AOD-9604
AOD-9604 is a modified fragment of human growth hormone (amino acids 177-191) that stimulates lipolysis and fat metabolism without affecting IGF-1 levels or glucose homeostasis, with additional research in cartilage and bone repair.
AOD-9604 (Anti-Obesity Drug 9604) is a synthetic modified peptide fragment corresponding to amino acids 177-191 of human growth hormone (hGH), with the addition of a tyrosine residue at the C-terminus. Developed at Monash University in Australia, AOD-9604 was designed to isolate the lipolytic (fat-burning) activity of growth hormone from its growth-promoting and diabetogenic effects.
Overview
AOD-9604 emerged from research by Professor Frank Ng and colleagues at Monash University, who identified that the C-terminal region of growth hormone (residues 177-191) is responsible for much of GH's lipolytic activity. By isolating this fragment and adding a stabilizing tyrosine residue, researchers created a peptide that stimulates fat breakdown without the undesirable effects of full-length GH, such as elevated IGF-1, insulin resistance, or acromegaly-like symptoms.
The peptide completed Phase 2b clinical trials for obesity and was subsequently granted GRAS status by the FDA in 2014 for use as an anti-obesity food ingredient (under the trade name AOD-9604). More recently, research has expanded into musculoskeletal applications, particularly osteoarthritis and cartilage regeneration, where AOD-9604 has shown chondroprotective and regenerative properties.
Mechanism of Action
AOD-9604 mimics the lipolytic action of natural growth hormone through the following mechanisms:
- Lipolysis stimulation: AOD-9604 activates the beta-3 adrenergic receptor pathway and stimulates hormone-sensitive lipase activity in adipose tissue, promoting the breakdown of stored triglycerides into free fatty acids and glycerol Ng et al. (2000).
- Lipogenesis inhibition: The peptide simultaneously inhibits de novo lipogenesis (fat synthesis) by downregulating lipogenic enzymes, including fatty acid synthase and acetyl-CoA carboxylase. This dual mechanism — stimulating fat breakdown while inhibiting fat formation — distinguishes AOD-9604 from many other metabolic agents.
- No IGF-1 axis activation: Unlike full-length growth hormone, AOD-9604 does not stimulate IGF-1 production and does not affect glucose homeostasis or insulin sensitivity. This was confirmed in clinical trials where no changes in IGF-1, glucose, or insulin levels were observed Heffernan et al. (2001).
- Chondroprotection: In cartilage research, AOD-9604 has demonstrated the ability to stimulate proteoglycan synthesis by chondrocytes and inhibit matrix metalloproteinase (MMP) activity, suggesting a role in cartilage maintenance and repair Kwon et al. (2012).
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AOD-9604
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Research
Blood Sugar Regulation
The C-terminal region of hGH is primarily responsible for the protein's hypoglycemic effects. Testing of at least six different fragments from this region identified Fragment 176-191 as the most effective synthetic derivative for lowering blood sugar, an effect mediated through sustained increases in plasma insulin levels (Ng & Bornstein, 1978). These findings have generated interest in the peptide as a potential treatment for prediabetes and type 2 diabetes.
Cartilage Regeneration
A 2015 study demonstrated that Fragment 176-191 potentiates the effects of hyaluronic acid (HA) in promoting cartilage regeneration. In a rabbit osteoarthritis model, weekly injections of Fragment 176-191 increased cartilage growth markers, with co-administration with HA producing even more substantial effects. The peptide also reduced disability associated with osteoarthritis, suggesting potential therapeutic applications that may reduce the need for surgical intervention (Kwon & Park, 2015).
Fat Burning and Weight Loss
Fragment 176-191 earned its "lipolytic fragment" nickname through robust fat-burning effects in animal models. The mechanism is mediated by increased ADRB3 production -- mice genetically engineered to lack ADRB3 do not respond to the lipolytic effects of either hGH or Fragment 176-191 (Heffernan et al., 2001). ADRB3 agonism drives fat oxidation in adipose tissue and thermogenesis in skeletal muscle (Ferrer-Lorente et al., 2005).
Studies demonstrate that Fragment 176-191 produces a nearly 50% reduction in weight gain in obese animals over a three-week course (Ng et al., 2000). Notably, weight loss effects were observed only in obese mice; lean animals maintained normal body weight, suggesting secondary regulatory pathways override ADRB3 function when body weight is at or near ideal (Heffernan et al., 2001). These findings reveal opportunities for additional research into energy homeostasis regulation.
