ACE-031 vs RAD-140
Emerging vs Emerging
monitor Mechanism-based · 46% Both ACE-031 and RAD-140 suppress the HPTA axis. Combined suppression deepens shutdown and extends recovery time. Plan PCT accordingly and monitor LH/FSH/testosterone.
Molecular Data
ACE-031 RAD-140
Weight — 393.83 Da
Half-life 12-15 days ~60 hours
Type Soluble activin receptor type IIB-Fc fusion protein Nonsteroidal selective androgen receptor modulator (C20H16ClN5O2)
Key Benefits
ACE-031
01 Significant lean mass increases (up to 1.7% in 29 days) observed in Phase 1 trials
02 Simultaneous reduction in fat mass alongside muscle gains
03 Long half-life (12-15 days) allows infrequent dosing
04 Broad TGF-beta ligand neutralization for robust anti-catabolic effects
05 Dose-dependent increases in thigh muscle volume confirmed by MRI
RAD-140
01 Potent anabolic activity in muscle tissue with high oral bioavailability
02 Tissue-selective action sparing the prostate and other androgen-sensitive organs
03 No aromatization to estrogen (no estrogen-related side effects such as water retention or gynecomastia)
04 No conversion to DHT (reduced risk of hair loss and prostate stimulation compared to testosterone)
05 Long half-life (~60 hours) permitting convenient once-daily oral dosing
06 Neuroprotective properties observed in preclinical models
07 Increased lean body mass and reduced fat mass in preclinical studies
Dosing Protocols
ACE-031
0.5-3 mg/kg IV every 2 weeks (clinical research doses only) / Every 2 weeks
Phase 1 Research Protocol (Healthy Volunteers) 0.1-3 mg/kg Single IV dose
Phase 2 Research Protocol (DMD) 0.5-2.5 mg/kg Every 2 weeks
RAD-140
10-20 mg/day / Once daily (oral)
Side Effects
ACE-031
Nosebleeds (epistaxis) - most frequently reported adverse event
Gum bleeding
Telangiectasia (dilated small blood vessels visible on skin)
Skin erythema (redness)
Minor injection site reactions
RAD-140
Testosterone suppression (dose-dependent, occurs in virtually all users by week 4-6)
Liver enzyme elevation (ALT, AST increases reported in clinical and anecdotal data)
Hair shedding (temporary, typically resolves after discontinuation)
Headaches (most common in the first 1-2 weeks, often transient)
Nausea (mild, usually with initial doses or on an empty stomach)
Lipid disruption (HDL suppression, LDL elevation)
Mild insomnia or sleep disturbance
Reduced libido and mood changes related to testosterone suppression
Contraindications
NEVER approved for human use - clinical development discontinued
History of bleeding disorders or vascular malformations
Concurrent anticoagulant or antiplatelet therapy
Known hypersensitivity to Fc fusion proteins
Pregnancy or breastfeeding
Pre-existing liver disease or elevated liver enzymes at baseline
Hormone-sensitive cancers (prostate cancer, certain breast cancers not being treated under clinical supervision)
Pregnancy or potential pregnancy (teratogenic risk from androgen receptor agonism)
Breastfeeding
Age under 25 (incomplete endocrine system maturation and higher risk of HPG axis disruption)
Concurrent use of hepatotoxic medications without medical supervision
Known cardiovascular disease (insufficient safety data for this population)
Research Evidence
ACE-031 RAD-140
Status Emerging Emerging
References 4 studies 5 studies
Latest — July 2020
FDA Approved No No
This comparison is for educational and research purposes only. Consult a healthcare professional before use.