vida: extract claims from 2026-04-23-glp1-substance-use-disorder-33-trials
Some checks are pending
Mirror PR to Forgejo / mirror (pull_request) Waiting to run
Some checks are pending
Mirror PR to Forgejo / mirror (pull_request) Waiting to run
- Source: inbox/queue/2026-04-23-glp1-substance-use-disorder-33-trials.md - Domain: health - Claims: 1, Entities: 0 - Enrichments: 3 - Extracted by: pipeline ingest (OpenRouter anthropic/claude-sonnet-4.5) Pentagon-Agent: Vida <PIPELINE>
This commit is contained in:
Teleo Agents
parent
ce579d137c
commit
0a6fdf2b31
3 changed files with 30 additions and 1 deletions
|
|
@ -32,3 +32,10 @@ WHO's conditional recommendation acknowledges 'limited long-term evidence' and '
|
||||||
**Source:** Frontiers in Clinical Diabetes and Healthcare 2025 review
|
**Source:** Frontiers in Clinical Diabetes and Healthcare 2025 review
|
||||||
|
|
||||||
Exercise helps preserve muscle mass and sustain weight loss after GLP-1 cessation. The review states that stopping GLP-1 therapy alone leads to weight regain, but exercise provides a partial mitigation pathway. Future obesity management will likely prioritize integrated approaches (pharmacotherapy + lifestyle) rather than pharmacotherapy replacing lifestyle.
|
Exercise helps preserve muscle mass and sustain weight loss after GLP-1 cessation. The review states that stopping GLP-1 therapy alone leads to weight regain, but exercise provides a partial mitigation pathway. Future obesity management will likely prioritize integrated approaches (pharmacotherapy + lifestyle) rather than pharmacotherapy replacing lifestyle.
|
||||||
|
|
||||||
|
|
||||||
|
## Extending Evidence
|
||||||
|
|
||||||
|
**Source:** PubMed 41696398 systematic review, 33 SUD trials
|
||||||
|
|
||||||
|
The continuous treatment requirement extends beyond metabolic conditions to substance use disorders. The same mesolimbic dopamine circuits that mediate hedonic eating also underlie addiction, suggesting GLP-1s would require chronic administration for SUD just as they do for obesity. This creates a parallel chronic-use economic model for an entirely new therapeutic category.
|
||||||
|
|
|
||||||
|
|
@ -0,0 +1,19 @@
|
||||||
|
---
|
||||||
|
type: claim
|
||||||
|
domain: health
|
||||||
|
description: The same VTA dopamine mechanism underlying GLP-1 effects on hedonic eating extends to addiction pathways creating a potential pharmacological common denominator for reward dysregulation conditions
|
||||||
|
confidence: experimental
|
||||||
|
source: PubMed 41696398 systematic review, Qeadan et al. Addiction 2025, Harvard Gazette 2026
|
||||||
|
created: 2026-04-23
|
||||||
|
title: GLP-1 receptor agonists may address multiple substance use disorders through shared mesolimbic dopamine circuit modulation with 33 clinical trials underway across alcohol opioid nicotine and cocaine use
|
||||||
|
agent: vida
|
||||||
|
sourced_from: health/2026-04-23-glp1-substance-use-disorder-33-trials.md
|
||||||
|
scope: causal
|
||||||
|
sourcer: PubMed/ClinicalTrials.gov systematic review
|
||||||
|
challenges: ["medical care explains only 10-20 percent of health outcomes because behavioral social and genetic factors dominate as four independent methodologies confirm"]
|
||||||
|
related: ["glp-1-receptor-agonists-require-continuous-treatment-because-metabolic-benefits-reverse-within-28-52-weeks-of-discontinuation", "medical care explains only 10-20 percent of health outcomes because behavioral social and genetic factors dominate as four independent methodologies confirm"]
|
||||||
|
---
|
||||||
|
|
||||||
|
# GLP-1 receptor agonists may address multiple substance use disorders through shared mesolimbic dopamine circuit modulation with 33 clinical trials underway across alcohol opioid nicotine and cocaine use
|
||||||
|
|
||||||
|
A systematic review of ClinicalTrials.gov identified 33 registered trials examining GLP-1 receptor agonists for substance use disorders: 15 for alcohol use disorder, 9 for nicotine/tobacco, 4 for cocaine, 4 for opioid use disorder, and 1 for methamphetamine. The mechanistic basis is shared with obesity treatment: GLP-1 receptors are expressed in the mesolimbic dopamine system (VTA, nucleus accumbens, amygdala) that underlies both hedonic eating and substance addiction. Early clinical evidence supports this mechanism: an RCT showed low-dose semaglutide reduced laboratory alcohol self-administration, drinks per drinking day, and craving in people with AUD. Real-world analysis by Qeadan et al. found that among people with pre-existing SUD, GLP-1 users showed fewer ER visits, hospitalizations, and deaths related to substance use. Animal studies demonstrate GLP-1s lower self-administration of opioids (heroin, fentanyl, oxycodone) and reduce relapse-like behavior. The breadth of the trial pipeline—with semaglutide as the most studied agent (n=15 trials)—indicates this is being taken seriously as a paradigm shift for addiction medicine. However, most OUD data remains in animal models, and human trial results are not yet published. The field is 2-3 years from definitive clinical evidence, making this experimental rather than proven.
|
||||||
|
|
@ -7,9 +7,12 @@ date: 2025-01-01
|
||||||
domain: health
|
domain: health
|
||||||
secondary_domains: []
|
secondary_domains: []
|
||||||
format: systematic review + news synthesis
|
format: systematic review + news synthesis
|
||||||
status: unprocessed
|
status: processed
|
||||||
|
processed_by: vida
|
||||||
|
processed_date: 2026-04-23
|
||||||
priority: high
|
priority: high
|
||||||
tags: [glp-1, addiction, SUD, alcohol-use-disorder, opioid-use-disorder, substance-use, clinical-trials, dopamine, reward-circuitry, semaglutide]
|
tags: [glp-1, addiction, SUD, alcohol-use-disorder, opioid-use-disorder, substance-use, clinical-trials, dopamine, reward-circuitry, semaglutide]
|
||||||
|
extraction_model: "anthropic/claude-sonnet-4.5"
|
||||||
---
|
---
|
||||||
|
|
||||||
## Content
|
## Content
|
||||||
Loading…
Reference in a new issue