Cell-Specific Alternative Splicing Increases Calcium Channel Current Density in the Pain Pathway

Cell-Specific Alternative Splicing Increases Calcium Channel Current Density in the Pain Pathway

N-type calcium channels are critical for pain transduction. Inhibitors of these channels are powerful analgesics, but clinical use of current N-type blockers remains limited by undesirable actions in other regions of the nervous system. We now demonstrate that a unique splice isoform of the N-type c...

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Veröffentlicht in:Neuron (Cambridge, Mass.) Mass.), 2004-01, Vol.41 (1), p.127-138
Hauptverfasser: Bell, Thomas J, Thaler, Christopher, Castiglioni, Andrew J, Helton, Thomas D, Lipscombe, Diane
Format: Artikel
Sprache:eng
Schlagworte:
Alternative Splicing
Analgesics
Animals
Calcium Channels, L-Type - genetics
Calcium Channels, L-Type - metabolism
Calcium Channels, N-Type - metabolism
Capsaicin - pharmacology
Electric Conductivity
Enzymes
Exons
Ganglia, Spinal - drug effects
Ganglia, Spinal - metabolism
Neurons
Neurons - drug effects
Neurons - metabolism
Nociceptors - drug effects
Nociceptors - metabolism
Pain - genetics
Pain - physiopathology
Protein Isoforms - metabolism
Rats
Rats, Sprague-Dawley
Rodents
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Zusammenfassung:N-type calcium channels are critical for pain transduction. Inhibitors of these channels are powerful analgesics, but clinical use of current N-type blockers remains limited by undesirable actions in other regions of the nervous system. We now demonstrate that a unique splice isoform of the N-type channel is restricted exclusively to dorsal root ganglia. By a combination of functional and molecular analyses at the single-cell level, we show that the DRG-specific exon, e37a, is preferentially present in Ca V2.2 mRNAs expressed in neurons that contain nociceptive markers, VR1 and Na V1.8. Cell-specific inclusion of exon 37a correlates closely with significantly larger N-type currents in nociceptive neurons. This unique splice isoform of the N-type channel could represent a novel target for pain management.
ISSN:0896-6273
1097-4199
DOI:10.1016/S0896-6273(03)00801-8