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Commonly combined with ChemAesthetic AOD9604 5mg in research protocols.
Ratings are based on published research data and are for informational purposes only.
AOD9604 is a 16-amino-acid fragment of hGH (176–191) that mimics the lipolytic action of GH without affecting IGF-1 or insulin. Phase II/III trials in obese patients demonstrated significant fat loss without the hyperglycaemic or anti-lipolytic side effects of full-length GH. Its short half-life and lack of anabolic activity make it suitable for metabolic research protocols.
Research Post
AOD-9604 (anti-obesity drug 9604) is a 16-amino-acid synthetic peptide corresponding to residues 177-191 of human growth hormone with a tyrosine residue at the N-terminus (Tyr-hGH 177-191), and a disulphide-bridged cyclic conformation. It was specifically developed to isolate the lipolytic activity of GH's C-terminal domain while eliminating anabolic, diabetogenic, and mitogenic effects associated with full-length GH.
Full-length GH has well-characterised lipolytic effects via stimulation of hormone-sensitive lipase (HSL) in adipocytes, promoting hydrolysis of stored triglycerides. However, GH also has anabolic effects on muscle and bone (via IGF-1), promotes insulin resistance, and stimulates cell proliferation through IGF-1R-mediated pathways — effects that are undesirable in an obesity treatment agent. The hypothesis behind AOD-9604 was that the lipolytic activity resides in a specific region of the GH molecule separable from its growth-promoting activity.
Research at Monash University identified the C-terminal region (residues 177-191) as the lipid metabolism regulatory domain of GH. AOD-9604 was synthesised to test whether this fragment could stimulate lipolysis in isolation, and subsequent work demonstrated it retains potent lipolytic activity without activating the GH receptor for anabolic or glycaemic signalling.
AOD-9604 does not bind or activate the classical GH receptor (GHR) at the binding sites that trigger JAK2-STAT5 signalling and subsequent IGF-1 production. Instead, it appears to directly activate β-3 adrenergic receptors on adipocytes and may interact with a distinct binding site on fat cells that triggers cAMP-mediated HSL activation. Importantly, AOD-9604 does not increase IGF-1 levels, does not produce insulin resistance, and does not stimulate bone or muscle growth — confirming the intended separation of activities.
Metabolic Pharmaceuticals (Australia) conducted an extensive clinical programme in obesity:
In 2014, the FDA granted AOD-9604 Generally Recognized As Safe (GRAS) status as a food ingredient, reflecting its established safety profile across the clinical programme. This is a notable regulatory milestone for a synthetic peptide and confirms the extensive human safety data generated during its development.
Subsequent to the obesity programme, research has investigated AOD-9604 in osteoarthritis and cartilage repair models. Preclinical data from Monash University demonstrated that AOD-9604 stimulates chondrocyte proliferation, proteoglycan synthesis, and cartilage matrix repair independent of its lipolytic effects. Phase II trials in knee osteoarthritis (Syngen study) showed improvements in pain and function scores, opening a new research direction for this compound.
