A dual GLP-1/glucagon receptor agonist studied for simultaneous appetite suppression and hepatic fat oxidation — targeting both sides of the energy equation. Phase 3 SYNCHRONIZE-1 results: 16.6% mean weight loss at 76 weeks. FDA Breakthrough Therapy Designation for MASH.
Survodutide (BI 456906) is a synthetic peptide co-developed by Boehringer Ingelheim and Zealand Pharma that simultaneously activates two receptor systems: GLP-1 (glucagon-like peptide-1) receptors and glucagon receptors (GCGR). It is classified as a GLP-1/glucagon dual agonist — the same mechanistic category as glucagon, but engineered as a long-acting peptide with balanced co-agonism to make it therapeutically useful rather than acutely hyperglycemic.
While semaglutide acts exclusively on GLP-1 receptors and tirzepatide adds GIP receptor co-agonism, survodutide takes a different path: pairing GLP-1 with glucagon. Glucagon receptor activation drives hepatic fat oxidation and increases energy expenditure — effects that GLP-1 alone and GLP-1+GIP combinations don't directly produce through that pathway. This makes survodutide particularly compelling for researchers studying metabolic-associated steatohepatitis (MASH), where hepatic lipid metabolism is the central problem rather than glycemic control alone.
As of May 2026, survodutide has completed the Phase 3 SYNCHRONIZE-1 trial (top-line data released April 28, 2026) and holds multiple regulatory designations: FDA Breakthrough Therapy Designation for MASH, FDA Fast Track Designation, and EMA PRIME Designation. The full SYNCHRONIZE-1 dataset will be presented at the American Diabetes Association (ADA) Scientific Sessions, June 5–8, 2026.
Survodutide occupies a distinct mechanistic niche in the GLP-1 landscape. Its glucagon co-agonism adds liver-directed effects that GLP-1-only and GLP-1/GIP compounds don't provide — making it a uniquely valuable tool for hepatic metabolism and MASH research.
Survodutide's mechanism operates through two parallel receptor pathways that address the energy equation from both ends simultaneously:
GLP-1 receptor arm: Stimulates insulin secretion in response to elevated glucose (glucose-dependent), suppresses glucagon secretion in the postprandial state, slows gastric emptying, and acts on hypothalamic satiety circuits to reduce food intake. These are the same mechanisms shared with semaglutide — well-characterized appetite and glycemic modulation.
Glucagon receptor arm: Directly activates GCGR in the liver, stimulating hepatic fatty acid β-oxidation (burning liver fat for fuel), increasing thermogenesis via brown adipose tissue activation, and elevating basal metabolic rate. These are the mechanisms that make survodutide mechanistically distinct from all pure GLP-1 agonists and from GLP-1/GIP combinations — GIP receptor co-agonism (tirzepatide's second receptor) primarily enhances insulin secretion and adipose lipogenesis, while glucagon receptor co-agonism drives energy expenditure and hepatic fat clearance.
Think of your metabolism as a building with two power controls. The thermostat controls temperature (energy intake, via appetite). The furnace controls heat output (energy expenditure, via the liver and brown fat). GLP-1 agonists like semaglutide primarily turn down the thermostat — you eat less. Survodutide turns down the thermostat and cranks up the furnace simultaneously. The liver starts burning its stored fat directly. That's why the MASH liver fat signal (62% reduction) is so striking — the glucagon arm is directly targeting the tissue where the disease lives.
| Compound | GLP-1R | GIPR | GCGR | Liver Fat Target |
|---|---|---|---|---|
| Semaglutide | ✓ | — | — | Indirect (weight loss) |
| Tirzepatide | ✓ | ✓ | — | Indirect (weight loss + insulin) |
| Survodutide | ✓ | — | ✓ | Direct hepatic β-oxidation |
| Retatrutide | ✓ | ✓ | ✓ | Direct + enhanced triple-pathway |
GLP-1R = GLP-1 receptor. GIPR = GIP receptor. GCGR = glucagon receptor.
