TY - JOUR
T1 - Obstruction enhances rho-kinase pathway and diminishes protein kinase C pathway in carbachol-induced calcium sensitization in contraction of α-toxin permeabilized guinea pig detrusor smooth muscle
AU - Shahab, Nouval
AU - Kajioka, Shunichi
AU - Takahashi-Yanaga, Fumi
AU - Onimaru, Mitsuho
AU - Matsuda, Miho
AU - Seki, Narihito
AU - Naito, Seiji
PY - 2012/4
Y1 - 2012/4
N2 - Aims We investigated the relative important role of rho kinase (ROK) and protein kinase C (PKC) pathways in carbachol (CCh)-induced Ca 2+ sensitization in α-toxin permeabilized Guinea pig detrusor smooth muscle (DSM) following bladder outlet obstruction (BOO). Methods Bladder outlet obstruction was created by placement of a silver jeweler's jump rings loosely round the urethro-vesical junction of Guinea pigs. Sham operated Guinea pig underwent a similar protocol without application of the ring and served as control. α-Toxin permeabilized DSM strips from control Guinea pigs and those subjected to 6-8 weeks of BOO were mounted horizontally for isometric force recording in 100μl relaxing solution on perspex block. The effect of ROK inhibitor (Y-27632) and PKC inhibitor (GF-109203X) on CCh-induced Ca 2+ sensitization was studied during sustained contraction. Permeabilized DSM strips were also stimulated by cumulative increase of Ca 2+ concentration compared to that in control in the presence and in the absence of sensitization-induced PKC activator, phorbol 12,13-dibutyrate. Results Ca 2+ sensitization-induced by CCh was greater in BOO compared to controls. This muscarinic agonist-induced Ca 2+ sensitization was inhibited by Y-27632 or GF-109203X. The inhibitory effect of Y-27632 (5μM) was greater while the inhibitory effect of GF-109203X (5μM) was smaller in BOO compared to that in controls. Phorbol 12,13-dibutyrate (1μM) markedly increased Ca 2+ sensitivity in controls but not in BOO. Conclusions Our findings provide the first evidence that BOO enhances the ROK pathway and diminishes the PKC pathway in CCh-induced Ca 2+ sensitization in contraction of permeabilized Guinea pig DSM and suggest that inhibitors of ROK might potentially relieve bladder dysfunction related to BOO.
AB - Aims We investigated the relative important role of rho kinase (ROK) and protein kinase C (PKC) pathways in carbachol (CCh)-induced Ca 2+ sensitization in α-toxin permeabilized Guinea pig detrusor smooth muscle (DSM) following bladder outlet obstruction (BOO). Methods Bladder outlet obstruction was created by placement of a silver jeweler's jump rings loosely round the urethro-vesical junction of Guinea pigs. Sham operated Guinea pig underwent a similar protocol without application of the ring and served as control. α-Toxin permeabilized DSM strips from control Guinea pigs and those subjected to 6-8 weeks of BOO were mounted horizontally for isometric force recording in 100μl relaxing solution on perspex block. The effect of ROK inhibitor (Y-27632) and PKC inhibitor (GF-109203X) on CCh-induced Ca 2+ sensitization was studied during sustained contraction. Permeabilized DSM strips were also stimulated by cumulative increase of Ca 2+ concentration compared to that in control in the presence and in the absence of sensitization-induced PKC activator, phorbol 12,13-dibutyrate. Results Ca 2+ sensitization-induced by CCh was greater in BOO compared to controls. This muscarinic agonist-induced Ca 2+ sensitization was inhibited by Y-27632 or GF-109203X. The inhibitory effect of Y-27632 (5μM) was greater while the inhibitory effect of GF-109203X (5μM) was smaller in BOO compared to that in controls. Phorbol 12,13-dibutyrate (1μM) markedly increased Ca 2+ sensitivity in controls but not in BOO. Conclusions Our findings provide the first evidence that BOO enhances the ROK pathway and diminishes the PKC pathway in CCh-induced Ca 2+ sensitization in contraction of permeabilized Guinea pig DSM and suggest that inhibitors of ROK might potentially relieve bladder dysfunction related to BOO.
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U2 - 10.1002/nau.21193
DO - 10.1002/nau.21193
M3 - Article
C2 - 22396250
AN - SCOPUS:84860222477
SN - 0733-2467
VL - 31
SP - 593
EP - 599
JO - Neurourology and Urodynamics
JF - Neurourology and Urodynamics
IS - 4
ER -