Literature DB >> 8568853

Volume-activated chloride currents in pancreatic duct cells.

B Verdon1, J P Winpenny, K J Whitfield, B E Argent, M A Gray.   

Abstract

We have used the patch clamp technique to study volume-activated Cl- currents in the bicarbonate-secreting pancreatic duct cell. These currents could be elicited by a hypertonic pipette solution (osmotic gradient 20 mOsm/l), developed over about 8 min to a peak value of 91 +/- 5.8 pA/pF at 60 mV (n = 123), and were inhibited by a hypertonic bath solution. The proportion of cells which developed currents increased from 15% in freshly isolated ducts to 93% if the ducts were cultured for 2 days. The currents were ATP-dependent, had an outwardly rectifying current/voltage (I-V) plot, and displayed time-dependent inactivation at depolarizing potentials. The anion selectivity sequence was: ClO4 = I = SCN > Br = NO3 > Cl > F > HCO3 > gluconate, and the currents were inhibited to a variable extent by DIDS, NPPB, dideoxyforskolin, tamoxifen, verapamil and quinine. Increasing the intracellular Ca2+ buffering capacity, or lowering the extracellular Ca2+ concentration, reduced the proportion of duct cells which developed currents. However, removal of extracellular Ca2+ once the currents had developed was without effect. Inhibiting protein kinase C (PKC) with either the pseudosubstrate PKC (19-36), calphostin C or staurosporine completely blocked development of the currents. We speculate that cell swelling causes Ca2+ influx which activates PKC which in turn either phosphorylates the Cl- channel or a regulatory protein leading to channel activation.

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Year:  1995        PMID: 8568853     DOI: 10.1007/bf00233545

Source DB:  PubMed          Journal:  J Membr Biol        ISSN: 0022-2631            Impact factor:   1.843


  41 in total

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2.  A calcium-permeable stretch-activated cation channel in renal proximal tubule.

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Review 4.  Biochemistry of multidrug resistance mediated by the multidrug transporter.

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5.  Effect of protein kinase C inhibitors on Cl- conductance required for volume regulation after L-alanine cotransport.

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Journal:  Am J Physiol       Date:  1992-04

6.  cAMP-regulated whole cell chloride currents in pancreatic duct cells.

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8.  Volume-activated chloride channels in HeLa cells are blocked by verapamil and dideoxyforskolin.

Authors:  M Díaz; M A Valverde; C F Higgins; C Rucăreanu; F V Sepúlveda
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9.  Differential effects of tamoxifen and I- on three distinguishable chloride currents activated in T84 intestinal cells.

Authors:  M A Valverde; G M Mintenig; F V Sepúlveda
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10.  Protein kinase C-mediated phosphorylation of the human multidrug resistance P-glycoprotein regulates cell volume-activated chloride channels.

Authors:  S P Hardy; H R Goodfellow; M A Valverde; D R Gill; V Sepúlveda; C F Higgins
Journal:  EMBO J       Date:  1995-01-03       Impact factor: 11.598

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  17 in total

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4.  Potent block of volume-activated chloride currents in endothelial cells by the uncharged form of quinine and quinidine.

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Journal:  Br J Pharmacol       Date:  1996-08       Impact factor: 8.739

5.  Regulation of bradykinin-induced activation of volume-sensitive outwardly rectifying anion channels by Ca2+ nanodomains in mouse astrocytes.

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6.  Autocrine signaling through ATP release represents a novel mechanism for cell volume regulation.

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Review 7.  The role of swelling-induced anion channels during neuronal volume regulation.

Authors:  S Basavappa; J C Ellory
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8.  Human cervical cancer cells use Ca2+ signalling, protein tyrosine phosphorylation and MAP kinase in regulatory volume decrease.

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9.  Non-pore lining amino acid side chains influence anion selectivity of the human CFTR Cl- channel expressed in mammalian cell lines.

Authors:  P Linsdell; S X Zheng; J W Hanrahan
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10.  Characterization of cell volume-sensitive chloride currents in freshly prepared and cultured pancreatic acinar cells from early postnatal rats.

Authors:  A Schmid; R Blum; E Krause
Journal:  J Physiol       Date:  1998-12-01       Impact factor: 5.182

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