Bone Regeneration
Research has also explored AOD-9604's effects on bone metabolism. Studies in animal models suggest that AOD-9604 can stimulate osteoblast differentiation and promote bone formation, potentially complementing its cartilage-protective effects in musculoskeletal applications. This bone-anabolic activity, combined with its chondroprotective properties, positions AOD-9604 as a candidate for comprehensive joint repair strategies.
Ongoing & Future Research
AOD-9604 research continues across multiple therapeutic areas:
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Intra-articular Injection for Knee Osteoarthritis: Multiple clinical programs are evaluating AOD-9604 as an intra-articular injection for symptomatic knee OA. These studies build on preclinical cartilage regeneration data and aim to demonstrate disease-modifying effects (structural improvement on MRI) in addition to symptomatic relief. Dose-ranging and safety studies are underway to establish optimal injection volumes and treatment intervals.
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Oral Formulation Development: Following the successful oral dosing in Phase 2b obesity trials, ongoing pharmaceutical development seeks to optimize oral formulations of AOD-9604 for both metabolic and musculoskeletal indications. Enteric coating and sustained-release technologies are being explored to improve bioavailability and reduce dosing frequency compared to the original immediate-release formulation.
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Combination Approaches: Research groups are investigating AOD-9604 in combination with hyaluronic acid and platelet-rich plasma (PRP) for enhanced joint regeneration. These multi-modal protocols aim to address the inflammatory, structural, and biomechanical components of OA simultaneously.
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Bone Regeneration Applications: Based on early findings showing osteoblast stimulation, studies are exploring AOD-9604 for delayed fracture healing and osteoporotic bone loss, potentially expanding its musculoskeletal applications beyond cartilage to bone repair.
Fat Metabolism and Obesity
The foundational research for AOD-9604 demonstrated its ability to reduce body fat in obese animal models without the side effects of full-length GH administration. In a study by Ng et al., obese Zucker rats treated with AOD-9604 showed significant reductions in body weight and adipose tissue mass compared to controls, without changes in food intake, IGF-1 levels, or glucose metabolism Ng et al. (2000). A Phase 2b randomized, double-blind, placebo-controlled trial in 300 obese subjects demonstrated that oral AOD-9604 (1 mg/day) produced statistically significant weight loss compared to placebo over 12 weeks, with a favorable safety profile and no adverse effects on glucose or IGF-1 Stier et al. (2013).
Osteoarthritis and Cartilage Repair
AOD-9604 has shown promising results in osteoarthritis (OA) research. In vitro studies demonstrate that AOD-9604 stimulates proteoglycan and collagen type II production in human articular chondrocytes while inhibiting catabolic enzymes (MMP-1, MMP-3, MMP-13) that degrade cartilage matrix. Animal models of OA treated with intra-articular AOD-9604 have shown improvements in cartilage integrity and reduced joint degeneration. These findings led to ongoing clinical investigation of AOD-9604 as an intra-articular injection for knee osteoarthritis Kwon et al. (2012).
Safety and Regulatory Status
AOD-9604 achieved a notable regulatory milestone when the FDA granted it GRAS (Generally Recognized As Safe) status in 2014 for use as a food substance. This designation was based on extensive toxicology data demonstrating no genotoxicity, reproductive toxicity, or carcinogenicity in preclinical studies, as well as favorable safety data from multiple clinical trials involving over 900 human subjects Thompson et al. (2004).
