M J Turnbull scite author profile

The site of action of the antispastic drug baclofen has long been considered to reside in the spinal cord although supraspinal effects have also been reported. This beta-chlorophenyl derivative of the neurotransmitter gamma-aminobutyric acid (GABA) depresses both monosynaptic and polysynaptic transmission in the cord possibly through a decrease in transmitter release rather than by any antagonism at postsynaptic receptors. Recently, baclofen has been shown to be a selective ligand for a bicuculline-insensitive GABA receptor (GABAB) site that occurs widely in the mammalian central nervous system including the spinal cord. The apparent importance of the cord in the therapeutic effects of this drug prompted us to ask whether they involve GABAB site activation. As an initial step we have located these receptors by autoradiography, comparing them with classical GABAA sites. We report here that GABAB sites, unlike GABAA sites, are present in high concentrations in laminae I, II, III and IV of the dorsal horn and that after the neonatal administration of capsaicin this binding is reduced by 40-50%.

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Selective antagonists at the opiate delta-receptor

Shaw¹,

Miller²,

Turnbull³

et al. 1982

Life Sciences

174

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GABA receptor multiplicityVisualization of different receptor types in the mammalian CNS

et al. 1984

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M J Turnbull

(–)Baclofen decreases neurotransmitter release in the mammalian CNS by an action at a novel GABA receptor

Bicuculline-insensitive gaba receptors on peripheral autonomic nerve terminals

Are baclofen-sensitive GABAB receptors present on primary afferent terminals of the spinal cord?

Selective antagonists at the opiate delta-receptor

GABA receptor multiplicityVisualization of different receptor types in the mammalian CNS

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