Development of a pharmacodynamic biomarker of opioid antagonism in adolescents with eating disorders: Study protocol for the naltrexone neuroimaging randomized controlled trial (NN-RCT).

Creator(s)

Stephani L. Stancil, Children's Mercy Kansas CityFollow
Mariah E. Brewe, Children's Mercy Kansas CityFollow
John Tumberger, Children's Mercy HospitalFollow
Michael Bartkoski, Children's Mercy Kansas CityFollow
Anna Burns, Children's Mercy Kansas CityFollow
Hung-Wen Yeh, Children's Mercy HospitalFollow
Morgan G. Brucks
James Bartolotti
Michaela Voss
Jeffrey R. Strawn
Susan Abdel-Rahman
Ann M. Davis, Children's Mercy HospitalFollow
William M. Brooks
Laura E. Martin

Document Type

Article

Publication Date

5-2025

Identifier

DOI: 10.1016/j.cct.2025.107874

Abstract

Eating disorders (ED) affect 5 % of youth, are associated with reward system alterations, and lead to substantial morbidity. Naltrexone, an opioid antagonist, is used to treat ED behaviors such as binge eating and purging. However, not all patients respond, and the optimal dose is unknown. Neuroimaging may serve as a tool to detect drug response in the brain, acting as a pharmacodynamic biomarker to support therapeutic optimization. Currently, no pharmacodynamic biomarkers for psychopharmacology exist. Building on pilot work, we present the protocol for a randomized controlled trial to validate neuroimaging as a pharmacodynamic biomarker of opioid antagonism in adolescents with ED. Youth aged 13-21 years with binge/purge ED are randomized to receive a single dose of oral naltrexone and placebo in a double-blind using a crossover design with an interdose interval ≥ 2 weeks. Task-based functional neuroimaging detects reward pathway modulation 2 h post-dose. Blood and urine are collected over a model-informed time course. Response (primary outcome) is defined as naltrexone-related blood oxygenation-level dependent signal change (Δ%BOLD) in a priori reward regions of interest and secondary exposure outcomes are naltrexone C_max and AUC_0-∞. Cohen's d will determine Δ%BOLD effect size, and an exposure-response model will identify target exposure to guide future dosing. This study addresses a critical knowledge gap by developing a non-invasive pharmacodynamic biomarker for youth with ED, with future applications in quantitative pharmacology, precision dosing, and the development of novel therapeutics.

Journal Title

Contemp Clin Trials

Volume

152

First Page

107874

Last Page

107874

MeSH Keywords

Adolescent; Female; Humans; Male; Young Adult; Biomarkers; Brain; Cross-Over Studies; Double-Blind Method; Feeding and Eating Disorders; Functional Neuroimaging; Magnetic Resonance Imaging; Naltrexone; Narcotic Antagonists; Neuroimaging; Randomized Controlled Trials as Topic; Reward

PubMed ID

40043750

Keywords

Adolescents; Eating disorders; Naltrexone; Opioid antagonism; Pharmacodynamic biomarker; fMRI

Recommended Citation

Stancil SL, Brewe ME, Tumberger J, et al. Development of a pharmacodynamic biomarker of opioid antagonism in adolescents with eating disorders: Study protocol for the naltrexone neuroimaging randomized controlled trial (NN-RCT). Contemp Clin Trials. 2025;152:107874. doi:10.1016/j.cct.2025.107874