TREATING CONSTIPATION CAUSED BY PAIN MEDICINES
Pain medicines often
lead to constipation for patients seeking long-term pain relief, but an
investigational once-daily drug may help, according to study led by the
University of Michigan Health System
Globally,
approximately 28 million to 35 million, or nearly half, of patients taking
opioids for long-term pain develop constipation. Patients get sub-optimal
results from laxatives.
The
results of two pivotal Phase 3 studies -- KODIAC-4 and KODIAC-5 of naloxegol,
an investigational treatment for opioid-induced constipation (OIC) -- were
published online first in the New England Journal of Medicine.
A
25 mg dose of the investigational drug naloxegol safely increased bowel
movements among opioid-induced constipation sufferers, compared to a placebo,
and the effects were maintained over a 12-week treatment period.
"The
studies showed rapid and sustained improvement for these patients, without
compromising their pain management," says lead study author and gastroenterologist
William Chey, M.D., professor of internal medicine at the U-M Health System.
Naloxegol
is an investigational peripherally-acting mu-opioid receptor antagonist, which
has been specifically designed for the treatment of opioid-induced constipation
(OIC), a common and often debilitating side effect of prescription medicines
used to treat osteoarthritis and chronic back pain.
Opioids
play an important role in chronic pain relief by binding to mu-receptors in the
brain, blocking the brain's ability to perceive brain. But they also bind to
mu-receptors in the bowel, contributing to constipation.
Naloxegol
is designed to block the binding of opioids to receptors in the
gastrointestinal tract without impacting the opioid receptors in the brain.
The
Phase 3 studies enrolled 652 people in one trial and 700 in another. The
12-week, multicenter, randomized, double blind, placebo-controlled pivotal
trials evaluated 12.5 mg and 25 mg doses of naloxegol, once-daily.
The
most commonly reported adverse effects with naloxegol were abdominal pain,
diarrhea, nausea, vomiting, flatulence and appeared to be dose-ordered,
occurring more commonly in the 25 mg group.
Most
adverse events were mild to moderate in severity and occurred shortly after
initiation of naloxegol. There was one major cardiovascular adverse event in
the 25 mg treatment group, one in the 12.5 mg treatment group and two among
those in the placebo group.
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