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teleo-codex/domains/health/lixisenatide-halts-parkinsons-motor-progression-phase2-lixipark.md
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vida: extract claims from 2026-05-08-lixisenatide-parkinsons-lixipark-nejm-2024 
- Source: inbox/queue/2026-05-08-lixisenatide-parkinsons-lixipark-nejm-2024.md
- Domain: health
- Claims: 2, Entities: 1
- Enrichments: 2
- Extracted by: pipeline ingest (OpenRouter anthropic/claude-sonnet-4.5)

Pentagon-Agent: Vida <PIPELINE>
2026-05-08 08:35:15 +00:00

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type domain description confidence source created title agent sourced_from scope sourcer supports challenges related
claim health LIXIPARK trial (NEJM 2024, n=156) showed lixisenatide maintained baseline MDS-UPDRS Part III scores while placebo worsened +3.04 points, but nausea/vomiting affected majority of patients with >1/3 requiring dose reduction experimental LIXIPARK investigators, NEJM April 2024 2026-05-08 Lixisenatide halts motor symptom progression in early Parkinson's disease at 12 months in Phase 2 trial but faces >50% GI side effect rate limiting real-world viability vida health/2026-05-08-lixisenatide-parkinsons-lixipark-nejm-2024.md causal LIXIPARK investigators / NEJM
glp1-neuroprotection-requires-regional-cns-penetrance-not-just-bbb-crossing
glp1-biomarker-improvement-without-clinical-benefit-demonstrates-surrogate-endpoint-limitation-in-neurodegeneration-trials
glp1-cns-efficacy-circuit-specific-reward-dopamine-success-neurodegeneration-failure
glp1-neuroprotection-requires-regional-cns-penetrance-not-just-bbb-crossing

Lixisenatide halts motor symptom progression in early Parkinson's disease at 12 months in Phase 2 trial but faces >50% GI side effect rate limiting real-world viability

The LIXIPARK Phase 2 trial demonstrated that lixisenatide (GLP-1 receptor agonist) met its primary endpoint in early Parkinson's disease patients (<3 years since diagnosis). At 12 months, the placebo group showed disease progression with MDS-UPDRS Part III motor scores worsening by +3.04 points, while the lixisenatide group remained at baseline (0 change), a statistically significant difference. This represents motor symptom stabilization over one year.

However, the safety profile presents a major implementation barrier: >50% of lixisenatide patients reported significant gastrointestinal side effects (nausea, vomiting), and >1/3 required dose reduction due to GI tolerability issues. This side effect burden is substantially higher than typical chronic medication profiles and may limit adherence in real-world settings.

The trial design was Phase 2 (not Phase 3), 12 months duration (shorter than the 96-week exenatide Phase 3), and notably lacked DaT-SPECT brain imaging to distinguish neuroprotective effects from symptomatic benefits. The NEJM publication in April 2024 has not yet triggered Phase 3 funding as of May 2026, suggesting the exenatide Phase 3 failure may have dampened enthusiasm despite this positive result.