Product DescriptionAICAR Peptide | Buy AICAR UK | Research Use OnlyAICAR — also known as Acadesine, AICA Riboside, and 5-Aminoimidazole-4-carboxamide ribonucleoside — is a naturally occurring nucleoside analogue and intermediate in the purine biosynthesis pathway that, when administered exogenously in research settings, is taken up into cells via nucleoside transporters and phosphorylated to ZMP (AICAR monophosphate), an AMP-mimetic that allosterically activates AMP-activated protein kinase (AMPK) — the master cellular energy sensor — triggering a coordinated downstream shift toward fat oxidation, glucose uptake, mitochondrial biogenesis, and suppression of anabolic energy-consuming pathways, making it the most widely used pharmacological AMPK activator and exercise mimetic in pre-clinical metabolic research. Buy AICAR in the UK from Peptides Lab UK with >99% HPLC-verified purity, batch-specific COA, and fast UK dispatch for laboratory and in vitro research use only.Distributed by Peptides Lab UK in lyophilised format for controlled laboratory research. Each batch is independently verified for purity. This compound is handled strictly in pre-clinical settings with no applications in human or veterinary medicine.What Is AICAR?AICAR (5-Aminoimidazole-4-carboxamide-1-β-D-ribofuranoside) is a synthetic cell-permeable nucleoside analogue and naturally occurring intermediate in the de novo purine biosynthesis pathway. Under normal physiological conditions, AICAR is present only transiently and at very low intracellular concentrations. When supplied exogenously in research models, it is transported into cells by the equilibrative nucleoside transporter ENT1 and rapidly phosphorylated by adenosine kinase to yield ZMP — the active intracellular species that mimics elevated AMP concentrations to engage the AMPK signalling cascade.AICAR was first studied in the 1980s as a cardioprotective agent through its relationship with adenosine signalling. Its role as a direct AMPK activator was formally established in 1995 by Corton et al., following Sullivan et al.’s earlier demonstration that the intracellular nucleotide form of AICAR (ZMP) mimicked the allosteric effects of AMP on rat liver AMPK. Since then, AICAR has become the most extensively used pharmacological tool for studying AMPK biology across virtually every metabolic tissue type and disease model.AICAR is classified as a prohibited substance under WADA regulations due to its metabolic activity profile in exercise models — making it relevant to both metabolic research and anti-doping assay development.Also Known AsAcadesineAICA Riboside / AICA-rAICAr5-Aminoimidazole-4-carboxamide ribonucleosideZMP precursor (intracellular active form: ZMP)CAS No. 2627-69-2How Does AICAR Work?Cellular Uptake and ZMP ConversionAICAR enters cells primarily via the equilibrative nucleoside transporter ENT1 — a well-characterised, widely expressed nucleoside uptake pathway that does not require receptor-mediated internalisation. Once inside, adenosine kinase phosphorylates AICAR to its active form, ZMP (5-aminoimidazole-4-carboxamide ribonucleotide), which accumulates intracellularly and mimics the effects of elevated AMP on the AMPK system.AMPK Activation — Allosteric and Phosphorylation MechanismsZMP binds to the γ subunit of AMPK, allosterically activating the enzyme and stimulating upstream phosphorylation at Thr172 by liver kinase B1 (LKB1). ZMP binding also protects the Thr172 phosphorylation site from dephosphorylation, sustaining AMPK activation. Detection of pThr172 AMPK by Western blot in cell lysates following AICAR treatment is the standard assay methodology for confirming AMPK engagement in any given tissue or cell type.AMPK-Dependent Downstream EffectsActivated AMPK coordinates a wide programme of downstream metabolic adaptations:GLUT4 translocation — increased glucose transporter expression and translocation to the plasma membrane in skeletal muscle cells, driving insulin-independent glucose uptakeFatty acid oxidation — phosphorylation and inhibition of acetyl-CoA carboxylase (ACC), reducing malonyl-CoA and de-suppressing carnitine palmitoyltransferase-1 (CPT1) to promote mitochondrial fatty acid import and oxidationmTORC1 inhibition — AMPK phosphorylates TSC2 and Raptor to suppress mTOR complex 1, inhibiting protein synthesis, ribosome biogenesis, and lipogenesisPGC-1α upregulation — AMPK drives expression of peroxisome proliferator-activated receptor gamma coactivator 1-alpha, promoting mitochondrial biogenesis and oxidative fibre gene expressionAutophagy and mitophagy — AMPK phosphorylates ULK1 at Ser555, initiating autophagosome assembly and selective