Mazdutide

Mazdutide (IBI-362 / LY3305677)

Developer: Innovent Bio (China); Eli Lilly (ex-China rights, code LY3305677)
Class: Dual GLP-1 receptor agonist + glucagon receptor (GCGR) agonist — same mechanistic class as Survodutide (BI 456906)
Route: Once-weekly subcutaneous injection
Regulatory status: NMPA-approved in China for chronic weight management (mid-2025) and T2D (late 2025); no FDA, EMA, or other ex-China approval found

Mazdutide and Survodutide are both dual GLP-1/GCGR agonists. They differ in sponsor, trial population, phase 3 maturity, and regulatory status. Do not treat them as interchangeable or conflate their evidence bases.

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TL;DR

Mazdutide is a dual GLP-1/GCGR agonist with the strongest evidence from GLORY-1, a phase 3 RCT in Chinese adults with obesity (n=610). At 48 weeks, mazdutide 6 mg produced −14.01% weight loss versus +0.30% placebo. It is NMPA-approved in China but has no FDA or EMA approval; non-Chinese phase 3 obesity outcomes are not available. GI adverse events dominate the safety profile. Direct head-to-head comparisons versus semaglutide 2.4 mg, Tirzepatide, Retatrutide, or Orforglipron have not been completed.

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Why it matters for Vitals

• Body composition: weight-loss magnitude is meaningful and in the range of injectable GLP-1 monotherapy benchmarks; lean mass impact is not well characterized (no published DXA data).
• Glycemic monitoring: T2D populations show HbA1c reduction; CGM translation is defensible in diabetes contexts but not in obesity-only users.
• Wearable interpretation: RHR/HRV/activity signals are expected class-level pharmacologic effects but are not mazdutide-specific; automated coaching rules do not exist.
• Coaching boundary: treat as an NMPA-approved medication topic in China-facing contexts; treat as investigational in all other jurisdictions; human signoff required for any dosing, stack, or adverse-event interpretation.

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Key facts

Parameter	Value
Half-life	~8 days at 16 mg (U.S. phase 1); supports once-weekly SC
Tmax	~72 h (slow absorption)
Dose range studied	3 mg, 4 mg, 4.5 mg, 6 mg, 9 mg, 10 mg, 16 mg
Phase 3 anchor	GLORY-1 (NCT05607680); Chinese adults with obesity/overweight
Weight loss, GLORY-1 6 mg / 48 wk	−14.01% vs +0.30% placebo
Weight loss, GLORY-1 4 mg / 48 wk	−11.00% vs +0.30% placebo
T2D evidence	Phase 2/3 vs placebo and vs dulaglutide (DREAMS-2); HbA1c + weight reductions confirmed
Safety	GI-dominant; mostly mild-to-moderate; low discontinuation due to AEs in GLORY-1
CV outcomes	No dedicated MACE/CVOT found
Regulatory (ex-China)	None found; no FDA NDA/BLA, EMA EPAR, or MAA identified

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Mechanism summary

Mazdutide is a unimolecular peptide dual agonist modeled on oxyntomodulin-like pharmacology.

GLP-1R agonism produces:

• Appetite suppression via hindbrain/hypothalamus
• Delayed gastric emptying → prolonged satiety
• Glucose-dependent insulin secretion

GCGR agonism produces:

• Hepatic glycogenolysis and gluconeogenesis stimulation
• Lipolysis and hepatic lipid oxidation
• Increased resting energy expenditure (thermogenesis) — biologically plausible; human mazdutide-specific REE measurement is a Gap

Mechanistic boundary: human studies confirm weight and glycemic effects but do not isolate the incremental GCGR contribution to weight loss. GCGR energy-expenditure claims are biologically plausible and class-supported; mazdutide-specific thermogenesis in humans is not directly established.

