undescribed reflex pathway: a smooth-to-striated muscle urethra-to-urethra reflex.







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