mitochondrial clearance (mitophagy)p53/p21 pathway — in stem cell and cancer models, AICAR-mediated AMPK activation engages p53/p21 to induce G1/S cell cycle arrest and modulate differentiationAMPK-Independent Mechanisms — An Important Research DistinctionA major body of published research has established that several effects previously attributed to AMPK following AICAR administration are in fact AMPK-independent. These include direct interference with purine and pyrimidine nucleotide synthesis (via ZMP’s role as a substrate in the purine biosynthesis pathway), adenosine pathway modulation (AICAR competes for nucleoside transporters and inhibits adenosine deaminase, raising extracellular adenosine concentrations), and direct activation of the Akt/PI3K pathway independently of AMPK. This AMPK-independent profile makes AICAR both a more complex research tool and a broader-spectrum metabolic probe than a selective AMPK activator — and is a critical consideration in experimental design and result interpretation.Adenosine Pathway ModulationAICAR shares structural similarities with adenosine and competes for nucleoside transporters, increasing extracellular adenosine concentrations. It also inhibits adenosine deaminase and shifts ATP catabolism toward adenosine production rather than inosine — a mechanism exploited in its original cardioprotective research applications, where elevated adenosine reduces ischaemia-reperfusion injury.What Does AICAR Do in Research?In laboratory and pre-clinical settings, AICAR has been studied as the defining pharmacological AMPK activator and exercise mimetic reference compound across a broad spectrum of metabolic and disease research. Applications include:AMPK biology — Thr172 phosphorylation, γ-subunit allosteric activation, LKB1-mediated upstream signalling, and AMPK isoform profilingExercise mimetic research — metabolic gene induction, oxidative fibre remodelling, and endurance capacity in sedentary animal modelsSkeletal muscle glucose uptake — GLUT4 translocation, insulin-independent glucose handling, and insulin resistance modelsFatty acid oxidation — ACC phosphorylation, CPT1 de-suppression, malonyl-CoA reduction, and lipid oxidation fluxMitochondrial biogenesis — PGC-1α upregulation, OXPHOS gene expression, mitochondrial mass and morphologyAutophagy and mitophagy — ULK1 Ser555 phosphorylation, autophagosome formation, and mitochondrial quality controlmTOR/mTORC1 signalling — TSC2 and Raptor phosphorylation, S6K1 and 4E-BP1 downstream effects, and anabolic pathway suppressionObesity and metabolic syndrome models — high-fat diet rodent models, adiposity, lipid profiles, and insulin sensitivityType 2 diabetes and glucose homeostasis — fasting glucose, glucose tolerance, and insulin resistance reversal in pre-clinical modelsCardiovascular and cardiac ischaemia research — adenosine pathway modulation, ischaemia-reperfusion protection, and cardiac AMPK biologyCancer cell biology — AMPK/mTOR crosstalk, cell cycle arrest, apoptosis modulation, nucleotide synthesis interference, and metabolic stress vulnerabilityCLL and haematological malignancy models — acadesine’s AMPK-independent pro-apoptotic activity in lymphoid cell lines and relapsed/refractory CLL researchStem cell biology — pluripotency gene network modulation (Klf4, Klf2, Nanog, Oct4, Sox2), ES cell self-renewal, and osteogenic/adipogenic differentiation researchDiabetic neuropathy models — AMPK-mediated mitophagy, DRG neuronal mitochondrial bioenergetics, and neuroprotection in T1D and T2D mouse modelsNeuroinflammation and neuroprotection — AMPK-dependent anti-inflammatory signalling and oxidative stress modulation in neuronal systemsAnti-doping assay development — AICAR detection methodology for WADA-regulated analytical researchAMPK-independent pharmacology — dissection of ZMP-mediated purine/pyrimidine biosynthesis interference and adenosine pathway effects independent of AMPK statusWhat Do Studies Say About AICAR?AICAR as the Founding AMPK ActivatorThe foundational 1995 work by Corton et al. established AICAR as the first cell-permeable AMPK activator for use in intact cells, building on Sullivan et al.’s prior confirmation that ZMP mimicked AMP’s allosteric effects on AMPK. Together, these studies created the methodological framework used in thousands of subsequent AMPK research publications — making AICAR the most historically cited pharmacological AMPK tool in the literature.The Exercise Mimetic Study — 44% Endurance ImprovementThe landmark 2008 study by Narkar, Evans et al. published in Cell demonstrated that 4 weeks of AICAR treatment in sedentary mice — without any exercise training — induced a