Mazdutide
Mazdutide (IBI362/LY3305677) is a GLP-1/glucagon dual receptor agonist developed by Innovent Biologics and Eli Lilly. This oxyntomodulin-based peptide analog is administered once weekly by subcutaneous injection and is being evaluated in Phase 3 trials for obesity and type 2 diabetes, with the glucagon component providing additional energy expenditure and hepatic fat reduction benefits.
Mazdutide (IBI362, also known as LY3305677) is a once-weekly subcutaneous GLP-1/glucagon dual receptor agonist co-developed by Innovent Biologics and Eli Lilly. Based on the oxyntomodulin backbone, mazdutide is designed to activate both the GLP-1 receptor and the glucagon receptor simultaneously, combining GLP-1-mediated appetite suppression and glycemic control with glucagon-mediated increases in energy expenditure and hepatic lipid mobilization.
Overview
Mazdutide is derived from oxyntomodulin, a naturally occurring 37-amino acid peptide hormone produced by intestinal L-cells alongside GLP-1 and released postprandially. Native oxyntomodulin activates both GLP-1 and glucagon receptors but has a half-life of only a few minutes, making it unsuitable for therapeutic use. Mazdutide is an engineered analog with chemical modifications — including fatty acid acylation for albumin binding — that extend its half-life to approximately one week, enabling once-weekly subcutaneous dosing.
The dual receptor agonism of mazdutide creates a fundamentally different metabolic profile compared to selective GLP-1R agonists like semaglutide. While the GLP-1R component drives appetite suppression, insulin secretion, and delayed gastric emptying (as with semaglutide), the glucagon receptor component stimulates hepatic glycogenolysis, gluconeogenesis (in a controlled manner), lipolysis, thermogenesis, and fatty acid oxidation. The net effect is enhanced weight loss through both reduced energy intake (GLP-1R) and increased energy expenditure (GCGR), with particularly notable effects on liver fat reduction.
Mazdutide is being primarily developed in China through Innovent Biologics' GLORY clinical trial program, with Phase 3 trials ongoing in both obesity and type 2 diabetes. It has received Breakthrough Therapy Designation from the Chinese National Medical Products Administration (NMPA) for obesity.
Mechanism of Action
Mazdutide exerts its therapeutic effects through coordinated activation of two metabolically important receptor systems:
GLP-1 Receptor Agonism: Mazdutide potently activates GLP-1 receptors on pancreatic beta cells, hypothalamic and brainstem neurons, and vagal afferents. This drives glucose-dependent insulin secretion, appetite suppression, delayed gastric emptying, and reduced food intake — the same mechanisms responsible for the metabolic benefits of semaglutide and other GLP-1R agonists.
Glucagon Receptor Agonism: Unlike pure GLP-1R agonists, mazdutide simultaneously activates hepatic glucagon receptors. Glucagon receptor signaling stimulates hepatic lipid oxidation, increases energy expenditure through thermogenesis, promotes amino acid catabolism, and drives lipolysis in adipose tissue. This component is particularly important for reducing hepatic steatosis and increasing total energy expenditure beyond what GLP-1R agonism alone achieves.
Synergistic Weight Loss Mechanism: The dual agonism creates a metabolic environment where energy intake is reduced (via GLP-1R-mediated anorexia) while energy expenditure is simultaneously increased (via GCGR-mediated thermogenesis). This bidirectional approach to energy balance may produce greater net weight loss than either receptor agonist alone.
Hepatic Fat Mobilization: Glucagon receptor activation in hepatocytes promotes fatty acid beta-oxidation, reduces de novo lipogenesis, and stimulates ketogenesis. Combined with GLP-1R-mediated improvements in insulin sensitivity and reduced lipotoxicity, mazdutide has shown substantial reductions in liver fat content, making it a strong candidate for MASH/NAFLD treatment.
Glycemic Regulation: Despite the glucagon component's hyperglycemic potential, the concurrent GLP-1R agonism provides glucose-dependent insulin secretion and glucagon suppression that counterbalances the glucose-raising effects. In clinical trials, mazdutide has consistently reduced HbA1c in patients with type 2 diabetes, demonstrating that the GLP-1R component predominates in glycemic control.
