Healthy Clinical Trial
Official title:
Proinflammatory Gene Expression and Prostanoid Levels in a Clinical Model of Tissue Injury
This study will evaluate how well different medications work to relieve pain following third
molar (wisdom tooth) extraction. Scientists believe that hormone-like substances called
prostanoids contribute to pain following oral surgery. Prostanoids are produced by
cyclooxygenase (COX) enzymes. This study will examine how different medicines inhibit the
COX enzymes and reduce the amount of prostanoids, and thus the amount of inflammation and
pain. The study will also look at genetic factors involved in the production of prostanoids
and the response to pain medication. (Only the bottom two wisdom teeth are extracted for
this study. Patients whose top wisdom teeth also need to be removed will have those teeth
extracted, also free of charge, at least 2 weeks after the first surgery.)
Healthy normal volunteers between 16 and 35 years of age who are in general good health and
who require third molar extraction may be eligible for this study. Candidates are screened
with a medical history and oral examination, including dental x-rays as needed to confirm
the need for third molar removal.
On the morning of surgery, patients have blood drawn to obtain DNA for genetic study. Women
of childbearing age have a urine pregnancy test. One hour before surgery, patients receive a
dose of rofecoxib (Vioxx® (Registered Trademark)), acetaminophen (Tylenol® (Registered
Trademark)), or placebo (a pill with no active ingredient). A half-hour before surgery, they
receive either a standard painkiller called keterolac (Toradol® (Registered Trademark))) or
placebo through an arm vein. All patients also receive the sedative midazolam (Versed®
(Registered Trademark)), also through an arm vein, to induce drowsiness and a local
anesthetic (lidocaine) to numb the mouth. After the mouth is numbed, but before the wisdom
teeth are extracted, a biopsy (removal of a small piece of tissue) is conducted in the area
of the cheek next to the wisdom tooth.
After the surgery, a small piece of tubing is placed into both extraction sites. Every 20
minutes for the next 3 hours, inflammatory fluid is collected from the tubing to measure
chemicals that are believed to cause pain and swelling. Patients complete questionnaires
every 20 minutes to rate their pain. Those who still have pain an hour after surgery may
request and receive a "rescue drug" called tramadol (Ultram® (Registered Trademark)) for
pain relief. Patients remain in the clinic from 3 to 6 hours to monitor the effects of the
study drugs as the anesthetic wears off.
After surgery a second biopsy is done to measure any changes in the chemicals being produced
in response to the surgery. For this biopsy, patients are assigned to one of two groups -
one group has the second biopsy within 3 hours of surgery, before taking the rescue drug,
and the other group returns to the clinic the next morning for a biopsy 24 hours after
surgery. Patients in the second group leave the clinic after surgery with two pain
medications (tramadol and the study drug) and forms to record pain ratings at home. They are
permitted to take only the pain medications provided and only at certain times.
At the end of their participation in the study, all patients are given the pain medication
flurbiprofen (Ocufen® (Registered Trademark)) to take at home.
Two cyclooxygenase isozymes, COX-1 and -2, are known to catalyze the rate-limiting step of
prostaglandin synthesis and are the targets of nonsteroidal anti-inflammatory drugs.
Recently, the presence of a variant of COX-1, named COX-3, has been demonstrated that is
especially sensitive to acetaminophen and strongly expressed in brain tissue. The proposed
study will examine prostanoid suppression in the periphery by inhibition of COX-1, -2, and
-3, and evaluate the time course of expression of COX isoenzymes in terms of level of mRNA
and protein itself.
Subjects (N equals 88) will be healthy volunteers scheduled for the surgical removal of
impacted third molars. Using a double-blinded, randomized, parallel study design, subjects
will be allocated to one of four treatment groups and will be administered a dose of blinded
medication or placebo. One hour prior to oral surgery, rofecoxib 50 mg, acetaminophen 1000
mg or placebo in two groups will be administered orally. Half hour prior to surgery,
ketorolac 30 mg or placebo, will be administered intravenously. Microdialysis will be
performed with sample collection concurrent with pain report over the immediate
postoperative period of three hours, and the collected transudate will be analyzed by ELISA
to evaluate prostanoid (prostaglandin E2, thromboxane B2) production. Subjects within each
group will be further randomized to have a biopsy collected at baseline prior to surgery and
either at the time when a subject asks for rescue drug within 3 hours or at 24 hours
following surgery. The biopsies will be frozen in liquid nitrogen and assayed later by
RT-PCR for levels of COX-1, COX-2, or COX-3 mRNA, and by microarray for evaluation of change
in overall mRNA expression. A portion of the biopsy samples will be immunostained to reveal
the tissue-specific pattern of each COX isoenzymes expression within the inflammatory
tissue, and another part of the biopsy samples will be analyzed by Western blot to quantify
the amount of protein. Fifty ml of blood will be collected from all subjects, and the single
nucleotide polymorphisms (SNPs) in the genes regulated by inflammatory responses such as
COX-1, COX-2, PGE receptors (EPs), and microsomal PGE synthase (mPGES) genes, will be
analyzed to investigate the role of genetic factors in individual differences of drug
responses. The analgesic effect of the drugs will be assessed in the clinic every 20 minutes
for the first three hours after extractions, and on the next morning before taking any
medication using two pain intensity assessment instruments: a category scale, and a visual
analog scale (VAS).
We anticipate that non-selective COX inhibitor, the selective COX-2 inhibitor, and the
selective COX-3 inhibitor will differentially alter prostanoid production over the time
course evaluated, and that primary sensory neurons innervating in the inflammatory tissues
may differentially express COX isoenzymes that differ in sensitivity to prototypic NSAIDs,
coxibs, and acetaminophen. We also anticipate that several SNPs will contribute to the
individual differences in COX expression and drug responses, which has implications for
individual variation in pain, analgesic responses, and neuronal plasticity.
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Endpoint Classification: Safety/Efficacy Study, Primary Purpose: Treatment
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