programme of oxidative metabolic gene expression in skeletal muscle and enhanced treadmill running endurance by 44%. Combined AICAR treatment and exercise training produced synergistic increases in oxidative myofibre content and endurance beyond either intervention alone, establishing AICAR as a true exercise mimetic and anchoring the AMPK-PGC-1α axis as a druggable target for metabolic reprogramming research.AMPK-Independent Effects — A Critical Systematic ReviewThe comprehensive 2021 systematic review by Dembitz, Lalic et al. published in International Journal of Molecular Sciences catalogued the evidence base for AICAR’s AMPK-independent effects — including direct interference with nucleotide synthesis, adenosine pathway modulation, and Akt/PI3K activation — and called for caution in interpreting AICAR-based studies as evidence of pure AMPK biology. This review is essential reading for researchers using AICAR, as it recontextualises a significant portion of the existing AMPK literature and identifies research areas where AMPK-independent effects are most likely to confound results.CLL and Cancer ResearchAcadesine has been evaluated in clinical trials in patients with relapsed and refractory chronic lymphocytic leukaemia (CLL). Pre-clinical work confirmed selective cytotoxic activity in CLL cell lines through an AMPK-independent mechanism, establishing the drug as a candidate research compound for haematological malignancy models. Multiple phase I and II trials provided pharmacokinetic and safety data used to characterise the acadesine backbone.Diabetic Polyneuropathy ModelsA 2024/2025 study published in International Journal of Molecular Sciences confirmed that AICAR treatment prevented and reversed experimental diabetic polyneuropathy in both T1D and T2D mouse models. AICAR increased pAMPK in dorsal root ganglion (DRG) neuronal extracts by 3-fold in HFD-fed mice, promoted ULK1 Ser555 phosphorylation and LC3-II-mediated mitophagy, and restored ADP-stimulated state 3 mitochondrial respiration in DRG neurons — establishing a mitophagy-dependent neuroprotective mechanism in diabetic nerve disease models.Stem Cell PluripotencyMicroarray analysis of AICAR-treated mouse embryonic stem cells confirmed significant upregulation of pluripotency-associated genes (Klf4, Klf2, Nanog, Oct4, Myc, Sox2) and downregulation of differentiation-associated transcription factors — demonstrating that AICAR engages both AMPK and non-AMPK pathways (including BMP, MAPK, and TGF-β) to modulate stem cell fate decisions and epigenetic modification.Key Cited StudiesCorton JM et al. (1995) — 5-Aminoimidazole-4-carboxamide ribonucleoside. A specific method for activating AMP-activated protein kinase in intact cells? Eur J Biochem 229(2):558–565. PMID: 7744080Sullivan JE et al. (1994) — Inhibition of lipolysis and lipogenesis in isolated rat adipocytes with AICAR, a cell-permeable activator of AMP-activated protein kinase. FEBS Lett 353(1):33–36. DOI: 10.1016/0014-5793(94)01006-4Narkar VA et al. (2008) — AMPK and PPARδ agonists are exercise mimetics. Cell 134(3):405–415. DOI: 10.1016/j.cell.2008.06.051. PMID: 18674809Dembitz V & Lalic H (2021) — AICAr, a widely used AMPK activator with important AMPK-independent effects: a systematic review. Int J Mol Sci 22(10):5271. DOI: 10.3390/ijms22105271. PMC8147799Van Den Neste E et al. (2010) — AICA-riboside (acadesine), an activator of AMP-activated protein kinase with potential for application in hematologic malignancies. Expert Opin Investig Drugs 19(5):571–578. DOI: 10.1517/13543781003703694Adamo A et al. (2012) — LKB1 regulates DNA damage-induced apoptosis in a cell-type-specific manner in pre-clinical models. (See also: AICAR in ES cell pluripotency — Shi et al. and Adamo et al. cited in STEMCELL Technologies product literature)Azmi S et al. (2024/2025) — Administration of AICAR, an AMPK activator, prevents and reverses diabetic polyneuropathy by regulating mitophagy. Int J Mol Sci 26(1):80. DOI: 10.3390/ijms26010080AICAR vs Other AMPK Activators and Exercise Mimetics in ResearchFeatureAICAR (Acadesine)MetforminGW501516 (Cardarine)Compound 991Primary MechanismZMP-mediated AMPK allosteric activationComplex I inhibition → AMPK indirect activationPPARδ agonistDirect AMPK β1/β2 activatorAMPK SelectivityModerate — significant AMPK-independent effectsLow — broad mitochondrial/metabolic effectsNot AMPK-dependentHigh — direct allosteric AMPK activatorCell PermeabilityHigh (ENT1 transporter)ModerateHigh (passive diffusion)ModerateZMP ConversionYes — active intracellular speciesNoNoNoPurine Synthesis InterferenceYes (AMPK-independent)NoNoNoAdenosine Pathway EffectsYes — adenosine