Literature DB >> 8748943

Generation of slow wave type action potentials in the mouse small intestine involves a non-L-type calcium channel.

J Malysz1, D Richardson, L Farraway, M O Christen, J D Huizinga.   

Abstract

Intrinsic electrical activities in various isolated segments of the mouse small intestine were recorded (i) to characterize action potential generation and (ii) to obtain a profile on the ion channels involved in initiating the slow wave type action potentials (slow waves). Gradients in slow wave frequency, resting membrane potential, and occurrence of spiking activity were found, with the proximal intestine exhibiting the highest frequency, the most hyperpolarized cell membrane, and the greatest occurrence of spikes. The slow waves were only partially sensitive to L-type calcium channel blockers. Nifedipine, verapamil, and pinaverium bromide abolished spikes that occurred on the plateau phase of the slow waves in all tissues. The activity that remained in the presence of L-type calcium channel blockers, the upstroke potential, retained a similar amplitude to the original slow wave and was of identical frequency. The upstroke potential was not sensitive to a reduction in extracellular chloride or to the sodium channel blockers tetrodotoxin and mexiletine. Abolishment of the Na+ gradient by removal of 120 mM extracellular Na+ reduced the upstroke potential frequency by 13 - 18% and its amplitude by 50 - 70% in the ileum. The amplitude was similarly reduced by Ni2+ (up to 5 mM), and by flufenamic acid (100 mu M), a nonspecific cation and chloride channel blocker. Gadolinium, a nonspecific blocker of cation and stretch-activated channels, had no effect. Throughout these pharmacological manipulations, a robust oscillation remained at 5 - 10 mV. This oscillation likely reflects pacemaker activity. It was rapidly abolished by removal of extracellular calcium but not affected by L-type calcium channel blockers. In summary, the mouse small intestine has been established as a model for research into slow wave generation and electrical pacemaker activity. The upstroke part of the slow wave has two components, the pacemaker component involves a non-L-type calcium channel.

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Year:  1995        PMID: 8748943     DOI: 10.1139/y95-208

Source DB:  PubMed          Journal:  Can J Physiol Pharmacol        ISSN: 0008-4212            Impact factor:   2.273


  14 in total

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Authors:  M F Klemm; B Exintaris; R J Lang
Journal:  J Physiol       Date:  1999-09-15       Impact factor: 5.182

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Authors:  G P Sergeant; M A Hollywood; K D McCloskey; K D Thornbury; N G McHale
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4.  Heterogeneous expression of transient outward currents in smooth muscle cells of the mouse small intestine.

Authors:  Jonathan C F Lee; Carlos Barajas-López; Jan D Huizinga
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5.  The bioelectrical basis and validity of gastrointestinal extracellular slow wave recordings.

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Journal:  J Physiol       Date:  1998-11-15       Impact factor: 5.182

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8.  Conditional genetic deletion of Ano1 in interstitial cells of Cajal impairs Ca2+ transients and slow waves in adult mouse small intestine.

Authors:  John Malysz; Simon J Gibbons; Siva A Saravanaperumal; Peng Du; Seth T Eisenman; Chike Cao; Uhtaek Oh; Dieter Saur; Sabine Klein; Tamas Ordog; Gianrico Farrugia
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9.  Voltage-dependent Ca Current Identified in Freshly Isolated Interstitial Cells of Cajal (ICC) of Guinea-pig Stomach.

Authors:  Young Chul Kim; Hikaru Suzuki; Wen-Xie Xu; Hikaru Hashitani; Woong Choi; Hyo-Yung Yun; Seon-Mee Park; Sei Jin Youn; Sang-Jeon Lee; Sang Jin Lee
Journal:  Korean J Physiol Pharmacol       Date:  2008-12-31       Impact factor: 2.016

10.  The alpha1H Ca2+ channel subunit is expressed in mouse jejunal interstitial cells of Cajal and myocytes.

Authors:  Simon J Gibbons; Peter R Strege; Sha Lei; Jaime L Roeder; Amelia Mazzone; Yijun Ou; Adam Rich; Gianrico Farrugia
Journal:  J Cell Mol Med       Date:  2008-12-24       Impact factor: 5.310

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