Wave Life Sciences (WVE) Study result summary
Event summary combining transcript, slides, and related documents.
Study result summary
8 Jul, 2026Key interim Phase 1 results and clinical impact
A single 240 mg dose of WVE-007 led to significant, placebo-adjusted reductions in visceral fat (−14%), total fat (−5.3%), waist circumference (−3.3%), and body weight (−1%) at six months, with lean mass preserved or increased (+2%).
Durable, dose-dependent suppression of Activin E was observed, with up to 88% mean maximum reduction and over 70% suppression maintained for at least seven months, supporting potential for once or twice-yearly dosing.
All reductions were placebo-adjusted and statistically significant (p < 0.05).
Greater fat loss was observed in participants with higher baseline visceral fat, with the 400 mg cohort showing a −5% reduction in visceral fat at three months.
WVE-007 was generally safe and well tolerated, with only mild or moderate adverse events, no serious safety signals, and no discontinuations through 600 mg.
Mechanism and clinical rationale
WVE-007 is a GalNAc-siRNA targeting INHBE, reducing Activin E to promote adipocyte lipolysis and fat loss while preserving muscle, unlike current incretin therapies.
Human genetic data show INHBE loss-of-function carriers have lower visceral fat, improved metabolic profiles, and reduced risk of type 2 diabetes and cardiovascular disease.
Suppression of Activin E is correlated with reductions in BMI, abdominal fat, and fasting insulin.
Preclinical data indicate WVE-007 induces fat loss and improves insulin sensitivity, with additive effects when combined with GLP-1 therapies.
The approach is orthogonal to GLP-1s, which often cause muscle loss and require frequent dosing; WVE-007 may enable infrequent dosing and is positioned as a potential add-on or maintenance therapy.
Study design and participant characteristics
Phase 1 (SAD) included otherwise healthy adults with BMI ~32 kg/m² and lower baseline visceral fat than typical phase II/III obesity studies; no diet or exercise modifications were made.
Baseline characteristics differed between 240 mg and 400 mg cohorts, with the latter having lower BMI and visceral fat.
Placebo arms did not include lifestyle interventions, isolating the drug effect.
Improvements in body composition were achieved without diet or exercise modifications.
Visceral fat-to-muscle ratio improved more with WVE-007 than with semaglutide, and was on par with bimagrumab, despite a healthier baseline population.
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