deaminase inhibition, extracellular adenosine elevationNoNoNoGlucose UptakeYes — GLUT4 translocation (skeletal muscle)Yes — hepatic glucose output reductionPartialYesFatty Acid OxidationYes — ACC phosphorylation, CPT1 activationYesYes (primary mechanism)YesMitochondrial BiogenesisYes — PGC-1α upregulationYesYes — PPARδ-drivenYesExercise Mimetic EvidenceYes — 44% endurance improvement (sedentary mice)NoYes — PPARδ-driven enduranceLimitedCancer / CLL ResearchYes — CLL clinical trials, cell cycle arrestYes — broad cancer metabolismLimitedNoWADA ProhibitedYesNoYesNoBest Research UseAMPK biology reference, exercise mimetic, metabolic studiesHepatic glucose/insulin research, AMPK indirect effectsPPARδ and endurance referenceSelective AMPK activation without purine biosynthesis interferenceQuality & Purity AssuranceEvery batch of AICAR from Peptides Lab UK is:>99% pure — HPLC and mass spectrometry verifiedSupplied with a full Certificate of Analysis (COA) on requestLyophilised powder for maximum stability and long shelf lifeManufactured under strict, controlled laboratory conditionsConsistent batch-to-batch quality for reproducible research resultsBuy AICAR UK — Product SpecificationsPropertyDetailFull NameAICAR / Acadesine / AICA RibosideAlso Known As5-Aminoimidazole-4-carboxamide ribonucleoside, AICAr, ZMP precursorCAS Number2627-69-2Molecular FormulaC₉H₁₄N₄O₅Molecular Weight258.23 g/molActive Intracellular FormZMP (phosphorylated by adenosine kinase)Primary TargetAMP-activated protein kinase (AMPK) — γ subunitPurity>99% (HPLC verified)FormLyophilised powderStorageStore dry at -20°C; protect from lightSolubilitySterile water or PBS; highly water-solubleAICAR Research ApplicationsAICAR (Acadesine) UK is supplied strictly for the following in vitro and pre-clinical research uses:AMPK activation — Thr172 phosphorylation, allosteric activation, LKB1 upstream signalling, and AMPK isoform characterisationExercise mimetic research — oxidative gene induction, PGC-1α/mitochondrial biogenesis, and endurance modelling in sedentary animal modelsSkeletal muscle glucose uptake — GLUT4 translocation, insulin-independent glucose handling, and insulin resistance modelsFatty acid oxidation — ACC phosphorylation, CPT1 activity, and lipid oxidation flux studiesmTOR/mTORC1 suppression and anabolic pathway inhibition researchAutophagy and mitophagy — ULK1 Ser555 signalling and mitochondrial quality control researchObesity, type 2 diabetes, and metabolic syndrome pre-clinical modelsCardiac ischaemia-reperfusion protection and adenosine pathway biologyCancer cell metabolism — AMPK/mTOR crosstalk, cell cycle arrest, and nucleotide synthesis interferenceCLL and haematological malignancy research — acadesine’s AMPK-independent cytotoxic mechanismsStem cell pluripotency and differentiation — ES cell fate decision and epigenetic modification researchDiabetic neuropathy models — AMPK-mediated mitophagy and DRG neuronal mitochondrial functionAMPK-independent pharmacology research — purine/pyrimidine biosynthesis and adenosine pathway dissectionAnti-doping and WADA-prohibited compound detection methodology developmentWhy Buy AICAR UK from Peptides Lab UK?Peptides Lab UK is a trusted UK peptides supplier providing research-grade compounds verified by independent HPLC testing. When you buy AICAR in the UK from us, you receive:99% purity, HPLC and MS verified, third-party testedFull COA documentation per batchFast same-day UK dispatch with tracked deliveryCompetitive pricing with bulk research discounts availableTrusted by researchers across the UK and EuropeResearch DisclaimerAll products supplied by Peptides Lab UK are intended strictly for in vitro laboratory research and scientific study use only. They are not intended for human consumption, veterinary use, or any medical or therapeutic application. AICAR (Acadesine) is not a licensed medicine or drug and has not been approved by the MHRA or FDA for use outside of its limited historical clinical trial contexts in cardiac ischaemia and haematological malignancy. AICAR is classified as a prohibited substance under WADA anti-doping regulations and is not approved for use in competitive sport. All research citations on this page relate to pre-clinical studies and peer-reviewed pharmacological research and do not constitute a claim of safety or therapeutic efficacy in humans. Peptides Lab UK accepts no liability for any misuse of research compounds. By purchasing, you confirm that you are a qualified researcher and that the product will be used solely within a controlled laboratory environment in compliance with all applicable UK laws, regulations, and institutional guidelines.






