Jefferies London Healthcare Conference 2025
Logotype for Wave Life Sciences Ltd

Wave Life Sciences (WVE) Jefferies London Healthcare Conference 2025 summary

Event summary combining transcript, slides, and related documents.

Logotype for Wave Life Sciences Ltd

Jefferies London Healthcare Conference 2025 summary

8 Jul, 2026

Strategic focus and technology

  • Emphasis on building a fully integrated RNA medicines platform targeting genetic diseases, leveraging advanced chemistry for high potency, specificity, and durability across RNA editing and siRNA modalities.

  • Expansion into novel targets such as inhibin E for obesity (WVE-007) and PNPLA3 for liver disease (WVE-008), with ongoing leadership in splicing and allele-specific approaches.

  • Commitment to optimizing oligonucleotide design to unlock new therapeutic modalities and best-in-class opportunities.

  • Entering a data-rich period with significant readouts expected in Q4 2025 and throughout 2026.

Inhibin E program for obesity

  • Inhibin E identified as a unique, genetically validated target for obesity, aiming to induce healthy fat loss without impacting lean mass.

  • Preclinical and early clinical data show dose-dependent, durable reductions in activin E, translating to fat loss equivalent to GLP-1s but sparing muscle and bone.

  • Human data demonstrate sustained activin E knockdown, with higher doses achieving up to 85% reduction and supporting potential for once-yearly dosing.

  • Upcoming Q4 update will provide three-month data on the 240 mg cohort, including metabolic biomarkers, DEXA body composition, and initial weight loss endpoints.

  • Phase 2 maintenance studies are planned to evaluate long-term weight maintenance and off-ramp strategies from incretins, with over 100 patients expected on therapy by mid-2026.

Alpha-1 antitrypsin deficiency (AATD) and RNA editing pipeline

  • RNA editing platform delivers potent, durable, and specific editing in liver, with clinical data showing correction of AATD patients to near-normal M protein levels at low doses.

  • Upcoming data will assess higher dose cohorts for durability and editing efficiency, focusing on M protein as the key efficacy marker.

  • Platform enables rapid translation from genetic insight to clinic, with PNPLA3 program entering clinical trials in 2026 for a large population at risk of liver disease.

  • Editing approach offers advantages over protein replacement and siRNA knockdown, particularly in restoring protein function and addressing substrate limitations.

Partial view of Summaries dataset, powered by Quartr API
AI can get things wrong. Verify important information.
All investor relations material. One API.
Learn more