Silencing of vanilloid receptor TRPV1 by RNAi reduces neuropathic and visceral pain in vivo |
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Authors: | Christoph Thomas Grünweller Arnold Mika Joanna Schäfer Martin K-H Wade Erik J Weihe Eberhard Erdmann Volker A Frank Robert Gillen Clemens Kurreck Jens |
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Affiliation: | Research and Development, Grünenthal GmbH, Aachen, Germany. |
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Abstract: | RNA interference (RNAi) has proven to be a powerful technique to study the function of genes by producing knock-down phenotypes. Here, we report that intrathecal injection of an siRNA against the transient receptor potential vanilloid receptor 1 (TRPV1) reduced cold allodynia of mononeuropathic rats by more than 50% over a time period of approximately 5 days. A second siRNA targeted to a different region of the TRPV1 gene was employed and confirmed the analgesic action of a TRPV1 knock-down. Furthermore, siRNA treatment diminished spontaneous visceral pain behavior induced by capsaicin application to the rectum of mice. The analgesic effect of siRNA-mediated knockdown of TRPV1 in the visceral pain model was comparable to that of the low-molecular weight receptor antagonist BCTC. Our data demonstrate that TRPV1 antagonists, including TRPV1 siRNAs, have potential in the treatment of both, neuropathic and visceral pain. |
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Keywords: | BCTC Capsaicin Neuropathic pain RNA interference Small interfering RNA Vanilloid receptor Visceral pain |
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