Reconstitution Calculator
Mazdutide
Mazdutide (IBI362, also known as LY3305677) is a once-weekly subcutaneous GLP-1/
Exceeds syringe capacity
Dose requires 2.000mL but syringe holds 1mL. Increase BAC water, use a larger syringe, or split injections.
Set up a clean workspace with all supplies ready.
1x / week for weeks
Research
Comparison with GLP-1R Selective Agonists
The theoretical advantage of GLP-1/glucagon dual agonism over selective GLP-1R agonism lies in the additional energy expenditure and hepatic fat reduction driven by the glucagon component. While head-to-head trials against semaglutide have not been completed for mazdutide, the weight loss magnitude observed in GLORY trials is competitive with semaglutide STEP trials, particularly considering the predominantly Chinese study population where BMI distributions differ from Western cohorts. The liver fat reduction data suggest mazdutide may have a distinct advantage in patients with concurrent hepatic steatosis.
Weight Loss (GLORY-1)
The Phase 3 GLORY-1 trial evaluated mazdutide in Chinese adults with obesity (BMI >=28) or overweight (BMI >=24) with at least one weight-related comorbidity. At 48 weeks, participants receiving mazdutide 9 mg once weekly achieved a mean body weight reduction of approximately 14.4% compared to baseline, with the placebo group achieving approximately 2.7%. Importantly, 61.8% of participants in the 9 mg group achieved at least 10% weight loss, and approximately 40% achieved 15% or greater reduction. Weight loss was progressive throughout the 48-week treatment period. Ji, L. et al. (2024) — Lancet Diabetes Endocrinol.
Type 2 Diabetes (GLORY-2)
The Phase 3 GLORY-2 trial evaluated mazdutide in Chinese adults with type 2 diabetes and overweight/obesity. Mazdutide produced clinically meaningful HbA1c reductions alongside significant weight loss, demonstrating its utility as a dual-action agent for patients with both conditions. Mean HbA1c reductions exceeded 1.5% from baseline at therapeutic doses, and significant proportions of patients achieved HbA1c targets of <7%. Lu, J. et al. (2024) — Lancet Diabetes Endocrinol.
Liver Fat Reduction
Mazdutide has shown particularly striking effects on hepatic steatosis. In Phase 2 studies, magnetic resonance imaging-proton density fat fraction (MRI-PDFF) assessments demonstrated liver fat reductions of 50-70% from baseline, substantially exceeding the reductions typically observed with selective GLP-1R agonists. The glucagon receptor component is believed to be the primary driver of this hepatic benefit, as glucagon directly stimulates hepatic fatty acid oxidation. These findings position mazdutide as a strong candidate for MASH/NAFLD, where no approved treatments currently exist. Tan, Q. et al. (2024) — Diabetes Obes. Metab.
Phase 2 Dose-Ranging
The Phase 2 dose-ranging study evaluated mazdutide at 3 mg, 4.5 mg, 6 mg, and 9 mg weekly doses over 24 weeks. Clear dose-response relationships were observed for both weight loss and glycemic improvement. The 6 mg and 9 mg doses showed the strongest efficacy, and these doses were advanced into Phase 3 trials. Tolerability was dose-dependent with gastrointestinal events as the primary adverse effects. He, W. et al. (2023) — Diabetes Obes. Metab.
Safety Profile
In Phase 2 and Phase 3 trials, mazdutide's adverse event profile is predominantly gastrointestinal and consistent with GLP-1R agonist pharmacology. Nausea occurred in 23-39% of participants, diarrhea in 12-19%, vomiting in 10-17%, and decreased appetite in 8-13%. Most GI events were mild to moderate and occurred during dose titration. Discontinuation rates due to adverse events were 5-9% across dose groups. Mild dose-dependent increases in heart rate (2-5 bpm) were observed. Notably, despite concerns that glucagon receptor activation could raise blood glucose, mazdutide consistently reduced HbA1c in diabetic populations and did not cause hyperglycemia in non-diabetic participants, indicating the GLP-1R component effectively counterbalances glucagon-driven glucose elevation. No pancreatitis signals were detected. Transient, mild elevations in liver transaminases (ALT/AST) were observed in some participants, potentially related to rapid hepatic fat mobilization rather than hepatotoxicity.
