Abstract

µ-Opioid receptors (MOR) are a major target of endogenous and exogenous opioids, including opioid pain medications. The µ-opioid neurotransmitter system is heavily implicated in the pathophysiology of chronic pain and opioid use disorder and, as such, central measures of µ-opioid system functioning are increasingly being considered as putative biomarkers for risk to misuse opioids. To explore the relationship between MOR system function and risk for opioid misuse, 28 subjects with chronic nonspecific back pain completed a clinically validated measure of opioid misuse risk, the Pain Medication Questionnaire (PMQ), and were subsequently separated into high (PMQ > 21) and low (PMQ ≤ 21) opioid misuse risk groups. Chronic pain patients along with 15 control participants underwent two separate [11C]-carfentanil positron emission tomography scans to explore MOR functional measures: one at baseline and one during a sustained pain-stress challenge, with the difference between the two providing an indirect measure of stress-induced endogenous opioid release. We found that chronic pain participants at high risk for opioid misuse displayed higher baseline MOR availability within the right amygdala relative to those at low risk. By contrast, patients at low risk for opioid misuse showed less pain-induced activation of MOR-mediated, endogenous opioid neurotransmission in the nucleus accumbens. This study links human in vivo MOR system functional measures to the development of addictive disorders and provides novel evidence that MORs and µ-opioid system responsivity may underlie risk to misuse opioids among chronic pain patients.

Highlights

  • Chronic pain is a serious, prevalent, worldwide health problem [1]

  • There were no significant differences in age between groups (F(2,40) = 2.7, p = 0.08)

  • A one-way ANOVA revealed significant group differences in ZKPQ-Sensation Seeking (F(2,37) = 4.19, p = 0.02) with Tukey’s posthoc comparisons indicating significantly higher ZKPQ-Sensation Seeking in Pain Medication Questionnaire (PMQ)-H compared to PMQ-L (p = 0.03), but only a trending toward significance when compared to the healthy controls (HC) group (p = 0.08)

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Summary

Introduction

Chronic pain is a serious, prevalent, worldwide health problem [1]. Opioids remain the frontline treatment for chronic pain conditions, contributing to what the Centers for Disease Control and Prevention have declared to be an opioid epidemic. In concert with a steady rise in prescription opioids, nonmedical use of these medications has increased, with opioids reportedly the most commonly abused drugs in the country [3]. In 2019, 9.7 million people (3.5%) aged 12 or older had misused prescription pain relievers in the past year [4]. Orthopedic pain (34.8%) was the primary reason for an opioid prescription, followed by dental conditions (17.3%), back pain (14.0%), and headache (12.9%) [5]. One-third of chronic pain patients endorse opioid misuse behaviors [6], but not every chronic pain patient prescribed opioids develops a problematic pattern of use. The processes which underlie enhanced misuse and addiction risk are not currently understood

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