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Results of a pilot multi-center genotype-based randomized placebo-controlled trial of propranolol to reduce pain after major thermal burn injury
Journal article   Peer reviewed

Results of a pilot multi-center genotype-based randomized placebo-controlled trial of propranolol to reduce pain after major thermal burn injury

Danielle C Orrey, Omar I Halawa, Andrey V Bortsov, Jeffrey W Shupp, Samuel W Jones, Linwood R Haith, Janelle M Hoskins, Marion H Jordan, Shrikant I Bangdiwala, Brandon Roane, …
The Clinical journal of pain, Vol.31(1), pp.21-29
01/01/2015
DOI: 10.1097/AJP.0000000000000086
PMCID: PMC4260989
PMID: 25084070
url
https://www.ncbi.nlm.nih.gov/pmc/articles/4260989View
Open Access

Abstract

Background: Results of previous studies suggest that beta-adrenoreceptor activation may augment pain, and that beta-adrenoreceptor antagonists may be effective in reducing pain, particularly in individuals not homozygous for the catechol-O-methyltransferase (COMT) high-activity haplotype.

Materials and Methods: Consenting patients admitted for thermal burn injury at participating burn centers were genotyped; those who were not high-activity COMT homozygotes were randomized to propranolol 240 mg/d or placebo. Primary outcomes were study feasibility (consent rate, protocol completion rate) and pain scores on study days 5 to 19. Secondary outcomes assessed pain and posttraumatic stress disorder symptoms 6 weeks postinjury.

Results: Seventy-seven percent (61/79) of eligible patients were consented and genotyped, and 77% (47/61) were genotype eligible and randomized. Ninety-one percent (43/47) tolerated study drug and completed primary outcome assessments. In intention-to-treat and per-protocol analyses, patients randomized to propranolol had worse pain scores on study days 5 to 19.

Conclusions: Genotype-specific pain medication interventions are feasible in hospitalized burn patients. Propranolol is unlikely to be a useful analgesic during the first few weeks after burn injury.

propranolol burn randomized control trial catechol-O-methyltransferase

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