Spontaneous phasic activity of the pig urinary bladder smooth muscle: characteristics and sensitivity to potassium channel modulators

Buckner, Steven A.; Milicic, Ivan; Daza, Anthony V.; Coghlan, Michael J.; Gopalakrishnan, Murali

doi:10.1038/sj.bjp.0704499

Cited by 95 publications

(114 citation statements)

References 33 publications

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“…Those other cell types include the endometrium which lies inside the myometrial smooth muscle of the uterus, the enteric nervous system which innervates the intestinal smooth muscle of the duodenum, and the urothelium which separates the detrusor smooth muscle of the bladder wall from the urine inside. But while these nonmuscular cells may be able to modulate spontaneous contractility of the adjacent smooth muscle cell layers (Gershon, 1981;Granger et al, 1986;Haynes and Pennefather, 1993;Buckner et al, 2002;Azadzoi et al, 2004;Bulbul et al, 2007;Kanai et al, 2007), they are not likely the primary site for gemfibrozil's relaxant effects. If, for example, gemfibrozil's relaxation of the duodenal contractility seen in Figure 5 were mediated solely by inhibition of enteric neuronal release of contractile neurotransmitters, then we would not expect to see its relaxant influence in uterus and bladder as well.…”

Section: Effects Of Gemfibrozil On Spontaneous Contractions Of Rat Utmentioning

confidence: 99%

“…uterus, duodenum and bladder. These tissues are known for their ability to exhibit spontaneously-occurring phasic rhythmic contractions, which are physiologically relevant and can be observed in vitro without the need to administer contractile agents (Small and Weston, 1971;Gershon, 1981;Granger et al, 1986;Leroy et al, 1991;Haynes and Pennefather, 1993;Buckner et al, 2002;Vedernikov et al, 2003;Azadzoi et al, 2004;Szigeti et al, 2005;Bulbul et al, 2007;Kanai et al, 2007). We determined if gemfibrozil inhibits these spontaneous activities.…”

Section: Introductionmentioning

confidence: 99%

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Evidence of direct smooth muscle relaxant effects of the fibrate gemfibrozil

Phelps

Peuler

2010

J. Smooth Muscle Res.

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Fibrates are commonly employed to treat abnormal lipid metabolism via their unique ability to stimulate peroxisome proliferator-activated receptor alpha (PPARα). Interestingly, they also decrease systemic arterial pressure, despite recent evidence that PPARα may contribute to expression of renin and related hypertension. Yet, mechanisms responsible for their potential antihypertensive activity remain unresolved. Rapid decreases in arterial pressure following bolus intravenous injections of bezafibrate strongly suggest they may relax arterial smooth muscle directly. But since bezafibrate is highly susceptible to photodegradation in aqueous media, it has never been critically tested for this possibility in vitro with isolated arterial smooth muscle preparations. Accordingly, we tested gemfibrozil which is resistant to photodegradation. We examined it over a therapeutically-relevant range (50-400 μM) for both acute and delayed relaxant effects on contractions of the isolated rat tail artery; contractions induced by either depolarizing its smooth muscle cell membranes with high potassium or stimulating its membrane-bound receptors with norepinephrine and arginine-vasopressin. We also examined these same gemfibrozil levels for effects on spontaneously-occurring phasic rhythmic contractile activity, typically not seen in arteries under in vitro conditions but commonly exhibited by smooth muscle of uterus, duodenum and bladder. We found that gemfibrozil significantly relaxed all induced forms of contraction in the rat tail artery, acutely at the higher test levels and after a delay of a few hours at the lower test levels. The highest test level of gemfibrozil (400 μM) also completely abolished spontaneously-occurring contractile activity of the isolated uterus and duodenum and markedly suppressed it in the bladder. This is the first evidence that a fibrate drug can directly relax smooth muscle contractions, either induced by various contractile agents or spontaneously-occurring. These findings are particularly relevant to both the recently renewed concern over the impact of fibrates on hypertension and a new understanding of their gastrointestinal side effects.

