Side-by-side · Research reference

MazdutidevsMT-1

Side-by-side comparison across mechanism, dosage, evidence, side effects, administration, and stack synergies. Citations on every claim where available.

APhase 3HUMAN-REVIEWED19/62 cited

BFDA-ApprovedHUMAN-REVIEWED9/51 cited

Mazdutide

GLP-1/Glucagon Dual Agonist · Oxyntomodulin Analogue · Phase 3

9 mgWeekly doseJi 2026

12.4%Weight lossAzam 2026

Phase 3Status (China)

SQ · Abdomen · Once WeeklyJi 2026

MT-1

α-MSH Analogue · FDA-Approved

16 mgImplant dose

13 AAPeptide lengthChawathe 2026

2019FDA approval

SQ Implant · 60-Day Release

01Mechanism of Action

Parameter

Mazdutide

MT-1

Primary target

GLP-1 receptor and glucagon receptorAbdul 2026 Elmendorf 2026

Melanocortin-1 receptor (MC1R) on melanocytesLangan 2010

Pathway

Dual agonism: GLP-1R → satiety, insulin secretion, gastric emptying delay; GCGR → hepatic lipolysis, energy expenditure, thermogenesisElmendorf 2026 Abulehia 2026

α-MSH analogue → MC1R activation → cAMP elevation → MITF transcription → eumelanin synthesis

Downstream effect

Weight loss via appetite suppression (GLP-1 axis) and increased energy expenditure (glucagon axis); improved glycemic control in T2D

Increased melanogenesis, photoprotection, reduced UV sensitivityLangan 2010

Feedback intact?

Yes — physiological receptor-mediated signaling preserved

Yes — exogenous MC1R agonism does not suppress endogenous α-MSH production

Origin

Synthetic oxyntomodulin analogue — endogenous peptide with dual GLP-1/glucagon activity

Synthetic 13-AA peptidomimetic with norleucine (position 4) and D-phenylalanine (position 7) substitutions for metabolic stabilityChawathe 2026

Antibody development

—

02Dosage Protocols

Parameter

Mazdutide

MT-1

Phase 2 studied dose

9 mg / weekJi 2026

Highest efficacy dose in obesity trial (BMI ≥30 kg/m²).Ji 2026

—

Frequency

Once weeklyJi 2026 Luo 2026

Every 60 days

Sustained release implant — no daily administration required.

Route

SubcutaneousJi 2026

Subcutaneous implant — upper arm or abdomen

Dose escalation

3 mg → 6 mg → 9 mg (titration schedule in trials)

Gradual escalation to minimize GI side effects.

—

Evidence basis

Phase 2 RCT / Phase 3 ongoingJi 2026 Luo 2026

Phase 3 RCT / FDA-approved orphan drug

Duration (trials)

24–48 weeks

—

Population

Non-diabetic adults BMI ≥30 kg/m² or ≥27 kg/m² with comorbidities

—

Phase 3 comparator

Semaglutide 1 mg/week (DREAMS-3 trial)Luo 2026

—

Standard dose

—

16 mg subcutaneous implant

FDA-approved formulation (Scenesse).

Indication

—

Erythropoietic protoporphyria (EPP)

Narrow FDA approval — not licensed for cosmetic tanning.

Duration

—

Seasonal use (spring–autumn typical)

Aligned with peak UV exposure months.

Stability

—

Norleucine/D-Phe substitutions enhance peptidase resistance

Modified structure vs endogenous α-MSH (Met⁴, L-Phe⁷).

03Metabolic / Fat Loss Evidence

Parameter

Mazdutide

MT-1

Percentage body weight loss

12.4% (pooled meta-analysis, 9 mg dose)

95% CI: -16.15% to -8.68%, random-effects model.Azam 2026

—

Absolute weight loss

9.8 kg (mean)Azam 2026

95% CI: -13.15 to -6.37 kg.Azam 2026

—

Responder rate (≥10% loss)

Not explicitly reported in available abstracts

—

Mechanism

Appetite suppression (GLP-1) + energy expenditure (glucagon)Elmendorf 2026

—

BMI reduction

Significant reduction in Chinese adults BMI ≥30 kg/m²Ji 2026

—

Visceral fat

Expected benefit from glucagon-mediated lipolysis (not quantified in abstracts)

—

Glycemic improvement

HbA1c reduction in T2D cohort (Phase 3 DREAMS-3)

