Article

Spontaneous Ca2+ signaling of interstitial cells in the guinea pig prostate.

Medicinal Chemistry and Drug Action, Monash Institute of Pharmaceutical Sciences, Parkville, Victoria, Australia.
The Journal of urology (impact factor: 4.02). 12/2011; 186(6):2478-86. DOI:10.1016/j.juro.2011.07.082 pp.2478-86
Source: PubMed

ABSTRACT We investigated whether prostate interstitial cells generate spontaneous Ca(2+) oscillation, a proposed mechanism underlying pacemaker potentials to drive spontaneous activity in stromal smooth muscle cells.
Intracellular free Ca(2+) in portions of guinea pig prostate and freshly isolated, single prostate interstitial cells were visualized using fluo-4 Ca(2+) fluorescence. Spontaneous electrical activity was recorded in situ with intracellular microelectrodes.
In whole tissue preparations spontaneous Ca(2+) flashes firing synchronously across all smooth muscle cells within the field of view resulted in muscle wall contractions. Nonpropagating Ca(2+) waves were also recorded in individual smooth muscle cells. Nifedipine (Sigma®) (1 μM) largely decreased or abolished these Ca(2+) flashes and suppressed slow wave discharge upon blockade of their superimposed action potentials. Isolated prostate interstitial cells were readily distinguished from smooth muscle cells by their spiky processes and lack of contraction during intracellular Ca(2+) increases. Prostate interstitial cells generated spontaneous Ca(2+) transients in the form of whole cell flashes, intracellular Ca(2+) waves or localized Ca(2+) sparks. All 3 Ca(2+) signals were abolished by nicardipine (1 μM), cyclopiazonic acid (10 μM), caffeine (Sigma) (10 mM) or extracellular Ca(2+) removal.
Prostate interstitial cells generate spontaneous Ca(2+) transients that occur at a frequency comparable to Ca(2+) flashes in situ or slow waves relying on functional internal Ca(2+) stores. However, unlike other interstitial cells in the urinary tract, Ca(2+) influx through L-type Ca(2+) channels is fundamental to Ca(2+) transient firings in prostate interstitial cells. Thus, it is not possible to conclude that prostate interstitial cells are responsible for pacemaker potential generation.

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Keywords

extracellular Ca(2+)
 
functional internal Ca(2+)
 
guinea pig prostate
 
individual smooth muscle cells
 
interstitial cells
 
intracellular Ca(2+)
 
Intracellular free Ca(2+)
 
intracellular microelectrodes
 
muscle wall contractions
 
Nonpropagating Ca(2+)
 
pacemaker potentials
 
proposed mechanism
 
prostate interstitial cells
 
single prostate interstitial cells
 
slow waves
 
smooth muscle cells
 
spontaneous Ca(2+)
 
stromal smooth muscle cells
 
superimposed action potentials
 
whole tissue preparations spontaneous Ca(2+)