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Section: Effects Of Gemfibrozil On Spontaneous Contractions Of Rat Utmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Evidence of direct smooth muscle relaxant effects of the fibrate gemfibrozil

Phelps

Peuler

2010

J. Smooth Muscle Res.

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“…Urinary bladder contractility is also modulated by K ϩ efflux through SK channels (27,33,35), which contribute to the afterhyperpolarization of the urinary bladder smooth muscle action potential (12,21); blocking SK channels results in an increase in detrusor SPCs (9,27,33,35). To determine whether SK channel activity, like BK channel activity, was different between mucosal and detrusor myocytes, we first compared the effects of the SK channel blocker apamin (300 nM) on mucosal and detrusor smooth muscle SPCs.…”

Section: R358mentioning

confidence: 99%

“…Given the prominent role that BK channels play in regulating detrusor contractility (9,25,29,32,33,58,69), we sought to determine their role in the regulation of mucosal smooth muscle contractility. To assess the relative importance of BK channels in the regulation of mucosal smooth muscle SPCs, we tested the effects of the BK channel blocker IbTX (100 nM) on the SPCs of mucosal and detrusor tissue strips.…”

Section: R357mentioning

confidence: 99%

Unique properties of muscularis mucosae smooth muscle in guinea pig urinary bladder

Heppner¹,

Layne²,

Pearson³

et al. 2011

American Journal of Physiology-Regulatory, Integrative and Comp

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The muscularis mucosae, a type of smooth muscle located between the urothelium and the urinary bladder detrusor, has been described, although its properties and role in bladder function have not been characterized. Here, using mucosal tissue strips isolated from guinea pig urinary bladders, we identified spontaneous phasic contractions (SPCs) that appear to originate in the muscularis mucosae. This smooth muscle layer exhibited Ca 2ϩ waves and flashes, but localized Ca 2ϩ events (Ca 2ϩ sparks, purinergic receptor-mediated transients) were not detected. Ca 2ϩ flashes, often in bursts, occurred with a frequency (ϳ5.7/min) similar to that of SPCs (ϳ4/min), suggesting that SPCs are triggered by bursts of Ca 2ϩ flashes. The force generated by a single mucosal SPC represented the maximal force of the strip, whereas a single detrusor SPC was ϳ3% of maximal force of the detrusor strip. Electrical field stimulation (0.5-50 Hz) evoked force transients in isolated detrusor and mucosal strips. Inhibition of cholinergic receptors significantly decreased force in detrusor and mucosal strips (at higher frequencies). Concurrent inhibition of purinergic and cholinergic receptors nearly abolished evoked responses in detrusor and mucosae. Mucosal SPCs were unaffected by blocking smallconductance Ca 2ϩ -activated K ϩ (SK) channels with apamin and were unchanged by blocking large-conductance Ca 2ϩ -activated K ϩ (BK) channels with iberiotoxin (IbTX), indicating that SK and BK channels play a much smaller role in regulating muscularis mucosae SPCs than they do in regulating detrusor SPCs. Consistent with this, BK channel current density in myocytes from muscularis mucosae was ϳ20% of that in detrusor myocytes. These findings indicate that the muscularis mucosae in guinea pig represents a second smooth muscle compartment that is physiologically and pharmacologically distinct from the detrusor and may contribute to the overall contractile properties of the urinary bladder. calcium imaging; large-conductance calcium-activated potassium channel; potassium channels; calcium flashes; spontaneous phasic contractions THE URINARY BLADDER is a hollow, muscular organ that serves two functions: urine storage and elimination. The bladder wall is composed of detrusor smooth muscle, which accounts for a large fraction of the bladder mass, and a layer of transitional epithelial cells known as the urothelium, which lines the luminal surface of the urinary bladder. The detrusor smooth muscle has been extensively characterized and is clearly responsible for the majority of the contractile properties of the urinary bladder (1, 69). The urothelium, which was originally thought to simply act as a passive, impermeable barrier that prevents the movement of solutes from the urine into the bloodstream, is now recognized to possess a broad range of sensory and signal transduction functions that greatly influence bladder physiology (for a review, see Ref. 5).The detrusor exhibits two primary modes of contractile behavior: nerve-evoked contractions and spontaneo...

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“…As previously reported (Buckner et al, 2002), spontaneous phasic activity was observed in many tissues that contracted with transient spikes that varied in frequency, duration, and amplitude. The tissue strips were exposed to varying concentrations of the test agents for 15 min and changes in contractility were assessed.…”

Section: Pig Bladder Relaxation Studiesmentioning

confidence: 55%