Literature DB >> 6319623

Model of electroretinogram b-wave generation: a test of the K+ hypothesis.

E A Newman, L L Odette.   

Abstract

Generation of the electroretinogram b-wave is simulated with a computer model representing a dark-adapted amphibian retina. The simulation tests the K+ hypothesis of b-wave generation, which holds that b-wave currents arise from localized Müller cell depolarizations generated by light-evoked increases in extracellular K+ concentration, [K+]o. The model incorporates the following components and processes quantitatively: 1) two time-dependent K+ sources representing the light-evoked [K+]o increases in the inner and outer plexiform layers, 2) a time- and [K+]o-dependent K+ sink representing the [K+]o decrease in the rod inner segment layer, 3) diffusion of released K+ through extracellular space, 4) active K+ reuptake and passive K+ drift across the Müller cell membrane, 5) spatial variations in the tortuosity factor and the volume fraction of extracellular space, 6) an extraretinal shunt resistance. Müller cells are modeled with 1) cytoplasmic resistance, 2) spatial variations in membrane permeability to K+, and 3) a membrane potential specified by the Nernst equation and transmembrane current flow. For specified K+ source and sink densities, the model computes [K+]o variations in time and retinal depth. Based on these [K+]o distributions, Müller cell potentials, current source-density profiles, and intraretinal and transretinal voltages are calculated. Imposed [K+]o distributions similar to those seen experimentally during the b-wave lead to the generation of a transient b-wave response and to a prolonged Müller response in the model system. These response time courses arise because the b-wave is dominated by the short-lived distal [K+]o increase, while the Müller response primarily reflects the long-lived proximal [K+]o increase. Current source-density distributions and intraretinal voltage profiles that are generated by the model at the peak of the b-wave closely resemble experimental results. The model generates a realistic slow PIII potential in response to prolonged [K+]o decreases in the distal retina and reproduces the K+ ejection results of Yanagida and Tomita (50) accurately. Simulations also suggest that tissue damage caused by K+-selective micropipettes in experimental preparations can lead to an underestimation of the distal [K+]o increase. The simulations demonstrate that the spatiotemporal properties of intraretinal b-wave voltages and currents and Müller cell responses can be generated according to the K+ hypothesis: by passive Müller cell depolarization driven by variations in [K+]o.

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Year:  1984        PMID: 6319623     DOI: 10.1152/jn.1984.51.1.164

Source DB:  PubMed          Journal:  J Neurophysiol        ISSN: 0022-3077            Impact factor:   2.714


  40 in total

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2.  Oscillatory potentials as predictors to amplitude and peak time of the photopic b-wave of the human electroretinogram.

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3.  K(+)-evoked Müller cell depolarization generates b-wave of electroretinogram in toad retina.

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5.  Efficient K+ buffering by mammalian retinal glial cells is due to cooperation of specialized ion channels.

Authors:  B Nilius; A Reichenbach
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6.  Effect of excitatory amino acids and analogues on [3H]acetylcholine release from amacrine cells of the rabbit retina.

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Journal:  J Physiol       Date:  1985-09       Impact factor: 5.182

7.  Contribution of membrane-damaging toxins to Bacillus endophthalmitis pathogenesis.

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8.  Electrophysiological evaluation of visual loss in Müller cell sheen dystrophy.

Authors:  U Kellner; H Kraus; H Heimann; H Helbig; N Bornfeld; M H Foerster
Journal:  Br J Ophthalmol       Date:  1998-06       Impact factor: 4.638

9.  Possible role of amacrine cells in the generation of the mammalian ERG b-wave.

Authors:  I Gottlob; L Wündsch; R Pflug
Journal:  Doc Ophthalmol       Date:  1985-10-30       Impact factor: 2.379

10.  Thermal sweat lactate in cystic fibrosis and in normal children.

Authors:  N Fellmann; A Labbe; A M Gachon; J Coudert
Journal:  Eur J Appl Physiol Occup Physiol       Date:  1985
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