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

5-Amino-1MQvsMGF

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

AAnimal-StrongAUTO-DRAFTED8/38 cited
BAnimal-StrongHUMAN-REVIEWED14/55 cited
5-Amino-1MQ
NNMT inhibitor · Methylation / SAM modulation
100–200 mgDaily dose (oral)Neelakantan 2018
AnimalEvidence levelNeelakantan 2018
HoursHalf-life (est)
Oral · Once daily fasted
MGF
IGF-1Ec Splice Variant · Muscle-Specific
IGF-1EcSplice variantArmakolas 2016
24-AASynthetic E-domain
Animal onlyHuman evidence
SQ · Research context only

01Mechanism of Action

Parameter
5-Amino-1MQ
MGF
Primary target
Nicotinamide N-methyltransferase (NNMT)Neelakantan 2018
Satellite cells (Pax7+) in skeletal muscleMoore 2018
Pathway
NNMT inhibition → preserved cellular SAM + NAD⁺ → restored methylation balance + ↑ thermogenic gene expressionNeelakantan 2018
Mechanical stress → IGF-1Ec mRNA upregulation → Local E-domain peptide release → Satellite cell activation
Downstream effect
Reversal of HFD-induced obesity in murine models; improved metabolic profileNeelakantan 2018
Satellite cell proliferation, myoblast differentiation, muscle fiber repair
Feedback intact?
Origin
Selective small-molecule inhibitor designed in academic medicinal chemistry programsNeelakantan 2018
Alternative splicing of IGF-1 gene (exons 4-6) produces IGF-1Ec precursor; E-domain cleaved post-translationallyArmakolas 2016Vassilakos 2017
Antibody development

02Dosage Protocols

Parameter
5-Amino-1MQ
MGF
Standard dose
100–200 mg / day oralNeelakantan 2018
Anecdotal community range; murine doses scaled.
Frequency
Once daily, fasted
Lower / starter dose
50 mg / day
Evidence basis
Animal-strong; no human RCT dataNeelakantan 2018
Animal models + in vitro only
Duration
8–12 weeks per cycle
Form
Oral capsule
Timing
Morning fasted preferred
Half-life
Hours (estimated; no human PK published)
Synthetic peptide
24-amino-acid E-domain sequence
Corresponds to human IGF-1Ec exons 4-6 region.
Rodent cardiac model
200 μg/kg via peptide-eluting microstructures
Post-MI injection; improved ejection fraction by 8 weeks.
Acute delivery (mouse MI)
Single bolus within 12 hrs post-infarctionShioura 2014
Delayed decompensation; no human protocol established.
Human evidence
None — no published clinical trials
All dosing extrapolated from animal models.
Detection in doping
Full-length MGF detected via LC-MS in illicit productsThevis 2014
WADA-prohibited since 2005; no therapeutic indication.

04Side Effects & Safety

Parameter
5-Amino-1MQ
MGF
GI symptoms
Mild nausea (anecdotal)
Methylation disruption
Theoretical risk if NNMT is over-inhibited (B vitamin metabolism)
Long-term safety
Unknown — no human trials
Cancer risk
Unclear — NNMT also studied in oncology contexts
Pregnancy / OB
Avoid
Drug interactions
Theoretical with niacin / B-vitamin supplements
Human safety data
None — no clinical trials published
Theoretical IGF-1 axis risk
Chronic IGF-1Ec overexpression linked to cancer progression (prostate, colorectal, breast)
Tumor promotion
IGF-1Ec overexpressed in osteosarcoma, colorectal polyps with dysplasia, endometrial cancer
Antibody development
Unknown — no longitudinal human exposure data
Local injection reaction
Presumed similar to other peptides (erythema, induration) — no direct evidence
Dysregulated expression with age
Older adults (70+ yrs) show blunted IGF-1Ec response post-exercise vs youngMoore 2018
Absolute Contraindications
5-Amino-1MQ
  • ·Pregnancy / breastfeeding
  • ·Active malignancy
MGF
  • ·Active malignancy or history of IGF-1-sensitive cancers (prostate, colorectal, breast, osteosarcoma)
  • ·No established therapeutic use — investigational only
Relative Contraindications
5-Amino-1MQ
  • ·Methylation-sensitive conditions (MTHFR mutation)
  • ·Concurrent niacin / NAD+ precursor supplementation (theoretical interference)
MGF
  • ·Family history of IGF-1-axis malignancies
  • ·Use outside research setting

05Administration Protocol

Parameter
5-Amino-1MQ
MGF
1. Form
Oral capsule. No injection.
MGF (E-domain peptide) has no approved clinical protocol. All published data derive from animal models or in vitro experiments.
2. Administration
Take with water, fasted preferred.
Commercially available MGF corresponds to the 24-amino-acid human E-domain (hEc). Rodent E-domain (Eb) is structurally distinct and not interchangeable.
3. Timing
Morning fasted.
Rodent studies used peptide-eluting polymeric microstructures (cardiac) or direct intramuscular injection. Routes and doses non-translatable to humans.Peña 2015Shioura 2014
4. Storage
Room temp ≤25 °C, dry place.
MGF peptides prohibited in sport since 2005. Detection via LC-MS established for full-length MGF products.Thevis 2014
5. Caveat
Monitor B-vitamin status with chronic use.
Any human use falls outside approved medical practice and regulatory frameworks. No safety or efficacy data exist.

06Stack Synergy

5-Amino-1MQ
— no documented stacks
MGF
+ BPC-157
Multi-pathway
View BPC-157

MGF activates satellite cells for muscle fiber repair; BPC-157 promotes angiogenesis, collagen synthesis, and tendon healing via distinct pathways (VEGF, FAK, integrin signaling). Theoretical synergy in post-injury contexts combines myogenic (MGF) and stromal (BPC-157) repair mechanisms. Both lack human validation.

MGF
No established dose
BPC-157
250–500 mcg SQ near injury site
Context
Animal models only
Primary benefit
Theoretical multi-tissue repair (muscle + tendon/ligament)
+ TB-500
Moderate
View TB-500

TB-500 (thymosin beta-4 fragment) enhances actin polymerization, cell migration, and angiogenesis—complementary to MGF satellite cell activation. Both upregulated post-injury; combined use presumed additive for muscle regeneration in preclinical models.

MGF
No established dose
TB-500
2–5 mg SQ weekly
Context
Animal models only
Primary benefit
Satellite cell activation + enhanced migration/angiogenesis