Pharmacokinetic Profile
Mazdutide — Pharmacokinetic Curve
Subcutaneous injection (once weekly)Ongoing & Future Research
- Global Phase 3 program: Expansion beyond China to global markets anticipated, potentially through Eli Lilly's development infrastructure.
- MASH/NASH: Dedicated Phase 2/3 trials for metabolic-associated steatohepatitis are anticipated based on the strong liver fat reduction data. The glucagon component's effect on hepatic fat oxidation makes mazdutide particularly suited for this indication.
- Cardiovascular outcomes: A dedicated CVOT will be needed for a cardiovascular risk reduction indication. Dual agonism may provide cardiovascular benefits through both weight loss and glucagon-mediated improvements in lipid metabolism.
- Combination with insulin: Studies in advanced T2D with insulin co-administration are expected.
- Higher-dose exploration: Whether doses above 9 mg could safely increase efficacy is under evaluation.
- Head-to-head comparisons: Comparator trials against semaglutide or tirzepatide would help position mazdutide relative to established GLP-1R agonists.
Quick Start
- Typical Dose
- Start 1.5-3mg weekly, titrate up to 6-9mg based on response
- Frequency
- Once weekly injection
- Route
- Subcutaneous injection (once weekly)
- Cycle Length
- 48-60+ weeks for optimal results per clinical trials
- Storage
- Refrigerate reconstituted solution at 2-8°C, use within 30 days; lyophilized powder at -20°C until reconstitution
Molecular Structure
- Formula
- Proprietary (modified peptide with fatty acid conjugate)
- Weight
- 4,563.1 Da Da
- Length
- 33 amino acids
- CAS
- 2375217-90-0
- PubChem CID
- 163321849
- Exact Mass
- 309.1597 Da
- LogP
- 0.9
- TPSA
- 101 Ų
- H-Bond Donors
- 2
- H-Bond Acceptors
- 6
- Rotatable Bonds
- 5
- Complexity
- 491
Identifiers (SMILES, InChI)
InChI=1S/C15H19N3O4/c1-8(2)15(3)14(21)17-12(18-15)11-10(13(19)20)5-9(6-16-11)7-22-4/h5-6,8H,7H2,1-4H3,(H,19,20)(H,17,18,21)/i4+1D3
NUPJIGQFXCQJBK-JGWVFYFMSA-NResearch Indications
Weight Loss
GLORY-2 demonstrated 20.1% weight loss with 9mg over 60 weeks; 48.7% achieved ≥20% reduction.
Significant reductions in waist circumference, systolic BP (-7.57 mmHg), triglycerides (-43%).
Exploratory analysis showed 80.2% reduction in liver fat, suggesting MASLD/MASH benefits.
Type 2 Diabetes
HbA1c reductions of 1.41-2.03% across trials; DREAMS-3 showed -2.03% vs semaglutide -1.84%.
48% achieved HbA1c <7.0% AND ≥10% weight loss versus 21% with semaglutide.
Cardiovascular
Systolic reduction of -7.57 mmHg, diastolic -2.98 mmHg in clinical trials.
Total cholesterol -16.82%, triglycerides -43.29%, LDL -17.07%.
Research Protocols
subcutaneous Injection
Dual GLP-1/glucagon receptor agonist administered once weekly.
