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The control of chloride conductance in rat parotid isolated acinar cells investigated by photorelease of caged compounds
Authors:Abdul A Hassoni  Peter T A Gray
Institution:(1) Department of Pharmacology, The School of Pharmacy, 29/39 Brunswick Square, WC1N 1AX London, UK;(2) Present address: Muscular Dystrophy Group Research Laboratories, School of Neurosciences, Newcastle General Hospital, University of Newcastle upon Tyne, NE46BE Newcastle upon Tyne, UK;(3) Present address: 52 Sudbourne Road, SW2 5AH London, UK
Abstract:The control of Cl conductance in rat parotid isolated acinar cells was studied by combined use of whole-cell recording and flash photolysis techniques. Cells were voltage-clamped either at a membrane potential of –40 mV or stepped between –85 mV and 0 mV. Bath-applied carbachol and noradrenaline evoked Cl current at –85 mV and K+ current at 0 mV. Similar current activations resulted from the photolytic release of either inositol trisphosphate (InsP 3) or Ca2+ by a brief near-UV flash. The peak amplitudes of the Cl conductance (at –85 mV), measured relative to the K+ conductance (at 0 mV), evoked by application of carbachol, noradrenaline or direct manipulation of cytosolic free calcium (Ca2+]i), were very similar, being 0.56±0.09 (mean±SEM,n=9), 0.52 ± 0.01 (n=7) and 0.46±0.06 (n=7). In contrast, the relative amplitude of the Cl conductance evoked by InsP3 was much larger: 1.49±0.24 (n=9). Neither bath application of isoprenaline nor photolysis of ldquocagedrdquo cAMP induced any detectable membrane current. The most probable interpretation of these results is that the observed activation of Cl conductance by agonists can be explained by the elevation of Ca2+]i alone. In addition, the present results provide further support for the previously reported suggestion that the Cl channels and the Ca2+-release sites are co-localised 10].
Keywords:Cl   conductance  Acinar cells  ldquoCagedgif" alt="ldquo" align="MIDDLE" BORDER="0">Cagedrdquo InsP 3" target="_blank">gif" alt="rdquo" align="MIDDLE" BORDER="0"> InsP 3  Nitr-5  Muscarinic receptor
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