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teleo-codex/inbox/queue/2026-05-08-glp1-cocaine-use-disorder-phase2-recruiting-2025.md
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type title author url date domain secondary_domains format status priority tags intake_tier
source GLP-1 Cocaine Use Disorder: Two Phase 2 Trials Recruiting, No Completed RCT — Preclinical Signal Extraordinary withpower.com / Pharmacy Times / PharmacyTimes https://www.pharmacytimes.com/view/semaglutide-could-offer-potential-treatment-for-cocaine-use-disorder 2025-01-01 health
article unprocessed medium
GLP-1
cocaine use disorder
substance use disorder
semaglutide
Phase 2 trial
addiction medicine
CUD
research-task

Content

Background: The All of Us Research Program nested case-control study (Abegaz et al., Frontiers in Psychiatry, March 10, 2026) found GLP-1 users had 75% lower odds of cocaine use disorder (OR=0.25, 95% CI 0.160.40, n=9,296 in CUD cohort). This is an extraordinary observational signal — no existing pharmacotherapy or behavioral intervention has achieved equivalent effect sizes for CUD.

Current trial status (as of May 2026):

Trial 1: Semaglutide + CBT for Cocaine Use Disorder

  • Phase 2, recruiting
  • Eligibility: diagnosed cocaine use disorder + BMI ≥25
  • Design: semaglutide combined with cognitive behavioral therapy (CBT)
  • Primary objective: reduce cocaine cravings and use
  • Source: withpower.com/trial/phase-2-cocaine-related-disorders-10-2025

Trial 2: Semaglutide for Cocaine Use Disorder (HIV cohort)

  • Phase 2, recruiting
  • Eligibility: cocaine use disorder in adults with and without HIV
  • Design: semaglutide vs. placebo for safety and effectiveness
  • Special population: testing in HIV+ population (important given high CUD prevalence in HIV-infected individuals)
  • Source: withpower.com/trial/phase-2-human-immunodeficiency-virus-hiv-infections-2-2025

Preclinical evidence:

  • Semaglutide reduced cocaine-seeking behavior significantly in rats (University of Gothenburg / University of Pennsylvania collaboration)
  • Mechanism: GLP-1R agonism in VTA/NAcc suppresses dopamine reward response to cocaine

Case report:

  • 54-year-old CUD patient on semaglutide: significant reduction in cocaine cravings over 12 weeks (single case, not controlled)

Current pharmacotherapy for CUD:

  • No FDA-approved pharmacotherapy exists for cocaine use disorder — this is the highest-unmet-need SUD category
  • Behavioral interventions (CBT, contingency management) have NNT 6-8
  • GLP-1 observational signal (OR=0.25) would represent unprecedented efficacy if confirmed

Expected timeline: Phase 2 results likely 2027-2028. No completed human RCT as of May 2026.

Agent Notes

Why this matters: Cocaine use disorder (CUD) has NO FDA-approved pharmacotherapy. It is the most treatment-resistant major SUD. If GLP-1 achieves even 50% of the observational effect size (OR=0.25 → adjusted OR ~0.5), it would be the first effective pharmacotherapy in a category that has resisted treatment development for decades. This is a potential paradigm shift in addiction medicine — larger than the AUD findings, which at least had naltrexone as an existing option.

What surprised me: The HIV-specific trial (Trial 2) is smart design — CUD is extremely prevalent in HIV+ populations, and semaglutide's metabolic benefits would be doubly valuable there. The HIV trial provides a real-world justification for off-label use even before CUD-specific approval.

What I expected but didn't find: Any completed Phase 2 human RCT results. All results for CUD are observational (All of Us) or preclinical. The field is still in early clinical development. The All of Us OR=0.25 signal hasn't yet triggered the kind of rapid Phase 2 mobilization that AUD saw (SEMALCO trial published JAMA Psychiatry 2025 — there's no equivalent CUD paper yet).

KB connections:

  • The All of Us study (archived 2026-05-07) provides the observational foundation for this trail; this archive tracks the RCT status
  • Connects to the SUD evidence convergence finding from Session 39: three designs for AUD/SUD broadly, but zero completed RCTs specifically for CUD
  • Belief 2 relevance: CUD has historically been considered a "behavioral" disorder resistant to pharmacological intervention. If GLP-1 establishes efficacy, it expands the clinical medicine contribution meaningfully — but would likely still require CBT (as SEMALCO showed for AUD)

Extraction hints:

  • Status claim: "No GLP-1 Phase 2 RCT for cocaine use disorder has reported results as of May 2026 — two trials recruiting. The only human CUD evidence is observational (All of Us, OR=0.25). Phase 2 results expected 2027-2028." [Confidence: proven — this is a factual status claim]
  • No high-confidence efficacy claims yet — this should NOT be extracted as an efficacy claim

Context: Cocaine use disorder is the highest-unmet-need SUD category. Two Phase 2 trials recruiting as of early 2025. No completed results. This archive serves as a tracking record for the extractor to know: don't extract efficacy claims yet, revisit when trial results publish.

Curator Notes (structured handoff for extractor)

PRIMARY CONNECTION: GLP-1 receptor agonists reduce substance use disorder risk by 40-75% (if this claim exists or is proposed from Session 39 sources) WHY ARCHIVED: Tracking the CUD trial status so future Vida sessions know exactly where the evidence stands — no completed RCT, two Phase 2 recruiting, check back 2027. EXTRACTION HINT: Do NOT extract efficacy claims. Extract only: (1) the status fact that no pharmacotherapy exists for CUD and (2) the trial pipeline status. The All of Us OR=0.25 should be cited as the observational basis, with confidence flagged as experimental pending RCT.