Skip to content
Specimen Atlas of Research Peptides81 plates · MIT
PeptidesDBan atlas
Side-by-side · Research reference

LivagenvsMT-1

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

AAnimal-StrongHUMAN-REVIEWED20/32 cited
BFDA-ApprovedHUMAN-REVIEWED9/51 cited
Livagen
Khavinson Bioregulator · Hepatoprotective Tetrapeptide
50%Dipeptidase inhibitionTimofeeva 2005
Oral / SQRoutes tested
LiverTarget tissueKhavinson 2001
Oral or SQ · Tissue-specific to liver
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
Livagen
MT-1
Primary target
Hepatocyte protein synthesis machineryBrodskiĭ 2001
Melanocortin-1 receptor (MC1R) on melanocytesLangan 2010
Pathway
Tissue-specific bioregulator → Hepatocyte stimulation → Protein synthesis normalizationBrodskiĭ 2001Khavinson 2001
α-MSH analogue → MC1R activation → cAMP elevation → MITF transcription → eumelanin synthesis
Downstream effect
Age-dependent enzyme normalization, hepatoprotection in fibrosis/hepatitis models, elevated protein synthesis in senescent hepatocytes
Increased melanogenesis, photoprotection, reduced UV sensitivityLangan 2010
Feedback intact?
Yes — exogenous MC1R agonism does not suppress endogenous α-MSH production
Origin
Directed chemical synthesis from amino acid analysis of liver polypeptide preparations (Ventvil)
Synthetic 13-AA peptidomimetic with norleucine (position 4) and D-phenylalanine (position 7) substitutions for metabolic stabilityChawathe 2026
Antibody development

02Dosage Protocols

Parameter
Livagen
MT-1
Animal dose (oral)
Not specified in abstracts; 2-week administration protocolTimofeeva 2005
Per os administration in rats.
Duration (experimental)
2 weeks (enzyme study); up to 24 months (cell culture)Timofeeva 2005Brodskiĭ 2001
Route
Oral or subcutaneous
Resists peptidase hydrolysis, enabling oral bioavailability.Timofeeva 2005
Subcutaneous implant — upper arm or abdomen
Evidence basis
Animal models (rats, 1–24 months age); in vitro hepatocyte cultureTimofeeva 2005Brodskiĭ 2001Khavinson 2002
Phase 3 RCT / FDA-approved orphan drug
Human data
None in provided literature
Standard dose
16 mg subcutaneous implant
FDA-approved formulation (Scenesse).
Frequency
Every 60 days
Sustained release implant — no daily administration required.
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).

04Side Effects & Safety

Parameter
Livagen
MT-1
Reported adverse effects
None documented in animal studies
Human safety data
No human trials in provided literature
Peptide hydrolysis
Weakly hydrolyzed; minimal breakdown by intestinal enzymesTimofeeva 2005
Nausea
Common (>10%) — mild, transient
Implant site reaction
Erythema, bruising, tenderness at insertion site
Hyperpigmentation
Generalised tanning (therapeutic effect), darkening of freckles/neviLangan 2010Habbema 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 2010Habbema 2017
Applies to internet/gym-sourced 'melanotan' — not FDA-approved Scenesse.
Absolute Contraindications
Livagen
MT-1
  • ·Hypersensitivity to afamelanotide or excipients
  • ·Hepatic impairment (no safety data)
  • ·Renal impairment (no safety data)
Relative Contraindications
Livagen
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
Livagen
MT-1
1. Route selection
Oral administration supported by peptidase resistance. Subcutaneous route used in organotypic culture experiments.Timofeeva 2005Khavinson 2001
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. Timing
No specific timing documented. Two-week protocols used in animal models with daily administration.Timofeeva 2005
Pressure applied post-insertion. Sterile dressing × 24 hrs. Avoid strenuous activity for 24–48 hrs to prevent extrusion.
3. Age-dependent response
Elderly individuals may exhibit different enzyme normalization patterns than younger cohorts, based on rat age-stratified findings.Timofeeva 2005
Slow biodegradable polymer matrix releases afamelanotide over 60 days, maintaining therapeutic plasma levels without daily dosing.
4. Repeat dosing
New implant every 60 days during high UV season (spring–autumn in temperate climates). Rotate implant sites to avoid scarring.
5. Monitoring
Baseline and periodic dermatologic exams to document pigmented lesions. Patient education on self-examination for new/changing nevi.