Download MendeleyMechanisms of peroxisome proliferator activated receptor gamma regulation by non-steroidal anti-inflammatory drugs.
Puhl, A.C., Milton, F.A., Cvoro, A., Sieglaff, D.H., Campos, J.C., Bernardes, A., Filgueira, C.S., Lindemann, J.L., Deng, T., Neves, F.A., Polikarpov, I., Webb, P.(2015) Nucl Recept Signal 13: e004-e004
- PubMed: 26445566
- DOI: https://doi.org/10.1621/nrs.13004
- Primary Citation of Related Structures:
4XTA, 4XUH, 4XUM - PubMed Abstract:
Non-steroidal anti-inflammatory drugs (NSAIDs) display anti-inflammatory, antipyretic and analgesic properties by inhibiting cyclooxygenases and blocking prostaglandin production. Previous studies, however, suggested that some NSAIDs also modulate peroxisome proliferator activated receptors (PPARs), raising the possibility that such off target effects contribute to the spectrum of clinically relevant NSAID actions. In this study, we set out to understand how peroxisome proliferator activated receptor-¦Ã (PPAR¦Ã/PPARG) interacts with NSAIDs using X-ray crystallography and to relate ligand binding modes to effects on receptor activity. We find that several NSAIDs (sulindac sulfide, diclofenac, indomethacin and ibuprofen) bind PPAR¦Ã and modulate PPAR¦Ã activity at pharmacologically relevant concentrations. Diclofenac acts as a partial agonist and binds to the PPAR¦Ã ligand binding pocket (LBP) in typical partial agonist mode, near the ¦Â-sheets and helix 3. By contrast, two copies of indomethacin and sulindac sulfide bind the LBP and, in aggregate, these ligands engage in LBP contacts that resemble agonists. Accordingly, both compounds, and ibuprofen, act as strong partial agonists. Assessment of NSAID activities in PPAR¦Ã-dependent 3T3-L1 cells reveals that NSAIDs display adipogenic activities and exclusively regulate PPAR¦Ã-dependent target genes in a manner that is consistent with their observed binding modes. Further, PPAR¦Ã knockdown eliminates indomethacin activities at selected endogenous genes, confirming receptor-dependence of observed effects. We propose that it is important to consider how individual NSAIDs interact with PPAR¦Ã to understand their activities, and that it will be interesting to determine whether high dose NSAID therapies result in PPAR activation.
Organizational Affiliation:
Instituto de F¨ªsica de S?o Carlos, Universidade de S?o Paulo, Av. Trabalhador Saocarlense 400, S?o Carlos, SP, 13560-970, Brazil (ACP, JCLC, AB, IP).
