Facial Pain Clinical Trial
Official title:
In Vivo Selectivity of Cyclooxygenase Inhibitors in the Oral Surgery Model
This study will evaluate the effects of the new anti-inflammatory drug, Celebrex, on
relieving pain after oral surgery. It is also designed to assess the drug's selective
inhibition of a chemical called cyclooxygenase-2 and not its closely related form,
cyclooxygenase-1. This selective inhibition allows pain alleviation without the adverse side
effects (e.g., bleeding and stomach upset) often associated with anti-inflammatory drugs.
Healthy volunteers who require removal of their third molars are eligible for this study.
Participants will have oral surgery for tooth extraction after receiving a local anesthetic
(lidocaine) in the mouth and a sedative (midazolam) through an arm vein. On the evening
before and 1 hour before surgery, patients will be given a dose of either the standard
anti-inflammatory drug ibuprofen (Advil, Nuprin, Motrin), or Celebrex, or a placebo (a pill
with no active ingredient). After surgery, a small piece of tubing will be placed in each
extraction site and tied to an adjacent tooth to hold it in place. Samples will be collected
from the tubing to measure chemicals involved in pain and inflammation. Patients will stay
in the clinic for up to 6 hours after surgery while the anesthetic wears off and will
complete pain questionnaires. During that time, they may receive acetaminophen plus codeine
(Tylenol 3), if needed, for pain. The tubing then will be removed and the patient discharged
with standard pain medication.
Prostanoids are mediators that have been implicated in all stages of inflammation. The
inhibition of prostanoid synthesis by NSAIDs forms the basis of their therapeutic as well as
side effects. NSAIDs directly inhibit cyclooxygenase [COX], which leads to reduction of
prostaglandin synthesis and also to gastric erosions, inhibition of platelet aggregation and
nephrotoxicity. The identification of the two isoforms of COX lead to the hypothesis that
COX-2 is responsible for the production of prostaglandins following tissue injury, while
COX-1 is involved in normal homeostasis.
The selective COX-2 inhibitors are believed to be efficacious anti-inflammatory drugs devoid
of the side effects associated with the inhibition of COX-1. However, the selectivity of
these drugs has only been demonstrated in vitro and ex vivo, which may not be a reliable
indicator of the in vivo selectivity. The proposed study aims to evaluate the in vivo
selectivity of celecoxib, a drug demonstrated to be a selective inhibitor of COX-2 in vitro
in the oral surgery model of acute inflammation.
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Endpoint Classification: Safety/Efficacy Study, Primary Purpose: Treatment
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