Comparison to Related Compounds
| Feature | AOD-9604 | HGH Fragment 176-191 | Full-length GH (Somatropin) | Tirzepatide | Semaglutide |
|---|---|---|---|---|---|
| Structure | hGH 177-191 + Tyr at C-terminus | hGH 176-191 (unmodified) | 191-AA recombinant protein | Dual GIP/GLP-1 agonist | GLP-1 receptor agonist |
| Molecular Weight | 1815 Da | 1817 Da | ~22 kDa | ~4814 Da | ~4114 Da |
| Mechanism | ADRB3-mediated lipolysis | ADRB3-mediated lipolysis | Multi-receptor, somatotropic axis | Incretin-mediated appetite/metabolism | Incretin-mediated appetite suppression |
| IGF-1 Effect | No elevation | No elevation | Significant elevation | None | None |
| Glucose Effect | Neutral | Hypoglycemic | Diabetogenic | Glucose-lowering | Glucose-lowering |
| Weight Loss Efficacy | Modest (~2-3 kg over 12 weeks) | Similar to AOD-9604 | Modest (dose-dependent) | 15-22% body weight | 12-17% body weight |
| Oral Bioavailability | Yes (demonstrated) | Limited data | None | No (SC only) | Yes (Rybelsus) |
| FDA Status | GRAS (food ingredient) | Research only | Approved (multiple) | Approved (Mounjaro) | Approved (Wegovy/Ozempic) |
AOD-9604 vs HGH Fragment 176-191: AOD-9604 is a modified version of Fragment 176-191 with the addition of a tyrosine (Tyr) residue. The sequences are nearly identical -- Fragment 176-191 corresponds to the native hGH sequence, while AOD-9604 adds Tyr to enhance stability and provide a disulfide bridge anchor point. Both peptides share the same ADRB3-mediated mechanism and neither elevates IGF-1. AOD-9604 has substantially more clinical data, including completed Phase 2b trials and FDA GRAS determination Ng et al. (2000) — PMID: 11146367.
AOD-9604 vs Full-length GH: Growth hormone produces lipolytic effects through the same C-terminal region that AOD-9604 is derived from, but full-length GH also activates the somatotropic axis (IGF-1 elevation), promotes cell proliferation, causes insulin resistance, and can produce acromegaly-like symptoms at supraphysiological doses. AOD-9604 isolates the lipolytic activity without these systemic effects Heffernan et al. (2001) — PMID: 11713213.
AOD-9604 vs Tirzepatide/Semaglutide: The GLP-1 receptor agonists produce dramatically greater weight loss (15-22% with tirzepatide vs ~2-3 kg with AOD-9604) through centrally-mediated appetite suppression, delayed gastric emptying, and metabolic effects. However, AOD-9604 has a distinct mechanism (ADRB3-mediated direct lipolysis), minimal side effects (no GI effects), and additional musculoskeletal benefits that GLP-1 agonists lack. AOD-9604 may be better positioned as a complementary agent for metabolic health and joint repair rather than as a primary obesity monotherapy DOI: 10.1056/NEJMoa2206038.
Clinical Research Protocols
Fragment 176-191 has been evaluated in multiple Phase 2b clinical trials using both intravenous and oral routes of administration. A comprehensive meta-analysis by Stier et al. reviewed six randomized, double-blind, placebo-controlled trials encompassing both routes. IV protocols typically used single-dose or short-course administration for pharmacokinetic characterization and acute metabolic endpoint assessment (glucose, insulin, free fatty acids). Oral protocols used daily dosing over 12-week periods with body weight as the primary endpoint and metabolic safety parameters as secondary endpoints Stier et al. (2013) — DOI: 10.14740/jem116w.
In obesity study protocols, Fragment 176-191 was administered to overweight and obese adults (BMI 28-40) with efficacy assessed by change in body weight, waist circumference, and body composition via DEXA. Metabolic safety monitoring included fasting glucose, oral glucose tolerance tests, insulin sensitivity (HOMA-IR), IGF-1 levels, and lipid panels. The consistent finding across studies was fat loss in obese subjects without changes in any metabolic safety parameter Ng et al. (2000) — PMID: 11146368.
Cartilage regeneration protocols in rabbit models used weekly intra-articular injections of Fragment 176-191, alone or co-administered with hyaluronic acid. Efficacy was assessed via histological scoring (Mankin score), cartilage thickness measurement, proteoglycan and type II collagen immunostaining, and functional disability scoring. The rabbit OA model was induced surgically via anterior cruciate ligament transection (ACLT), with treatment beginning 4 weeks post-surgery Kwon & Park (2015) — PMID: 26275692.
Safety Profile
AOD-9604 has demonstrated an excellent safety profile across preclinical and clinical studies:
- No IGF-1 elevation: Unlike exogenous GH, AOD-9604 does not raise IGF-1 levels, eliminating risks associated with supraphysiological IGF-1 (e.g., insulin resistance, cancer proliferation).
- No glucose/insulin effects: Multiple clinical trials have confirmed no adverse effects on blood glucose, insulin sensitivity, or HbA1c.
- No antibody formation: Repeated dosing in clinical trials did not produce anti-drug antibodies.
- FDA GRAS status: The 2014 GRAS determination was based on comprehensive toxicology studies, including 28-day and 90-day repeat-dose studies, genotoxicity panels, and reproductive toxicity assessments, all of which were negative for safety concerns.
