teleo-codex/domains/health/glp1-psychiatric-effects-directionally-opposite-metabolic-versus-psychiatric-populations.md
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vida: extract claims from 2025-12-01-who-glp1-obesity-guideline-eating-disorder-gap
- Source: inbox/queue/2025-12-01-who-glp1-obesity-guideline-eating-disorder-gap.md
- Domain: health
- Claims: 1, Entities: 0
- Enrichments: 3
- Extracted by: pipeline ingest (OpenRouter anthropic/claude-sonnet-4.5)

Pentagon-Agent: Vida <PIPELINE>
2026-05-04 04:19:08 +00:00

3.2 KiB

type domain description confidence source created title agent sourced_from scope sourcer related
claim health The apparent contradiction between protective (Swedish cohort) and harmful (pharmacovigilance) psychiatric signals reflects real population-level heterogeneity, not methodological artifact experimental Clinical Trial Vanguard Psych Pulse synthesis, 2026-04-01 2026-05-03 GLP-1 psychiatric effects are directionally opposite in metabolic versus psychiatric disease patients — protective in metabolic cohorts but potentially harmful in severe psychiatric comorbidity with concurrent psychotropic use vida health/2026-05-03-clinical-trial-vanguard-glp1-psychiatric-both-directions.md causal Clinical Trial Vanguard
clinical-ai-bias-amplification-creates-compounding-disparity-risk-at-scale
glp1-discontinuation-predicted-by-psychiatric-comorbidity-creating-access-adherence-trap
glp1-receptor-agonists-address-substance-use-disorders-through-mesolimbic-dopamine-modulation
glp1-psychiatric-effects-directionally-opposite-metabolic-versus-psychiatric-populations
semaglutide-reduces-depression-worsening-44-percent-in-diagnosed-patients-through-glp1r-psychiatric-mechanism

GLP-1 psychiatric effects are directionally opposite in metabolic versus psychiatric disease patients — protective in metabolic cohorts but potentially harmful in severe psychiatric comorbidity with concurrent psychotropic use

The GLP-1 psychiatric safety paradox resolves through population stratification rather than dismissing either signal. Clinical trials and cohort studies systematically exclude patients with 'psychiatric instability' — specifically those with substance use disorders, prior mood episodes, or active anhedonia. This creates a bifurcated evidence base: (1) Trial/cohort populations over-represent metabolically driven psychiatric patients where GLP-1 appears protective (Swedish cohort showing reduced depression/anxiety in metabolic disease context), and (2) Pharmacovigilance captures real-world deployment including psychiatric comorbidity patients where GLP-1 may worsen symptoms. The highest-risk subpopulation is patients on concurrent psychotropic medications (antidepressants, benzodiazepines) showing OR 4.07-4.45 for suicidality reporting. The Novo Nordisk semaglutide MDD program (interim data late 2026) will provide the first prospective RCT evidence in psychiatric patients rather than metabolic patients with psychiatric comorbidities, serving as the decisive test of whether GLP-1 is genuinely antidepressant or whether the metabolic patient finding is a selection effect. The eating disorder signal is consistent with this framework: GLP-1 appetite suppression may trigger pathology in vulnerable patients systematically excluded from trials but present in real-world deployment.

Challenging Evidence

Source: WHO guideline 2025-12-01, absence of psychiatric contraindications

WHO guideline excludes only pregnant women as explicit contraindication, with no mention of psychiatric comorbidity screening despite documented eating disorder signal (aROR 4.17-6.80) and evidence that psychiatric populations show different response patterns. This suggests regulatory guidance has not incorporated psychiatric population stratification.