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What the current evidence suggests

Strongest evidence (Confirmed)

• GLORY-1 phase 3: −10.09% (4 mg) and −12.55% (6 mg) at week 32; −11.00% (4 mg) and −14.01% (6 mg) at week 48, vs placebo (PMID 40421736)
• Phase 2 obesity: dose-related −6.7%, −10.4%, −11.3% at 3/4.5/6 mg vs −1.0% placebo at 24 weeks (PMID 38092790)
• T2D: HbA1c and weight reduction vs placebo and vs dulaglutide (PMID 37943529, 41407859, 41407860)

Supported evidence

• High-dose 9–16 mg phase 1b: large short-term weight loss; sample sizes small; early-phase only (PMID 36247927, 40832785)
• Dual GLP-1/GCGR mechanism is biologically plausible for combined appetite suppression + energy-expenditure effect

Key gaps

• No completed direct obesity head-to-head vs semaglutide 2.4 mg, Tirzepatide, Retatrutide, survodutide, or Orforglipron
• DREAMS-3 compares mazdutide 6 mg vs semaglutide 1 mg in T2D+obesity — outcomes not yet found (baseline only; PMID 41260459)
• GLORY-2 9 mg phase 3 obesity outcomes not yet published
• Non-Chinese phase 3 obesity data not found
• Lean mass / DXA body composition data not found
• Dedicated MACE/CVOT not found
• Active metabolite profile not established
• BBB / tissue distribution not established

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Risks and uncertainty

• GI adverse events are the primary tolerability barrier; mostly mild-to-moderate in GLORY-1
• Lipase elevations reported in small phase 1b T2D trial; no investigator-suspected pancreatitis; cardiac ischemia events judged unrelated (PMID 35750681)
• Long-term CV safety is the largest open gap — no MACE/CVOT data available
• Jurisdiction gap: all completed phase 3 obesity trials are in Chinese adults; non-Chinese efficacy and tolerability are unknown
• Regulatory gap: no FDA, EMA, or other ex-China approval, label, or NDA/BLA/EPAR found
• Lean mass: no DXA data published; assume uncertain impact; apply standard GLP-1 Muscle Preservation precautions
• GCGR energy-expenditure: not directly measured in mazdutide human trials

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Comparison to related GLP-1 class agents

Drug	Mechanism	Approx. weight loss	Key distinction
Semaglutide 2.4 mg	GLP-1 mono	~15%	Established CV evidence; FDA approved
Tirzepatide	GLP-1 + GIP dual	~21%	GIP adds lipid buffering; FDA approved
Retatrutide	GLP-1 + GIP + Glucagon triple	~28.7%	GCGR prevents plateau; phase 3
Orforglipron	GLP-1 mono, oral non-peptide	~9–11%	Oral; no fasting; GI tolerability limits
Survodutide	GLP-1 + Glucagon dual (BI 456906)	~15% (phase 2)	Phase 3 SYNCHRONIZE; MASH signal
Mazdutide	GLP-1 + Glucagon dual	~14% (phase 3)	China-approved only; Chinese adults; no head-to-head data

Indirect comparisons differ by population, duration, estimand, background, and dose. Do not use this table to claim superiority or equivalence.

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Vitals monitoring protocol

mazdutide_monitoring_policy:
  evidence_status: investigational (ex-China); approved (China only)
  human_signoff_required: true
  direct_metrics:
    - body_weight
    - waist_or_bmi
    - glycemic_labs_when_diabetes_context_exists
    - gi_symptoms
    - appetite_or_decreased_appetite_self_report
  proxy_metrics:
    - resting_heart_rate
    - hrv
    - activity
    - cgm_metrics_in_diabetes_context_only
  speculative_metrics:
    - wearable_energy_expenditure
    - sleep_recovery_rules
    - automated_adherence_detection
  disallowed_claims:
    - fda_approved_without_label_source
    - best_in_class_without_head_to_head_data
    - validated_wearable_coaching_rules
    - non_chinese_efficacy_without_trial_data

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Related notes

• GLP-1 GIP Glucagon — mechanism note; shared by Retatrutide, Tirzepatide, Survodutide, Mazdutide
• Survodutide — same dual GLP-1/GCGR class; different sponsor, population, phase 3 maturity
• Retatrutide — GLP-1/GIP/Glucagon triple; ~28.7% weight loss; phase 3
• Tirzepatide — GLP-1/GIP dual; ~21% weight loss; FDA approved
• Semaglutide — GLP-1 mono; ~15% weight loss; established CV evidence
• Orforglipron — oral non-peptide GLP-1; FDA approved 2026
• GLP-1 Muscle Preservation — lean mass risk across GLP-1 class; applies to Mazdutide
• GLP-1 RA NAION Safety Signal — class-level safety signal; regulatory review ongoing
• GLP-1 RA Pancreatitis Safety Signal — class-level safety signal; relative risk ~2–3×
• Peptides MOC
• Vitals Knowledge Map