# Metabolic mechanisms of cardioprotection through alpha-1A adrenergic receptor activation > **NIH NIH R01** · UNIV OF NORTH CAROLINA CHAPEL HILL · 2024 · $536,932 ## Abstract The heart consumes more ATP than any other organ, the vast majority of which is generated by fatty acid oxidation (FAO) coupled to oxidative phosphorylation (OXPHOS) in mitochondria. The sympathetic nervous system (SNS) regulates numerous aspects of mitochondrial function through activation of alpha-1-adrenergic receptors (α1-ARs) and beta-ARs (β-ARs) in cardiomyocytes, as we recently reviewed. Persistent stimulation of cardiac β-ARs causes pathological structural and metabolic changes resulting in myocardial energy depletion and heart failure (HF), but α1-ARs exert adaptive effects in the failing heart, mitigating the toxicity of chronic β-AR activation. The mechanisms underlying this cardioprotection remain largely unclear. There are three α1-AR subtypes: A, B, and D. Mounting evidence indicates that the α1A subtype protects cardiomyocytes against multiple types of injury. We previously published that a selective α1A agonist increases ATP content in anthracycline-exposed failing mouse hearts. Our preliminary data now show that permeabilized cardiac muscle fibers and isolated mitochondria from knockout mice lacking the αA-AR (α1AKO) exhibit decreased FAO and diminished activity of electron transport chain (ETC) Complex I and II. We also recently found that treatment with a selective α1A agonist enhances Complex I, II and IV activity in uninjured mouse hearts and protects cardiac energetic capacity and contractile function in mice subjected to experimental myocardial infarction. Collectively, these findings suggest a novel mechanism for α1A-mediated cardioprotection, as regulation of neither FAO nor OXPHOS by β1-ARs has been studied previously. We now propose three Specific Aims to build upon our published findings and novel preliminary data to test the central hypothesis that α1A-ARs metabolically support the uninjured heart and protect the failing heart by enhancing mitochondrial oxidative capacity. Aim 1 will determine whether α1A-ARs enhance OXPHOS in the heart through cardiomyocyte-autonomous effects using our cardiomyocyte-specific β1A knockout mice, novel focused studies of α1A skeletal muscle FAO regulation, and a high fat diet model. Aim 2 will find if α1A-ARs preserve energetic capacity through maintenance of long chain FAO and regulation of ETC enzyme activity, coupling in vivo profiling of α1A knockout and α1A agonist treated mouse hearts with mechanistic in vitro approaches. Aim 3 will test whether selective α1A-AR agonists act as mitotropes—drugs that enhance mitochondrial function--to protect against HF using three clinically relevant mouse models: chronic isoproterenol infusion, cardiomyocyte-specific loss of FAO (Carnitine palmitoyl transferase 2 knockout), and a Duchenne Muscular Dystrophy model in which Complex I activity is impaired. If successfully completed, the proposed experiments have the potential to significantly expand our understanding of SNS regulation of cardiomyocyte mitochondrial function, elucidating new mechanis... ## Key facts - **NIH application ID:** 10766274 - **Project number:** 5R01HL140067-07 - **Recipient organization:** UNIV OF NORTH CAROLINA CHAPEL HILL - **Principal Investigator:** Brian C Jensen - **Activity code:** R01 (R01, R21, SBIR, etc.) - **Funding institute:** NIH - **Fiscal year:** 2024 - **Award amount:** $536,932 - **Award type:** 5 - **Project period:** 2017-12-15 → 2027-12-31 ## Primary source NIH RePORTER: https://reporter.nih.gov/project-details/10766274 ## Citation > US National Institutes of Health, RePORTER application 10766274, Metabolic mechanisms of cardioprotection through alpha-1A adrenergic receptor activation (5R01HL140067-07). Retrieved via AI Analytics 2026-05-27 from https://api.ai-analytics.org/grant/nih/10766274. Licensed CC0. --- *[NIH grants dataset](/datasets/nih-grants) · CC0 1.0*