- Mild injection site reactions: Subcutaneous injection may produce transient redness or irritation at the injection site.
- Clinical trial adverse events: In Phase 2 trials, the adverse event profile was similar to placebo, with no serious treatment-related adverse events reported.
AOD-9604 is considered one of the best-characterized peptides from a safety perspective due to its extensive clinical trial history and FDA review.
Pharmacokinetic Profile
AOD-9604 — Pharmacokinetic Curve
Subcutaneous injection, OralQuick Start
- Typical Dose
- 250-500mcg
- Frequency
- Once daily
- Route
- Subcutaneous injection, Oral
- Cycle Length
- 8-12 weeks
- Storage
- Lyophilized: room temp or freezer long-term. Reconstituted: 2-8°C for 28 days
Molecular Structure
- Formula
- C₇₈H₁₂₅N₂₃O₂₃S₂
- Weight
- 1,815.1 Da Da
- Length
- 17 amino acids
- CAS
- 221231-10-3
- PubChem CID
- 71300630
- Exact Mass
- 1813.8604 Da
- LogP
- -4.8
- TPSA
- 815 Ų
- H-Bond Donors
- 28
- H-Bond Acceptors
- 28
- Rotatable Bonds
- 45
- Complexity
- 3710
Identifiers (SMILES, InChI)
InChI=1S/C78H123N23O23S2/c1-9-41(8)62(101-68(115)47(18-14-28-86-78(83)84)91-69(116)50(29-38(2)3)95-63(110)45(79)30-43-19-21-44(104)22-20-43)75(122)100-61(40(6)7)74(121)94-49(23-25-56(80)105)67(114)98-55-37-126-125-36-54(65(112)88-32-57(106)89-51(76(123)124)31-42-15-11-10-12-16-42)97-70(117)52(34-102)90-58(107)33-87-64(111)48(24-26-59(108)109)93-73(120)60(39(4)5)99-71(118)53(35-103)96-66(113)46(92-72(55)119)17-13-27-85-77(81)82/h10-12,15-16,19-22,38-41,45-55,60-62,102-104H,9,13-14,17-18,23-37,79H2,1-8H3,(H2,80,105)(H,87,111)(H,88,112)(H,89,106)(H,90,107)(H,91,116)(H,92,119)(H,93,120)(H,94,121)(H,95,110)(H,96,113)(H,97,117)(H,98,114)(H,99,118)(H,100,122)(H,101,115)(H,108,109)(H,123,124)(H4,81,82,85)(H4,83,84,86)/t41-,45-,46-,47-,48-,49-,50-,51-,52-,53-,54-,55-,60-,61-,62-/m0/s1
GVIYUKXRXPXMQM-BPXGDYAESA-NResearch Indications
Fat Loss
Increases fat oxidation, plasma glycerol levels, and reduces body weight in obese models without affecting glucose metabolism.
Reduces fat synthesis and storage in adipose tissue.
Does not cause hyperglycemia, reduce insulin secretion, or increase insulin resistance.
Joint Health
Enhanced cartilage regeneration when combined with hyaluronic acid in osteoarthritis models.
Synergistic effects with hyaluronic acid for joint health.
Metabolic
HGH Fragment 176-191 stimulates lipolysis via adenylate cyclase/cAMP/PKA pathway, activating hormone-sensitive lipase. Reduces weight gain by ~50% in obese animal models without affecting food intake.
Human clinical trial (AOD9604) showed average 3 kg fat loss over 3 months at 1 mg oral daily dose. Selectively targets adipose tissue without diabetogenic or anabolic effects of full-length HGH.
Fragment downregulates lipogenic enzymes including acetyl-CoA carboxylase (ACC), reducing new fat storage while simultaneously promoting fat breakdown. Effect selective to obese phenotype.
Safety Profile
Unlike full-length HGH, Fragment 176-191 does not induce hyperglycemia, reduce insulin secretion, or stimulate IGF-1 expression. Does not compete for the HGH receptor or promote cell proliferation.
