A binding site for nonsteroidal anti-inflammatory drugs in fatty acid amide hydrolase

Bertolacci, Laura; Romeo, Elisa; Veronesi, Marina; Magotti, Paola; Albani, Clara; Dionisi, Mauro; Lambruschini, Chiara; Scarpelli, Rita; Cavalli, Andrea; De Vivo, Marco; Piomelli, Daniele; Garau, Gianpiero

doi:10.1021/ja308733u

In addition to inhibiting the cyclooxygenase (COX)-mediated biosynthesis of prostanoids, various widely used nonsteroidal anti-inflammatory drugs (NSAIDs) enhance endocannabinoid signaling by blocking the anandamide-degrading membrane enzyme fatty acid amide hydrolase (FAAH). The X-ray structure of FAAH in complex with the NSAID carprofen, along with site-directed mutagenesis, enzyme activity assays, and NMR analysis, has revealed the molecular details of this interaction, providing information that may guide the design of dual FAAH-COX inhibitors with superior analgesic efficacy. © 2012 American Chemical Society.

A binding site for nonsteroidal anti-inflammatory drugs in fatty acid amide hydrolase

Bertolacci, Laura;Romeo, Elisa;Veronesi, Marina;Magotti, Paola;Albani, Clara;Dionisi, Mauro;Lambruschini, Chiara;Scarpelli, Rita;Cavalli, Andrea;De Vivo, Marco;Piomelli, Daniele;Garau, Gianpiero

2013-01-01

Abstract

In addition to inhibiting the cyclooxygenase (COX)-mediated biosynthesis of prostanoids, various widely used nonsteroidal anti-inflammatory drugs (NSAIDs) enhance endocannabinoid signaling by blocking the anandamide-degrading membrane enzyme fatty acid amide hydrolase (FAAH). The X-ray structure of FAAH in complex with the NSAID carprofen, along with site-directed mutagenesis, enzyme activity assays, and NMR analysis, has revealed the molecular details of this interaction, providing information that may guide the design of dual FAAH-COX inhibitors with superior analgesic efficacy. © 2012 American Chemical Society.