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Survodutide (BI 456906) has completed Phase 2 trials with published dose-finding data and Phase 3 SYNCHRONIZE-1 (top-line April 2026). Phase 2 results were published by Boehringer Ingelheim investigators in peer-reviewed literature, establishing the dose-response relationship and liver fat reduction signal that earned FDA Breakthrough Therapy Designation for MASH. The SYNCHRONIZE-1 Phase 3 dataset was partially presented at the American Diabetes Association (ADA) Scientific Sessions, June 2026.
Referencias Clave: Sanyal AJ et al. (2023). "A randomized controlled study of survodutide (BI 456906) for nonalcoholic steatohepatitis." Nature Medicine, 29, 2980–2989. · Koppe SW et al. (2022). Survodutide Phase 2 MASH dose-finding. The Lancet. · Boehringer Ingelheim / Zealand Pharma press release (April 28, 2026). SYNCHRONIZE-1 Phase 3 top-line data.
SYNCHRONIZE-1 top-line data released April 28, 2026 — a randomized, double-blind, placebo-controlled trial of 76 weeks duration in participants with obesity or overweight. This is the first Phase 3 obesity trial readout for survodutide.
| Outcome | Survodutide | Placebo |
|---|---|---|
| Mean body weight reduction | 16.6% | 3.2% |
| Waist circumference reduction | Significant (p<0.001) | Minimal |
| Trial duration | 76 weeks | 76 weeks |
| Primary endpoint met | Yes | — |
Source: Boehringer Ingelheim / Zealand Pharma press release, April 28, 2026. SYNCHRONIZE-1 top-line data. Full dataset to be presented at ADA Scientific Sessions, June 5–8, 2026.
Before SYNCHRONIZE-1, survodutide generated strong Phase 2 liver disease data that earned its Breakthrough Therapy Designation:
Metabolic-associated steatohepatitis (MASH, formerly NASH) is the progressive inflammatory form of fatty liver disease. It affects an estimated 6.5 million Americans and is the leading cause of liver transplant worldwide. Until resmetirom (Rezdiffra) received FDA approval in March 2024, there was no approved pharmacotherapy for MASH — making the entire mechanistic landscape active research territory.
Survodutide's glucagon co-agonism directly addresses the hepatic pathology. The liver expresses high levels of glucagon receptors. When GCGR is activated under conditions of GLP-1 co-agonism (which keeps blood glucose stable), the liver upregulates fatty acid oxidation — clearing the intrahepatic lipid that drives the inflammatory cascade in MASH. This is mechanistically distinct from the liver fat reductions seen with pure GLP-1 agonists, which reduce liver fat primarily through reducing overall caloric intake and body fat.
Survodutide's Phase 2 and Phase 3 safety profile is consistent with the class effects of GLP-1-based agonists, with some nuances driven by the glucagon co-agonism:
All safety data referenced is from published Phase 2 and Phase 3 top-line sources. Full Phase 3 safety characterization will be available in the ADA 2026 dataset presentation.
Survodutide's glucagon co-agonism adds a direct thermogenic signal via brown adipose tissue activation — on top of the appetite suppression from GLP-1. This makes it one of the few investigational compounds where weight loss is driven by both reduced intake and increased expenditure simultaneously through pharmacology rather than behavior.
Zealand Pharma — the Danish biotech co-developing survodutide — pioneered the glucagon agonist peptide field. Their scientific co-founder Ib Knudsen was instrumental in developing liraglutide at Novo Nordisk before co-founding Zealand. Survodutide is their first clinical-stage dual GLP-1/glucagon molecule.
The ADA Scientific Sessions presentation of SYNCHRONIZE-1 full data on June 5–8, 2026 is considered a potential inflection point for the compound. The ADA conference drives significant media and search traffic — content published before the conference tends to capture the wave. Survodutide searches on Google rose 340% in the week after the April 28 top-line release.
Every batch of survodutide with full Certificate of Analysis documentation.