The neural signature of methylphenidate-enhanced memory disruption in human drug addiction: a randomized clinical trial

Ahmet O. Ceceli
Sarah G. King
K. Rachel Drury
Natalie McClain
John Gray
Priyanthi S. Dassanayake
Jeffrey H. Newcorn
Daniela Schiller
Nelly Alia-Klein
Rita Z. Goldstein

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Abstract

Background

Drug-related memories can hinder abstinence goals in drug addiction. Promoting non-drug memories via ventromedial prefrontal cortex- (vmPFC) and amygdala-guided extinction yields mixed success. Post-retrieval extinction (RE) destabilizes and updates memories during reconsolidation, improving extinction. Supplementing RE, we tested methylphenidate (MPH), a dopamine-agonist that promotes PFC-dependent learning and memory in cocaine use disorder (CUD). In an Early Phase 1 double-blind randomized clinical trial using a within-subjects design, participants received oral MPH (20 mg) or placebo before the retrieval of some of the conditioned stimuli (i.e., reminded CS+ vs. non-reminded CS+) followed by extinction; lab-simulated drug-seeking was measured the following day.

Results

Lower vmPFC activity following non-reminded CS+ (standard extinction) under placebo replicated the putative impairments in CUD; separately, RE (trend) and MPH conditions recruited the vmPFC, and RE’s vmPFC-reliance correlated with drug-seeking only under placebo. Crucially, MPH-combined RE normalized cortico-limbic processing, bypassing the vmPFC and its amygdala connectivity.

Conclusions

Pharmacologically-enhanced drug memory modulation may inform intervention development for addiction recovery.

Version published to 10.1101/2025.04.29.25326658v1 on medRxiv
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