ACE-031
Emerging researchMyostatin Inhibitor | Experimental Muscle Growth
ACE-031 is a soluble form of the activin type IIB receptor (ActRIIB) fused to an IgG1 Fc domain.
Molecular & research data
- Half-life
- 12-15 days
- Primary targets
- actriib, myostatin, tgf-beta
- Routes (research)
- Injectable
- Storage
- 2-8°C; protect from light. Not commercially available.
Overview
ACE-031 is a soluble form of the activin type IIB receptor (ActRIIB) fused to an IgG1 Fc domain. It functions as a decoy receptor, binding and neutralizing myostatin and other TGF-beta superfamily members that normally limit muscle growth. Originally developed by Acceleron Pharma for Duchenne muscular dystrophy (DMD), ACE-031 reached Phase 2 clinical trials before development was halted due to vascular side effects including nosebleeds and telangiectasia. In healthy volunteers, a single dose produced significant increases in lean mass and reductions in fat mass within 29 days.
Mechanism of action
ACE-031 acts as a ligand trap for members of the TGF-beta superfamily. By mimicking the extracellular domain of the ActRIIB receptor, it intercepts myostatin (GDF-8), activin A, activin B, and GDF-11 before they can bind cell-surface receptors and activate Smad2/3 signaling. Blocking this pathway removes the natural brake on muscle protein synthesis and satellite cell proliferation, resulting in rapid skeletal muscle hypertrophy. The Fc fusion domain extends circulating half-life through FcRn-mediated recycling and provides bivalent ligand binding.
Key research findings
- Significant lean mass increases (up to 1.7% in 29 days) observed in Phase 1 trials
- Simultaneous reduction in fat mass alongside muscle gains
- Long half-life (12-15 days) allows infrequent dosing
- Broad TGF-beta ligand neutralization for robust anti-catabolic effects
- Dose-dependent increases in thigh muscle volume confirmed by MRI
Research applications
Muscle Growth
- Muscle Hypertrophy — Phase 1 data showed statistically significant lean mass increases (average +1.7%) after a single IV dose in healthy postmenopausal women.
- Muscular Dystrophy — Phase 2 trial in DMD patients showed improvements in lean body mass and bone mineral density, but trial was halted due to vascular adverse events.
- Muscle Wasting / Cachexia — Preclinical models demonstrate robust prevention of muscle loss in disease states through myostatin pathway inhibition.
Body Composition
- Fat Loss — Phase 1 trial subjects showed concurrent fat mass reductions alongside lean mass gains, suggesting favorable nutrient partitioning.
- Bone Density — DMD trial data showed increases in bone mineral density, consistent with known effects of ActRIIB pathway modulation on bone metabolism.
ACE-031 FAQ
Why did ACE-031 development stop if it showed such impressive muscle gains?+
ACE-031 was halted during Phase 2 clinical trials due to serious vascular side effects including recurrent nosebleeds, gum bleeding, and telangiectasia (dilated small blood vessels visible on skin). These dose-limiting adverse events suggested off-target effects on vascular homeostasis that outweighed the muscle-building benefits, making further development unsafe.
How much muscle can ACE-031 actually build in humans?+
Phase 1 data in healthy postmenopausal women showed statistically significant lean mass increases (+1.7%) and thigh muscle volume increases (+5.1%) after a single IV dose within 29 days. However, development never progressed to Phase 3, so real-world efficacy at therapeutic doses and long-term safety remain unproven in larger populations.
Can I use ACE-031 as a research chemical if I can find it?+
ACE-031 has never been approved for human use and clinical development was discontinued. Any product sold as ACE-031 is of unknown origin and quality. The compound is a complex fusion protein sensitive to degradation, making DIY sourcing extremely risky with high contamination likelihood.
Does ACE-031 work through a different mechanism than myostatin inhibitors like follistatin?+
No. ACE-031 is a soluble activin receptor that acts as a ligand trap, while follistatin directly binds myostatin. Both ultimately inhibit myostatin signaling, but through different mechanisms. Theoretically combined use might be synergistic, but clinical data on combinations doesn't exist.
References
- [1]A soluble activin receptor type IIB (ACE-031) increases lean body mass and muscle strength in healthy postmenopausal womenJournal of Clinical Endocrinology & Metabolism
- [2]A phase 2 trial of ACE-031, a soluble activin receptor type IIB, in boys with Duchenne muscular dystrophyNeuromuscular Disorders
- [3]Pharmacokinetic, pharmacodynamic, and safety results from a first-in-human study of ACE-031, a novel activin receptor type IIB/Fc fusion proteinJournal of Clinical Pharmacology
- [4]Myostatin inhibition in health and diseaseAnnual Review of Cell and Developmental Biology
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Last reviewed: 2026-06-26. Information is provided for research and educational reference only — see our disclaimer.