—

Comparator efficacy

Head-to-head vs semaglutide 1 mg (Phase 3 pending publication)Luo 2026

—

Key publications

Ji et al. Med 2026 · Azam et al. Diab Obes Metab 2026 · Luo et al. Contemp Clin Trials 2026

—

04Side Effects & Safety

Parameter

Mazdutide

MT-1

Gastrointestinal symptoms

Nausea, vomiting, diarrhea (most common, GLP-1 effect)

—

Injection site reactions

Erythema, pruritus, local discomfort

—

Hypoglycemia

Low risk in non-diabetic cohort; monitor in T2D with insulin or sulfonylureas

—

Cardiovascular effects

Increased heart rate (glucagon effect, transient)

—

Pancreatitis risk

Theoretical (incretin class effect); monitor amylase/lipase if abdominal pain

—

Thyroid C-cell tumors

Black box warning for GLP-1 class (rodent data); human relevance unclear

—

Gallbladder disease

Cholelithiasis, cholecystitis (rapid weight loss effect)

—

Tolerability

Generally well-tolerated; GI effects diminish with dose titration

—

Nausea

—

Common (>10%) — mild, transient

Implant site reaction

—

Erythema, bruising, tenderness at insertion site

Hyperpigmentation

—

Generalised tanning (therapeutic effect), darkening of freckles/neviLangan 2010 Habbema 2017

Expected melanogenic response — complicates pigmented lesion surveillance.

Melanocytic changes

—

Rapid pigmentation of existing nevi; new melanocytic lesions reported with unregulated useHabbema 2017

Requires dermatologic monitoring; theoretical melanoma concern with chronic stimulation.

Headache

—

Occasional (MC1R-independent melanocortin effects)

Photosensitivity (paradoxical)

—

Rare phototoxic reactions despite melanin increase

Contamination risk (unregulated)

—

Impurity, infection, blood-borne virus transmission from illicit melanotan productsLangan 2010 Habbema 2017

Applies to internet/gym-sourced 'melanotan' — not FDA-approved Scenesse.

Absolute Contraindications

Mazdutide

·Personal or family history of medullary thyroid carcinoma
·Multiple endocrine neoplasia syndrome type 2 (MEN 2)
·Hypersensitivity to mazdutide or excipients
·Pregnancy

MT-1

·Hypersensitivity to afamelanotide or excipients
·Hepatic impairment (no safety data)
·Renal impairment (no safety data)

Relative Contraindications

Mazdutide

·History of pancreatitis
·Severe gastroparesis or GI motility disorders
·Diabetic retinopathy (monitor, risk of worsening with rapid glycemic change)
·Renal impairment (limited data, use with caution)

MT-1

·History of melanoma or atypical nevi (melanocortin receptor stimulation concern)Habbema 2017
·Pregnancy/lactation (insufficient data)
·Photosensitive dermatoses (other than EPP)

05Administration Protocol

Parameter

Mazdutide

MT-1

1. Preparation

Supplied as pre-filled pen or reconstituted vial (per manufacturer instructions). Inspect solution — should be clear, colorless to pale yellow. Discard if cloudy or particulate matter present.

Performed by trained healthcare provider. Sterile technique. Small incision in upper arm (triceps) or lower abdomen using trocar. 16 mg rod (4 mm × 1.5 cm) inserted subcutaneously.

2. Injection site

Subcutaneous — abdomen preferred, also thigh or upper arm. Rotate sites weekly. Avoid areas with scarring, moles, or active inflammation.

Pressure applied post-insertion. Sterile dressing × 24 hrs. Avoid strenuous activity for 24–48 hrs to prevent extrusion.

3. Timing

Once weekly, same day each week. May be taken with or without food. If dose missed, administer within 3 days; if >3 days, skip and resume next scheduled dose.

Slow biodegradable polymer matrix releases afamelanotide over 60 days, maintaining therapeutic plasma levels without daily dosing.

4. Storage

Refrigerate 2–8 °C. Do not freeze. May be kept at room temperature (<25 °C) for up to 14 days if needed. Protect from light.

New implant every 60 days during high UV season (spring–autumn in temperate climates). Rotate implant sites to avoid scarring.

5. Needle technique

Use supplied needle or compatible insulin syringe (if reconstituting). Pinch skin, inject at 90° angle. Hold 5–10 seconds before withdrawing needle to prevent leakage.

Baseline and periodic dermatologic exams to document pigmented lesions. Patient education on self-examination for new/changing nevi.