Frequency‐dependent depression of inhibition in guinea‐pig neocortex in vitro by GABAB receptor feed‐back on GABA release.

Deisz, Rudolf A.; Prince, David A.

doi:10.1113/jphysiol.1989.sp017629

Cited by 330 publications

(239 citation statements)

References 62 publications

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“…In sUce preparations, GABA and other neurotransmitters have been shown to act presynaptically to produce frequency-dependent depression of IPSPs (Deisz & Prince, 1989) and EPSPs (Kang, 1995). Thus, depression observed at longer inter-stimulus intervals may be due to substances acting presynaptically to modulate the probability of release (Castro-Alamancos, 1997).…”

Section: The Decrementai Responsementioning

confidence: 99%

Input-specific effects of acetylcholine on sensory and intracortical evoked responses in the “barrel cortex” in vivo

2003

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Section: The Decrementai Responsementioning

confidence: 99%

Input-specific effects of acetylcholine on sensory and intracortical evoked responses in the “barrel cortex” in vivo

2003

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“…Thus the depression in the amplitude of the IPSCs observed with paired stimulation of neocortical GABAergic synapses (Deisz and Prince, 1989;Fleidervish and Gutnick, 1995;Thomson et al, 1996) could be explained, at least partially, by accumulation of receptors in desensitized states. It is important to note, however, that the effect of receptor desensitization during repetitive stimulation would be minimized if the GABA A receptors are not saturated during synaptic transmission.…”

Section: Functional Implicationsmentioning

confidence: 99%

Properties of GABA_AReceptors Underlying Inhibitory Synaptic Currents in Neocortical Pyramidal Neurons

Galarreta

Hestrin

1997

J. Neurosci.

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Rapid applications of GABA (from 10 M to 10 mM) to outsideout patches were used to study the role that the kinetic properties of GABA A receptors play in determining the time course of IPSCs in neocortical pyramidal neurons. Currents induced by rapid applications of brief (1 msec) pulses of GABA (1 mM) showed a biexponential decay phase that seems to involve the entry of GABA A receptors into desensitized states. This conclusion is based on the similar fast decay kinetics of the response to brief and prolonged pulses of GABA and on the correlation between the degree of paired-pulse depression and the decay rate of the currents induced by brief pulses.Under nonequilibrium conditions we found that the concentration-response curve of pyramidal GABA A receptors has an EC 50 of 185 M (GABA pulse of 1 msec). The decay time course of the patch currents in response to brief applications of GABA was insensitive to agonist concentrations at the range from 50 M to 10 mM. Faster decay rates were observed only in response to pulses of 10 M GABA. These data are compatible with the suggestion that briefer openings derive from a monoliganded state and that these are negligible when receptor activation is Ͼ2%. Assuming that GABA transients at neocortical synapses are fast, a several millimolar GABA concentration would be needed to saturate the postsynaptic GABA A receptors.

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“…In this respect, in the CA1 region of the hippocampus, physiological activation of postsynaptic GABA B receptors results in the late inhibitory postsynaptic potential (IPSP B ) (Dutar & Nicoll, 1998a;Soltesz et al, 1988;Otis et al, 1993;SolõÂ s & Nicoll, 1992) whereas activation of presynaptic GABA B receptors results in pairedpulse depression of synaptic inhibition (i.e. a GABA B autoreceptor e ect: Thompson & GaÈ hwiler, 1989;Deisz & Prince, 1989;Davies et al, 1990;Olpe et al, 1994) which causes paired-pulse widening of synaptic excitation (Nathan et al, 1990;Nathan & Lambert, 1991;Davies & Collingridge, 1996). By determining the IC 50 values for antagonism of the late IPSP, and comparing these with those for antagonism of paired-pulse widening of EPSPs for six structurally di erent GABA B receptor antagonists, we have attempted to address whether synaptically activated pre-and post-synaptic GABA B receptors at GABAergic synapses can be di erentiated pharmacologically.…”

mentioning

confidence: 99%

Comparison of antagonist potencies at pre‐ and post‐synaptic GABA_B receptors at inhibitory synapses in the CA1 region of the rat hippocampus

Pozza

Manuel

Steinmann

et al. 1999

British J Pharmacology

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1 Synaptic activation of g-aminobutyric acid (GABA) B receptors at GABA synapses causes (a) postsynaptic hyperpolarization mediating a slow inhibitory postsynaptic potential/current (IPSP/C) and (b) presynaptic inhibition of GABA release which depresses IPSPs and leads to paired-pulse widening of excitatory postsynaptic potentials (EPSPs). To address whether these e ects are mediated by pharmacologically identical receptors the e ects of six GABA B receptor antagonists of widely ranging potencies were tested against each response. 2 Monosynaptic IPSP B s were recorded in the presence of GABA A , AMPA/kainate and NMDA receptor antagonists. All GABA B receptor antagonists tested depressed the IPSP B with an IC 50 based rank order of potency of CGP556795CGP56433=CGP55845A=CGP524324CGP511764 CGP36742. 3 Paired-pulse EPSP widening was recorded as an index of paired-pulse depression of GABAmediated IPSP/Cs. A similar rank order of potency of antagonism of paired-pulse widening was observed to that for IPSP B inhibition. 4 Comparison of the IC 50 values for IPSP B inhibition and paired-pulse EPSP widening revealed a close correlation between the two e ects in that their IC 50 s lay within the 95% con®dence limits of a correlation line that described IC 50 values for inhibition of paired-pulse EPSP widening that were 7.3 times higher than those for IPSP B inhibition. 5 Using the compounds tested here it is not possible to assign di erent subtypes of GABA B receptor to pre-and post-synaptic loci at GABAergic synapses. However, 5 ± 10 fold higher concentrations of antagonist are required to block presynaptic as opposed to postsynaptic receptors when these are activated by synaptically released GABA.

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Frequency‐dependent depression of inhibition in guinea‐pig neocortex in vitro by GABAB receptor feed‐back on GABA release.

Cited by 330 publications

References 62 publications

Input-specific effects of acetylcholine on sensory and intracortical evoked responses in the “barrel cortex” in vivo

Input-specific effects of acetylcholine on sensory and intracortical evoked responses in the “barrel cortex” in vivo

Properties of GABA_AReceptors Underlying Inhibitory Synaptic Currents in Neocortical Pyramidal Neurons

Comparison of antagonist potencies at pre‐ and post‐synaptic GABA_B receptors at inhibitory synapses in the CA1 region of the rat hippocampus

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Frequency‐dependent depression of inhibition in guinea‐pig neocortex in vitro by GABAB receptor feed‐back on GABA release.

Cited by 330 publications

References 62 publications

Input-specific effects of acetylcholine on sensory and intracortical evoked responses in the “barrel cortex” in vivo

Input-specific effects of acetylcholine on sensory and intracortical evoked responses in the “barrel cortex” in vivo

Properties of GABAAReceptors Underlying Inhibitory Synaptic Currents in Neocortical Pyramidal Neurons

Comparison of antagonist potencies at pre‐ and post‐synaptic GABAB receptors at inhibitory synapses in the CA1 region of the rat hippocampus

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Properties of GABA_AReceptors Underlying Inhibitory Synaptic Currents in Neocortical Pyramidal Neurons

Comparison of antagonist potencies at pre‐ and post‐synaptic GABA_B receptors at inhibitory synapses in the CA1 region of the rat hippocampus