GABA(B) receptor phosphorylation regulates KCTD12-induced K(+) current desensitization

GABA(B) receptors assemble from GABA(B)1 and GABA(B2) subunits. GABA(B2) additionally associates with auxiliary KCTD subunits (named after their K(+) channel tetramerization-domain). GABA(B) receptors couple to heterotrimeric G–proteins and activate inwardly-rectifying K(+) channels through the βγ s...

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Detalles Bibliográficos
Autores principales: Adelfinger, Lisa, Turecek, Rostislav, Ivankova, Klara, Jensen, Anders A., Moss, Stephen J., Gassmann, Martin, Bettler, Bernhard
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2014
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4402209/
https://www.ncbi.nlm.nih.gov/pubmed/25065880
http://dx.doi.org/10.1016/j.bcp.2014.07.013
Descripción
Sumario:GABA(B) receptors assemble from GABA(B)1 and GABA(B2) subunits. GABA(B2) additionally associates with auxiliary KCTD subunits (named after their K(+) channel tetramerization-domain). GABA(B) receptors couple to heterotrimeric G–proteins and activate inwardly-rectifying K(+) channels through the βγ subunits released from the G-protein. Receptor-activated K(+) currents desensitize in the sustained presence of agonist to avoid excessive effects on neuronal activity. Desensitization of K(+) currents integrates distinct mechanistic underpinnings. GABA(B) receptor activity reduces protein kinase-A activity, which reduces phosphorylation of serine-892 in GABA(B2) and promotes receptor degradation. This form of desensitization operates on the time scale of several minutes to hours. A faster form of desensitization is induced by the auxiliary subunit KCTD12, which interferes with channel activation by binding to the G-protein βγ subunits. Here we show that the two mechanisms of desensitization influence each other. Serine-892 phosphorylation in heterologous cells rearranges KCTD12 at the receptor and slows KCTD12-induced desensitization. Likewise, protein kinase-A activation in hippocampal neurons slows fast desensitization of GABA(B) receptor-activated K(+) currents while protein kinase-A inhibition accelerates fast desensitization. Protein kinase-A fails to regulate fast desensitization in KCTD12 knock-out mice or knock-in mice with a serine-892 to alanine mutation, thus demonstrating that serine-892 phosphorylation regulates KCTD12-induced desensitization in vivo. Fast current desensitization is accelerated in hippocampal neurons carrying the serine-892 to alanine mutation, showing that tonic serine-892 phosphorylation normally limits KCTD12-induced desensitization. Tonic serine-892 phosphorylation is in turn promoted by assembly of receptors with KCTD12. This cross-regulation of serine-892 phosphorylation and KCTD12 activity sharpens the response during repeated receptor activation.

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