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vida: extract claims from 2026-05-03-evoke-evoke-plus-semaglutide-alzheimers-phase3-failure
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- Source: inbox/queue/2026-05-03-evoke-evoke-plus-semaglutide-alzheimers-phase3-failure.md
- Domain: health
- Claims: 0, Entities: 1
- Enrichments: 3
- Extracted by: pipeline ingest (OpenRouter anthropic/claude-sonnet-4.5)

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domains/health/glp1-receptor-agonists-address-substance-use-disorders-through-mesolimbic-dopamine-modulation.md
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@ -74,3 +74,10 @@ First RCT evidence: 26-week trial of 108 AUD+obesity patients showed semaglutide
**Source:** Clinical Trial Vanguard 2026-04-01 **Source:** Clinical Trial Vanguard 2026-04-01
Concurrent psychotropic medication use (antidepressants, benzodiazepines) shows OR 4.07-4.45 for suicidality in GLP-1 users, suggesting the dopaminergic mechanism may interact adversely with psychiatric medications rather than uniformly benefiting substance use disorder patients. The protective AUD signal may be specific to metabolic disease + AUD comorbidity rather than primary psychiatric AUD. Concurrent psychotropic medication use (antidepressants, benzodiazepines) shows OR 4.07-4.45 for suicidality in GLP-1 users, suggesting the dopaminergic mechanism may interact adversely with psychiatric medications rather than uniformly benefiting substance use disorder patients. The protective AUD signal may be specific to metabolic disease + AUD comorbidity rather than primary psychiatric AUD.
## Extending Evidence
**Source:** The Lancet 2026, EVOKE/EVOKE+ Phase 3 failure
EVOKE/EVOKE+ Alzheimer's failure provides critical boundary evidence for GLP-1 CNS mechanism specificity. Semaglutide succeeds in addiction (VTA dopamine reward circuits) but fails in neurodegeneration (amyloid/tau pathways), demonstrating that GLP-1 receptor activation produces pathway-specific effects rather than broad neuroprotection. This supports the mesolimbic dopamine mechanism for addiction while ruling out generalized CNS benefit claims.

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# EVOKE/EVOKE+ Trials
**Type:** Phase 3 clinical trials
**Sponsor:** Novo Nordisk
**Intervention:** Oral semaglutide 14mg (flexible dose)
**Indication:** Early-stage symptomatic Alzheimer's disease (mild cognitive impairment or mild dementia with confirmed amyloid positivity)
**Status:** Failed (2026)
## Trial Design
- **Design:** Two parallel Phase 3, double-blind, placebo-controlled trials
- **Population:** n=3,808 total, ages 55-85
- **Duration:** 104 weeks primary endpoint, 156 weeks extended follow-up
- **Primary endpoints:** Cognitive and global decline measures
## Results
**Primary endpoints:** Not met in either trial. Semaglutide did not demonstrate superiority to placebo in slowing cognitive or global decline.
**Secondary endpoints:**
- No delay in time to progression to dementia (MCI subgroup, pooled analysis)
- **Biomarker findings:** Up to 10% reduction in CSF core AD biomarkers (amyloid, tau)
- Significant reductions in CSF neuroinflammation markers
- **Critical gap:** Biomarker improvements did not translate to clinical benefit
## Scientific Interpretation
The biomarker-clinical benefit dissociation suggests three possible explanations:
1. Dose insufficient to produce clinical effect despite biomarker change
2. Treatment window too late (early symptomatic disease already past intervention point)
3. Neuroinflammation/AD pathobiology not rate-limiting in this population
## Implications
**For GLP-1 CNS expansion:** Establishes mechanism specificity boundary. Semaglutide shows efficacy in addiction (VTA dopamine pathways) but not neurodegeneration (amyloid/tau pathways), indicating GLP-1 CNS effects are pathway-specific rather than universally neuroprotective.
**For Alzheimer's drug development:** Adds to evidence that biomarker improvement (even in core AD pathology markers) does not guarantee clinical benefit, raising questions about surrogate endpoint validity.
**For prevention vs. treatment:** May indicate GLP-1 has preventive rather than therapeutic value in neurodegeneration, requiring different trial design in at-risk populations.
## Timeline
- **2026-04-15** — Results published in The Lancet
- **2026-04** — Novo Nordisk announces discontinuation of 1-year extension periods for both trials
## Sources
- The Lancet (2026): "Efficacy and safety of oral semaglutide 14 mg (flexible dose) in early-stage symptomatic Alzheimer's disease (evoke and evoke+): two phase 3, randomised, placebo-controlled trials"
- Alzheimer's Drug Discovery Foundation analysis
- NeurologyLive coverage

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inbox/queue/2026-05-03-evoke-evoke-plus-semaglutide-alzheimers-phase3-failure.md → inbox/archive/health/2026-05-03-evoke-evoke-plus-semaglutide-alzheimers-phase3-failure.md
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@ -7,10 +7,13 @@ date: 2026-04-15
domain: health domain: health
secondary_domains: [] secondary_domains: []
format: research-article format: research-article
status: unprocessed status: processed
processed_by: vida
processed_date: 2026-05-03
priority: medium priority: medium
tags: [GLP-1, semaglutide, Alzheimers, neurodegeneration, Phase-3, clinical-failure, biomarker-gap, CNS] tags: [GLP-1, semaglutide, Alzheimers, neurodegeneration, Phase-3, clinical-failure, biomarker-gap, CNS]
intake_tier: research-task intake_tier: research-task
extraction_model: "anthropic/claude-sonnet-4.5"
--- ---
## Content ## Content