| Literature DB >> 18337008 |
Narender R Gavva1, James J S Treanor, Andras Garami, Liang Fang, Sekhar Surapaneni, Anna Akrami, Francisco Alvarez, Annette Bak, Mary Darling, Anu Gore, Graham R Jang, James P Kesslak, Liyun Ni, Mark H Norman, Gabrielle Palluconi, Mark J Rose, Margaret Salfi, Edward Tan, Andrej A Romanovsky, Christopher Banfield, Gudarz Davar.
Abstract
The vanilloid receptor TRPV1 has been identified as a molecular target for the treatment of pain associated with inflammatory diseases and cancer. Hence, TRPV1 antagonists have been considered for therapeutic evaluation in such diseases. During Phase I clinical trials with AMG 517, a highly selective TRPV1 antagonist, we found that TRPV1 blockade elicited marked, but reversible, and generally plasma concentration-dependent hyperthermia. Similar to what was observed in rats, dogs, and monkeys, hyperthermia was attenuated after repeated dosing of AMG 517 (at the highest dose tested) in humans during a second Phase I trial. However, AMG 517 administered after molar extraction (a surgical cause of acute pain) elicited long-lasting hyperthermia with maximal body temperature surpassing 40 degrees C, suggesting that TRPV1 blockade elicits undesirable hyperthermia in susceptible individuals. Mechanisms of AMG 517-induced hyperthermia were then studied in rats. AMG 517 caused hyperthermia by inducing tail skin vasoconstriction and increasing thermogenesis, which suggests that TRPV1 regulates vasomotor tone and metabolic heat production. In conclusion, these results demonstrate that: (a) TRPV1-selective antagonists like AMG 517 cannot be developed for systemic use as stand alone agents for treatment of pain and other diseases, (b) individual susceptibility influences magnitude of hyperthermia observed after TRPV1 blockade, and (c) TRPV1 plays a pivotal role as a molecular regulator for body temperature in humans.Entities:
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Year: 2008 PMID: 18337008 DOI: 10.1016/j.pain.2008.01.024
Source DB: PubMed Journal: Pain ISSN: 0304-3959 Impact factor: 6.961