4.4 Article

Effect of depolarizing GABAA-mediated membrane responses on excitability of Cajal-Retzius cells in the immature rat neocortex

Journal

JOURNAL OF NEUROPHYSIOLOGY
Volume 106, Issue 4, Pages 2034-2044

Publisher

AMER PHYSIOLOGICAL SOC
DOI: 10.1152/jn.00699.2010

Keywords

cortical development; shunting inhibition; intracellular chloride concentration; rheobase

Funding

  1. Deutsche Forschungsgemeinschaft (DFG) [Ki 835/2]

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Kolbaev SN, Achilles K, Luhmann HJ, Kilb W. Effect of depolarizing GABA(A)-mediated membrane responses on excitability of Cajal-Retzius cells in the immature rat neocortex. J Neurophysiol 106: 2034-2044, 2011. First published July 20, 2011; doi:10.1152/jn.00699.2010.-In immature neurons activation of ionotropic GABA receptors induces depolarizing membrane responses due to a high intracellular Cl- concentration ([Cl-](i)). However, it is difficult to draw conclusions about the functional consequences of subthreshold GABAergic depolarizations, since GABAergic membrane shunting and additional effects on voltage-dependent ion channels or action potential threshold must be considered. To systematically investigate factors that determine the GABAergic effect on neuronal excitability we performed whole cell patch-clamp recordings from Cajal-Retzius cells in immature rat neocortex, using [Cl-](i) between 10 and 50 mM. The effect of focal GABA application was quantified by measuring various parameters of GABAergic responses including the shift in minimal threshold current (rheobase). The rheobase shift was correlated with other parameters of the GABAergic responses by multiple linear regression analyses with a set of simple mathematical models. Our experiments demonstrate that focal GABA application induces heterogeneous rheobase shifts in Cajal-Retzius cells that could not be predicted reliably from [Cl-](i) or the GABAergic membrane depolarization. Implementation of a linear mathematical model, which takes the GABAergic membrane conductance and the difference between action potential threshold and GABA reversal potential into account, resulted in a close correlation between calculated and experimentally obtained rheobase shifts. Addition of a linear term proportional to the GABAergic membrane depolarization improved the accuracy of correlation. The main advantage of using multiple linear regression with simple models is that direction and strength of GABAergic excitability shifts can be analyzed by using only measured parameters of GABAergic responses and with minimal a priori information about cellular parameters.

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