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vida: extract claims from 2026-05-09-pmc12374370-glp1-parkinson-updated-meta-analysis-2025 
- Source: inbox/queue/2026-05-09-pmc12374370-glp1-parkinson-updated-meta-analysis-2025.md
- Domain: health
- Claims: 0, Entities: 1
- Enrichments: 2
- Extracted by: pipeline ingest (OpenRouter anthropic/claude-sonnet-4.5)

Pentagon-Agent: Vida <PIPELINE>
2026-05-09 04:19:54 +00:00

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type entity_type name full_name domain status
entity research_program MOST-ABLE Trial Oral Semaglutide for Parkinson's Disease Motor Symptoms Trial health active

MOST-ABLE Trial

Type: Phase 2/3 randomized controlled trial
Intervention: Oral semaglutide 7mg and 14mg daily
Population: n=99 patients with Parkinson's disease
Location: Japan
Primary Endpoint: Motor symptom improvement (MDS-UPDRS Part III)

Overview

MOST-ABLE is the first randomized controlled trial testing semaglutide specifically for Parkinson's disease motor symptoms. Unlike prior GLP-1 Parkinson's trials (exenatide, liraglutide, lixisenatide), this study uses oral semaglutide, which has a distinct CNS access mechanism via tanycytes targeting hypothalamus and brainstem regions.

Significance

The trial addresses a critical evidence gap: all prior GLP-1 Parkinson's RCTs used older GLP-1 agonists with different CNS penetrance profiles. Exenatide's Phase 3 failure (Lancet Feb 2025) revealed that blood-brain barrier crossing does not guarantee substantia nigra penetrance. Semaglutide's tanycyte-mediated CNS access may provide superior regional distribution, but this remains empirically unproven.

Timeline

  • 2024 — Protocol published, enrollment completed
  • Nov-Dec 2025 — Data collection completed
  • 2026 — Results expected (as of May 2026, publication pending)

Context

Meta-analysis of 5 prior GLP-1 Parkinson's RCTs (n=708) shows narrow motor benefit (MDS-UPDRS Part III -2.06, 95% CI -4.09 to -0.03) but no functional quality of life improvement. MOST-ABLE results will determine whether semaglutide's distinct CNS access mechanism translates to superior clinical efficacy.

Sources

  • PMC12374370 meta-analysis (Jan 2025)
  • Session 40 GLP-1 Parkinson's divergence analysis (May 2026)