TY - JOUR T1 - Phenotyping the Function of TRPV1-Expressing Sensory Neurons by Targeted Axonal Silencing JF - The Journal of Neuroscience JO - J. Neurosci. SP - 315 LP - 326 DO - 10.1523/JNEUROSCI.2804-12.2013 VL - 33 IS - 1 AU - Christian Brenneis AU - Katrin Kistner AU - Michelino Puopolo AU - David Segal AU - David Roberson AU - Marco Sisignano AU - Sandra Labocha AU - Nerea Ferreirós AU - Amanda Strominger AU - Enrique J. Cobos AU - Nader Ghasemlou AU - Gerd Geisslinger AU - Peter W. Reeh AU - Bruce P. Bean AU - Clifford J. Woolf Y1 - 2013/01/02 UR - http://www.jneurosci.org/content/33/1/315.abstract N2 - Specific somatosensations may be processed by different subsets of primary afferents. C-fibers expressing heat-sensitive TRPV1 channels are proposed, for example, to be heat but not mechanical pain detectors. To phenotype in rats the sensory function of TRPV1+ afferents, we rapidly and selectively silenced only their activity, by introducing the membrane-impermeant sodium channel blocker QX-314 into these axons via the TRPV1 channel pore. Using tandem mass spectrometry we show that upon activation with capsaicin, QX-314 selectively accumulates in the cytosol only of TRPV1-expressing cells, and not in control cells. Exposure to QX-314 and capsaicin induces in small DRG neurons a robust sodium current block within 30 s. In sciatic nerves, application of extracellular QX-314 with capsaicin persistently reduces C-fiber but not A-fiber compound action potentials and this effect does not occur in TRPV1−/− mice. Behavioral phenotyping after selectively silencing TRPV1+ sciatic nerve axons by perineural injections of QX-314 and capsaicin reveals deficits in heat and mechanical pressure but not pinprick or light touch perception. The response to intraplantar capsaicin is substantially reduced, as expected. During inflammation, silencing TRPV1+ axons abolishes heat, mechanical, and cold hyperalgesia but tactile and cold allodynia remain following peripheral nerve injury. These results indicate that TRPV1-expressing sensory neurons process particular thermal and mechanical somatosensations, and that the sensory channels activated by mechanical and cold stimuli to produce pain in naive/inflamed rats differ from those in animals after peripheral nerve injury. ER -