--- type: entity entity_type: research_program name: Exenatide-PD3 Trial domain: health status: completed --- # Exenatide-PD3 Trial **Type:** Phase 3 randomized controlled trial **Drug:** Exenatide (GLP-1 receptor agonist) **Indication:** Parkinson's disease (disease-modifying therapy) **Design:** Multicenter, double-blind, placebo-controlled, n=194, 96 weeks **Sites:** 6 UK research hospitals **Funding:** National Institute for Health and Care Research (NIHR) **Primary Endpoint:** Movement symptom progression (motor function) **Status:** Failed (February 2025) ## Overview Exenatide-PD3 was the largest and longest GLP-1 receptor agonist trial in Parkinson's disease to date. It tested whether exenatide once-weekly could slow disease progression by providing neuroprotection to dopaminergic neurons in the substantia nigra. ## Results **Primary endpoint:** FAILED — exenatide did not stop movement symptoms from worsening over 96 weeks versus placebo. **Secondary endpoints:** FAILED — no benefit in non-motor symptoms (quality of life, cognition, mood) compared to placebo. **DaT-SPECT imaging:** No significant change versus placebo. This biomarker tracks dopaminergic neuron degeneration; zero signal indicates no neuroprotection at the structural level. **CSF analysis (mechanistic finding):** Only small amounts of exenatide reached the substantia nigra, the brain region affected by Parkinson's. This suggests insufficient CNS penetration to the target region, despite exenatide crossing the blood-brain barrier in other areas. ## Context This trial directly contradicts earlier Phase 2 work (Foltynie group, n=59) which showed significant motor benefit at 9 months (P=0.001). The Phase 3 failure raises questions about: - Phase 2 selection bias or underpowering - Regional brain penetrance as the limiting factor (not BBB crossing per se) - Whether the Phase 2 signal was spurious ## Implications The failure complicates the GLP-1 neuroprotection hypothesis. Two other GLP-1 agonists (semaglutide, liraglutide) remain in ongoing Phase 3 trials for Parkinson's. The CSF finding suggests that different GLP-1 agonists with distinct CNS penetration mechanisms (e.g., semaglutide via albumin binding → tanycytes) may achieve different substantia nigra concentrations and potentially different outcomes. ## Expert Response Dr. Katherine Fletcher (Parkinson's UK): "Really disappointing news" and "a setback." Concerns raised that the failure may impact funding for other GLP-1 trials in Parkinson's. ## Timeline - **2025-02-04** — Phase 3 results published in The Lancet: all endpoints failed, CSF analysis reveals insufficient substantia nigra penetration ## References - The Lancet, February 4, 2025: [Exenatide-PD3 Phase 3 Results](https://www.thelancet.com/journals/lancet/article/PIIS0140-6736(24)02808-3/fulltext) - Parkinson's UK press response, February 2025