Amanda L. Sharpe, Ph.D.

Assistant Professor

Pharmaceutical Sciences

Phone (405) 271-6593 x47243

Fax (405) 271-7505

Email amanda-sharpe@ouhsc.edu


Summary

The Sharpe lab is interested in understanding the contribution of neuropeptides such as proopiomelanocortin, neurotensin, and corticotropin releasing factor to addiction, obesity, and age-related cognitive impairment, and in the development of therapeutics to treat these conditions. We use behavioral (operant conditioning), anatomical, pharmacological, and molecular approaches to address our research questions, often in combination with genetic mouse models. We are interested in the normal physiological role for these neuropeptides, as well as the adaptations that occur in this neurocircuitry under the conditions of obesity, food restriction, and chronic drug use. The long-term goals of our lab are to 1) elucidate the pharmacology and neurocircuitry involved in the regulation of appetite for and consumption of rewards (both food and drug), and 2) to determine the contribution of hypothalamic neuropeptides to age-related conditions such as obesity and cognitive decline.



Grants

Effect of obesity on proopiomelanocortin regulation of reward and feeding

Presbyterian Health Foundation

07/01/2018 - 06/30/2019

Effects of dietary restriction on age-related neurophysiological adaptations: From behavior to single dopaminergic neurons

Oklahoma Medical Research Foundation

05/01/2018 - 04/30/2021


Publications & Presentations

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    21. Pastor R, Reed C, Burkhart-Kasch S, Li N, Sharpe A, Coste S C, Stenzel-Poore M P, Phillips T J. Ethanol concentration-dependent effects and the role of stress on ethanol drinking in corticotropin-releasing factor type 1 and double type 1 and 2 receptor knockout mice. Psychopharmacology. 2011; 218 : 169-77

    22. Sharpe A, Phillips T J. Central urocortin 3 administration decreases limited-access ethanol intake in nondependent mice. Behavioural pharmacology. 2009; 20 : 346-51

    23. Sharpe A, Low M J. Proopiomelanocortin peptides are not essential for development of ethanol-induced behavioral sensitization. Alcoholism, clinical and experimental research. 2009; 33 : 1202-7

    24. Sharpe A, Coste S C, Burkhart-Kasch S, Li N, Stenzel-Poore M P, Phillips T J. Mice deficient in corticotropin-releasing factor receptor type 2 exhibit normal ethanol-associated behaviors. Alcoholism, clinical and experimental research. 2005; 29 : 1601-9

    25. Sharpe A, Tsivkovskaia N O, Ryabinin A E. Ataxia and c-Fos expression in mice drinking ethanol in a limited access session. Alcoholism, clinical and experimental research. 2005; 29 : 1419-26

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Grants

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    1. Role of estrogen receptor-alpha in aging and sex-specific responses to 17 alpha-estradiol. NIH. Start Date: 2021. End Date: 2026.

    2. Plasticity of GABA input to VTA dopamine neurons in opioid use disorders. Misc Federal. Start Date: 2021. End Date: 2025.

    3. The role of melanocortin-4 receptors on astrocytes in the hypothalamus on inflammaging, adiposity, and weight regulation. Non-federal. Start Date: 2023.

    4. Astrocytic melanocortin 4 receptors and their role in inflammation and obesity. Intramural Funding. Start Date: 2022. End Date: 2023.

    5. The role of proopiomelanocortin neurons in age-related cognitive decline. NIH. Start Date: 2019. End Date: 2022.

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Awards and Honors

                                                                                            1. . Harold Hamm Diabetes Center Travel Award. Date: 2019.  




Education

                                                                                            1.  Degree: Post-doctoral fellowship. Oregon Health Sciences University. Date: 2008.  

                                                                                            2.  Degree: Ph D. Wake Forest University. Date: 2002.  

                                                                                            3.  Degree: B. Pharm. Ohio Northern University. Date: 1997.  




Administrative Assignments


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