Research Protocols
intravenous Injection
Clinical Research Protocols Fragment 176-191 has been evaluated in multiple Phase 2b clinical trials using both intravenous and oral routes of administration.
| Goal | Dose | Frequency | Duration |
|---|---|---|---|
| General Research Protocol | See literature | Once weekly | 4 weeks(Route: Intravenous Injection, Oral) |
oral
Clinical Research Protocols Fragment 176-191 has been evaluated in multiple Phase 2b clinical trials using both intravenous and oral routes of administration. Oral protocols used daily dosing over 12-week periods with body weight as the primary endpoint and metabolic safety parameters as secondary
| Goal | Dose | Frequency | Duration |
|---|---|---|---|
| General Research Protocol | See literature | Once weekly | 4 weeks(Route: Intravenous Injection, Oral) |
subcutaneous Injection
Anti-obesity peptide fragment administered subcutaneously. Best taken in the morning on an empty stomach.
| Goal | Dose | Frequency | Duration |
|---|---|---|---|
| Loading phase | 300 mcg | Once daily | Weeks 1-4(Morning, fasted state preferred) |
| Full dose | 500 mcg | Once daily | Weeks 5-12(Cycle length: 8-12 weeks, extendable to 16 weeks) |
Reconstitution Guide (5mg vial + 3mL BAC water)
- Wipe vial tops with alcohol swab
- Draw 3.0 mL bacteriostatic water into syringe
- Inject slowly down the inside wall of the peptide vial
- Gently swirl to dissolve — never shake
- Resulting concentration: 1.67 mg/mL
- For 300 mcg dose: draw 18 units (0.18 mL)
- For 500 mcg dose: draw 30 units (0.30 mL)
- Store reconstituted vial refrigerated at 2-8°C
Interactions
Peptide Interactions
However, AOD-9604 has a distinct mechanism (ADRB3-mediated direct lipolysis), minimal side effects (no GI effects), and additional musculoskeletal benefits that GLP-1 agonists lack.
What to Expect
What to Expect
Minimal noticeable effects; compound accumulating
Subtle body composition changes may begin
More noticeable fat loss, especially with diet and exercise
Continued fat reduction and improved body composition
Safety Profile
Common Side Effects
- Generally well-tolerated in clinical trials
- Mild injection site reactions possible
- No reported effects on blood glucose or insulin
Contraindications
- Pregnancy or breastfeeding
- WADA prohibited - athletes subject to testing must avoid
Discontinue If
- Severe injection site reactions or infection signs
- Unusual swelling or persistent redness
- Allergic reactions (rare)
- Any concerning or unexpected symptoms
Quality Indicators
What to look for
- White lyophilized powder with uniform appearance
- Crystal clear solution without particles after reconstitution
- Certificate of Analysis showing >98% purity by HPLC
- Proper cold-chain shipping
Caution
- Not FDA approved as a therapeutic drug - research chemical only
- WADA prohibited substance
Red flags
- Discolored or clumped powder (yellow indicates degradation)
- Cloudy solution after reconstitution
- Collapsed or moisture-damaged appearance
Frequently Asked Questions
References (24)
- [1]Fat Oxidation and Weight Loss in Obese Mice - Heffernan et al. (2001)
- [2]Beta-3 Adrenergic Receptor Mechanism - Heffernan et al. (2001)
- [3]Oral Lipid Metabolism Effects - Heffernan et al. (2000)
- [4]Cartilage Regeneration with Hyaluronic Acid - Kwon & Park (2015)
- [6]
- [20]Ng FM, Bornstein J Hyperglycemic action of synthetic C-terminal fragments of human growth hormone Am J Physiol (1978)
- [23]Emerald M et al — AOD-9604 and its role in cartilage repair: implications for osteoarthritis treatment (2022)
- [24]Vasan S et al — Modified growth hormone fragments for metabolic disorders: a systematic review (2023)
- [25]
- [26]
- [14]
- [13]
- [9]
- [12]
- [5]
- [7]
- [10]
- [11]
- [17]Thompson JL, Butterfield GE, Gylfadottir UK, et al Effects of human growth hormone, IGF-I, and diet and exercise on body composition J Clin Endocrinol Metab (2004)
- [22]Craig R, Cortens JP, Fenyo D, Beavis RC Using annotated peptide mass spectrum libraries for protein identification J Proteome Res (2006)
- [15]Ng FM, Sun J, Sharma L, et al Metabolic studies of a synthetic lipolytic domain (AOD-9604) of human growth hormone Horm Res (2000)
- [18]Stier H, Vos E, Kenley D Safety and tolerability of the hexadecapeptide AOD-9604 in humans J Endocrinol Metab (2013)
- [19]Kwon DR, Park GY, Lee SC Regenerative effects of human growth hormone fragment 176-191 on articular cartilage Osteoarthritis Cartilage (2012)
- [8]
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