Opioid-induced Hyperalgesia Clinical Trial
In the proposed study, we will build upon our previous studies validating and characterizing hyperalgesia in MM samples to explore it's underlying mechanism from a pharmacological perspective. Utilizing a double-blind, placebo-controlled designs, the proposed work will evaluate the ability of dextromethorphan , an N-methyl-D-aspartate (NMDA)-antagonists to diminish or reverse the opioid-induced hyperalgesia complicating the pain states suffered by MM patients. Specifically, in a sample of MM patients, dextromethorphan, theorized to interfere with the development of opioid-induced hyperalgesia will be evaluated for its ability to ameliorate or diminish the opioid-induced hyperalgesia in these patients as reflected by changes on pain threshold and tolerance to both cold-pressor and electrical pain, at peak and trough methadone blood levels. The results of this work will not only provide pharmacologic insight into the mechanisms underlying poor pain tolerance in this at-risk population, but also direction for the medical management of pain complicated by opioid-induced hyperalgesia.
Addressing the undertreatment of clinical pain has become a national priority, with a
central goal being to identify effective interventions for those subgroups of patients most
at risk for suffering unrelieved pain (NIH Program Announcement PA-01-115). In fact, the
undertreatment of pain was recently ruled a form of patient abuse with a California court
awarding one million dollars in damages to the family of such a patient. Novel data
accumulated by our investigative group has shown that patients maintained on the mu-opioid
agonist, methadone, for the treatment of addiction, are significantly hyperalgesic to
cold-pressor experimental pain as compared to normal controls. This diminished pain
tolerance, in addition to the contextual prohibitions associated with providing known opioid
addicts with opioid analgesics, makes them a population uniquely vulnerable to the
undertreatment of pain. Unfortunately, little is known about how to best manage the pain
suffered by the over 120,000 methadone-maintained (MM) patients in this country, in part
because the hyperalgesia they suffer appears to be akin to neuropathic pain and
opioid-induced.
In the proposed series of studies, the Principal Investigator (a first-time R01 applicant)
will build upon her previous studies validating and characterizing hyperalgesia in MM
samples to explore it's underlying mechanism from a pharmacological perspective. Utilizing
slightly different double-blind, placebo-controlled designs, the proposed work will evaluate
the ability of three classes of medication (N-methyl-D-aspartate (NMDA)-antagonists,
adjuvant anticonvulsant analgesics, and novel opioid analgesics) to diminish or reverse the
opioid-induced hyperalgesia complicating the pain states suffered by MM patients.
Specifically, in a sample of MM patients, (1) dextromethorphan, which interferes with the
development of opioid-induced hyperalgesia, (2) gabapentin, which has proven efficacy in
treating neuropathic pain, and (3) oxycodone, which has novel opioid activity, will each be
evaluated for its ability to ameliorate or diminish the opioid-induced hyperalgesia in these
patients as reflected by changes on pain threshold and tolerance to both cold-pressor and
electrical pain, at peak and trough methadone blood levels. The results of this work will
not only provide pharmacologic insight into the mechanisms underlying poor pain tolerance in
this at-risk population, but also direction for the medical management of pain complicated
by opioid-induced hyperalgesia.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Completed |
NCT01210079 -
Hyperalgesia in Methadone-Maintained Patients: Can it be Treated?
|
Phase 2 | |
| Completed |
NCT00246532 -
Opiate-Induced Tolerance & Hyperalgesia in Pain Patients
|
Phase 4 | |
| Completed |
NCT04059978 -
Pain Response to Cannabidiol in Opioid-induced Hyperalgesia, Acute Nociceptive Pain and Allodynia By Using a Model Mimicking Acute Pain in Healthy Adults
|
N/A |