| Goal | Dose | Frequency | Duration |
|---|---|---|---|
| Standard — Initiation | 2.5 mg | Once weekly | Weeks 1-4 |
| Standard — Full dose | 5 mg | Once weekly | Weeks 5-8+ |
| Advanced — Phase 1 | 5 mg | Once weekly | Weeks 1-4 |
| Advanced — Phase 2 | 7.5 mg | Once weekly | Weeks 5-8 |
| Advanced — Phase 3 | 10 mg | Once weekly (split into 2 injections) | Weeks 9-12+(Min 8 weeks. Trials studied 12-48 weeks.) |
Reconstitution Guide (5mg vial + 3mL BAC water)
- Wipe vial tops with alcohol swab
- Draw 3.0 mL bacteriostatic water into syringe (standard) or 2.0 mL (high-dose)
- Inject slowly down the inside wall of the peptide vial
- Gently swirl to dissolve — never shake
- Resulting concentration: 1.67 mg/mL (3.0 mL) or 2.5 mg/mL (2.0 mL)
- For 2.5 mg dose (3.0 mL reconstitution): draw 150 units (1.50 mL)
- For 5 mg dose (2.0 mL reconstitution): draw 200 units (2.00 mL)
- Store reconstituted vial refrigerated at 2-8°C
Interactions
Peptide Interactions
Hepatic Fat Mobilization: Glucagon receptor activation in hepatocytes promotes fatty acid beta-oxidation, reduces de novo lipogenesis, and stimulates ketogenesis.
Mazdutide is derived from oxyntomodulin, a naturally occurring 37-amino acid peptide hormone produced by intestinal L-cells alongside GLP-1 and released postprandially.
- Head-to-head comparisons: Comparator trials against semaglutide or tirzepatide would help position mazdutide relative to established GLP-1R agonists.
The theoretical advantage of GLP-1/glucagon dual agonism over selective GLP-1R agonism lies in the additional energy expenditure and hepatic fat reduction driven by the glucagon component. While head-to-head trials against semaglutide have not been completed for mazdutide, the weight loss magnitu...
What to Expect
What to Expect
Appetite reduction, possible mild nausea, decreased portion sizes
Early weight loss begins (1-2%), improved satiety after meals
Dose escalation phase, GI symptoms typically improving, 3-5% weight loss
Steady weight loss continues (7-12%), energy expenditure effects evident
Significant weight reduction (12-17%), metabolic markers improving
Peak effects (up to 20% weight loss), sustained improvements in BP, lipids, glucose
Safety Profile
Common Side Effects
- Nausea (mild-moderate, typically improves over time)
- Diarrhea
- Vomiting
- Increased heart rate (5-17 bpm observed)
Contraindications
- Personal or family history of medullary thyroid carcinoma
- MEN2 syndrome history (class warning for GLP-1 agonists)
- Pregnancy or breastfeeding (insufficient safety data)
Discontinue If
- Severe or persistent abdominal pain (potential pancreatitis)
- Neck lumps, hoarseness, or difficulty swallowing
- Severe nausea/vomiting preventing adequate nutrition or hydration
- Signs of severe hypoglycemia (confusion, sweating, shakiness)
- Severe allergic reactions (rash, difficulty breathing, facial swelling)
- Unusual mood changes, depression, or suicidal thoughts
- Signs of gallbladder problems (severe upper right abdominal pain)
Quality Indicators
What to look for
- White to off-white lyophilized powder without clumping or discoloration
- Completely clear and colorless appearance after reconstitution—no visible particles
- Intact vial seal and clear labeling with mg dosage, batch numbers, expiration dates
Caution
- Source verification critical—available from research chemical suppliers
Red flags
- Clumping, discoloration, or moisture in powder
- Persistent cloudiness or particles after reconstitution indicates degradation
Frequently Asked Questions
References (14)
- [7]
- [15]
- [1]GLORY-1 Phase 3 Trial (2025)
- [2]GLORY-2 Phase 3 Trial (2025)
- [3]DREAMS-3 Phase 3 Trial - Head-to-Head vs Semaglutide (2025)
- [4]Phase 2 T2D Trial (2024)
- [6]
- [10]
- [12]Lu, J. et al Mazdutide for the treatment of type 2 diabetes in Chinese adults (GLORY-2) Lancet Diabetes Endocrinol. (2024)
- [13]He, W. et al Mazdutide Phase 2 dose-finding study Diabetes Obes. Metab. (2023)
- [8]
- [5]
- [9]
- [14]Tan, Q. et al Effects of mazdutide on hepatic fat content Diabetes Obes. Metab. (2024)
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