Irritable Bowel Syndrome Clinical Trial
Official title:
Characterization of Pain Processing Mechanisms in Irritable Bowel Syndrome
This study is being done to collect new information on irritable bowel syndrome, a disease
that causes abdominal pain that does get better with treatment or keeps coming back
("chronic"). To better understand what causes the irritable bowel syndrome, we are studying
drugs used to treat pain, dextromethorphan, naloxone, fentanyl, and lidocaine. We will study
the effects these drugs have on experimental pain.
Dextromethorphan is used in non-prescription cough syrups. Naloxone is used for reversing
the effects of narcotic pain relievers. Fentanyl is a narcotic used to treat pain and to
make a person relaxed (sedated) before anesthesia. The purpose of this study is to see what
kinds of pain are affected by these drugs in persons who have irritable bowel syndrome and
persons who do not have this problem.
Irritable Bowel Syndrome (IBS) is a common gastrointestinal disorder characterized by
chronic abdominal pain and altered bowel function (diarrhea and/or constipation) that
effects up to 20% of the United States population. Although the pathophysiology of IBS is
unknown, visceral hypersensitivity (i.e., decreased pain thresholds in response to gut
distension) is a biological marker of the disorder. The mechanisms that lead to visceral
hypersensitivity, however, are currently unknown. As a consequence of our current
VA-supported studies, our laboratory has acquired evidence that patients with IBS and
visceral hypersensitivity also have cutaneous hypersensitivity in response to experimental
thermal pain stimuli. These new findings differ from previous investigations that indicated
IBS-associated hypersensitivity is limited to the gut. Rather, our data suggest that
patients with IBS have alterations in central pain processing mechanisms that may represent
the underlying pathophysiological basis for visceral and cutaneous hypersensitivity. Based
on our preliminary data, we propose that alterations in spinal processing mechanisms are
similar in patients with IBS to those that have been described for patients with other
chronic pain disorders. Cutaneous hypersensitivity is also seen in other chronic pain
conditions such as fibromyalgia where altered central pain processing mechanisms have been
shown to be responsible for maintaining hypersensitivity. In our current proposal, we
hypothesize that IBS patients have increased peripheral and central afferent processing of
nociceptive cutaneous and visceral stimuli.
Our objectives are as follows:
- Specific Objective #1. To determine if lidocaine applied to the rectum decreases
visceral hyperalgesia, as tested by nociceptive rectal distension.
- Specific Objective #2. To determine if lidocaine applied to the rectum decreases
cutaneous heat hyperalgesia to test for the presence or absence of central hyperalgesia
in IBS patients.
- Specific Objective #3. To determine the relationships between doses of IV lidocaine,
serum levels of IV lidocaine, and their anti-hyperalgesic effects, as tested by rectal
distension and cutaneous heat stimulation.
Specific Objective #4. To determine the effect of rectal lidocaine on clinical pain and
clinical symptoms of IBS.
The proposed studies will test the central hypothesis using well-controlled sensory stimuli
designed to separately evaluate central and peripheral mechanisms. The objectives will be
accomplished by systematically applying and comparing pharmacological and psychophysical
studies to IBS patients and controls. This application is an extension of the principal
investigator's current VA Advanced Career Development Award that examines the neurobiology
of visceral hypersensitivity in Persian Gulf veterans who returned home with chronic
abdominal pain. The proposed Clinical Research Program will study afferent mechanisms of
visceral and cutaneous hypersensitivity in veterans with IBS. Our laboratory is uniquely
positioned to use our expertise in psychophysical and pharmacologic evaluation of patients
with fibromyalgia to study patients with IBS. The results of this current proposal will lead
to larger clinical trials with sodium-channel blockers (i.e., lidocaine, mexiletine) as
potential therapeutic agents for veterans with IBS.
;
Allocation: Randomized, Endpoint Classification: Pharmacokinetics/Dynamics Study, Intervention Model: Crossover Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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