4.4 Article

Adolescents and Young Adults With Sickle Cell Disease Nociplastic Pain and Pain Catastrophizing as Predictors of Pain Interference and Opioid Consumption

期刊

CLINICAL JOURNAL OF PAIN
卷 39, 期 7, 页码 326-333

出版社

LIPPINCOTT WILLIAMS & WILKINS
DOI: 10.1097/AJP.0000000000001119

关键词

sickle cell disease; nociplastic pain; pain catastrophizing

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The objective of this study was to characterize nociceptive pain and pain catastrophizing among adolescents and young adults with sickle cell disease (SCD), and to determine whether these characterizations are associated with subsequent opioid consumption and pain interference. The results showed that nociceptive pain features increased the likelihood of opioid consumption and pain interference. Therefore, it is important to consider the impact of nociceptive pain features in managing pain in SCD patients.
Objectives:Some patients with sickle cell disease (SCD) have features of nociplastic pain. While research suggests that many patients with nociplastic pain consume more opioids due to opioid nonresponsiveness, little is known about the impact of nociplastic pain and pain catastrophizing on opioid consumption and pain interference among adolescents and young adults (AYA) with SCD. The purpose of this study was to (1) characterize nociplastic pain and pain catastrophizing among AYA with SCD, and (2) determine whether these characterizations are associated with subsequent opioid consumption and pain interference 1 month after characterization. Methods:Participants completed surveys characterizing nociplastic pain and catastrophizing at a routine clinic visit (baseline). Thereafter, participants received weekly text messages that included pain interference and opioid consumption surveys. Multipredictor 2-part models were used to evaluate the predictive relationships between baseline characterizations and subsequent pain interference, and opioid consumption. Results:Forty-eight AYA aged 14 to 35 completed baseline measures. Twenty-five percent of participants had scores suggestive of nociplastic pain. Greater nociplastic pain features significantly increased the odds of consuming opioids (odds ratio=1.2) and having greater interference from pain (odds ratio=1.46). Regression analyses found that greater baseline nociplastic pain characteristics were significantly associated with opioid consumption (& beta;=0.13) and pain interference (& beta;=0.061); whereas higher pain catastrophizing scores predicted less opioid consumption (& beta;=-0.03) and less pain interference (& beta;=-0.0007). Discussion:In this sample of AYA with SCD, features of nociplastic pain predicted higher subsequent opioid consumption and pain interference. Being aware of nociplastic pain features in patients with SCD may better guide individualized pain management.

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