Complementary roles of murine NaV1.7, NaV1.8 and NaV1.9 in acute itch signalling

Acute pruritus occurs in various disorders. Despite severe repercussions on quality of life treatment options remain limited. Voltage-gated sodium channels (Na V ) are indispensable for transformation and propagation of sensory signals implicating them as drug targets. Here, Na V 1.7, 1.8 and 1.9 were compared for their contribution to itch by analysing Na V -specific knockout mice. Acute pruritus was induced by a comprehensive panel of pruritogens (C48/80, endothelin, 5-HT, chloroquine, histamine, lysophosphatidic acid, trypsin, SLIGRL, β-alanine, BAM8-22), and scratching was assessed using a magnet-based recording technology. We report an unexpected stimulus-dependent diversity in Na V channel-mediated itch signalling. Na V 1.7 −/− showed substantial scratch reduction mainly towards strong pruritogens. Na V 1.8 −/− impaired histamine and 5-HT-induced scratching while Na V 1.9 was involved in itch signalling towards 5-HT, C48/80 and SLIGRL. Furthermore, similar microfluorimetric calcium responses of sensory neurons and expression of itch-related TRP channels suggest no change in sensory transduction but in action potential transformation and conduction. The cumulative sum of scratching over all pruritogens confirmed a leading role of Na V 1.7 and indicated an overall contribution of Na V 1.9. Beside the proposed general role of Na V 1.7 and 1.9 in itch signalling, scrutiny of time courses suggested Na V 1.8 to sustain prolonged itching. Therefore, Na V 1.7 and 1.9 may represent targets in pruritus therapy.