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Neuroendocrine mechanisms of behavioral changes induced by hypoglycemia
Park, Min Jung
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https://hdl.handle.net/2142/17052
Description
- Title
- Neuroendocrine mechanisms of behavioral changes induced by hypoglycemia
- Author(s)
- Park, Min Jung
- Issue Date
- 2010-08-31T20:30:38Z
- Director of Research (if dissertation) or Advisor (if thesis)
- Freund, Gregory G.
- Doctoral Committee Chair(s)
- Donovan, Sharon M.
- Committee Member(s)
- Freund, Gregory G.
- Johnson, Rodney W.
- Woods, Jeffrey A.
- Department of Study
- Nutritional Sciences
- Discipline
- Nutritional Sciences
- Degree Granting Institution
- University of Illinois at Urbana-Champaign
- Degree Name
- Ph.D.
- Degree Level
- Dissertation
- Keyword(s)
- insulin
- hypoglycemia
- social exploration
- social withdrawal
- depression
- depressive-like behavior
- adrenergic receptors
- antidepressants
- norepinephrine
- epinephrine
- corticosterone
- mice
- Abstract
- Hypoglycemia is associated with a variety of adverse behaviors including fatigue, confusion, social withdrawal, anhedonia and depressive-like behaviors. While these clinical symptoms are well characterized, the mechanisms of their cause are not understood. Here, we investigated how insulin-induced hypoglycemia causes social withdrawal and changes in mood. To investigate effects on social withdrawal, male 8-12-week-old C57BL/6J mice were injected intraperitoneally with saline and/or insulin (0.8 or 1.2units/kg). Insulin generated significant hypoglycemia with the lowest blood glucose levels of 64±4 and 48±5mg/dl for 0.8 and 1.2units/kg of insulin, respectively. Insulin at either dose caused near total social withdrawal at 0.75h, with full recovery not occurring until 4h (0.8units/kg) or 8h (1.2units/kg) post-insulin injection. Insulin also caused a marked elevation in plasma catecholamines. Basal 12h fasting norepinephrine (NE) and epinephrine (Epi) were 287±38 and 350±47pg/ml, respectively. Insulin at 0.8units/kg increased plasma NE and Epi to 994±73 and 1842±472 pg/ml, respectively. Administration of exogenous NE or Epi caused social withdrawal similar in magnitude to insulin. Importantly, administration of the β-2 adrenergic receptor agonist terbutaline also caused social withdrawal, while administration of the β-2 adrenergic receptor antagonist butoxamine blocked NE-induced social withdrawal. Finally, butoxamine blocked insulin-induced social withdrawal. These data demonstrate that hypoglycemia-associated social withdrawal is dependent on catecholamines via a β-2 receptor-mediated pathway. Next, we investigated how insulin-induced hypoglycemia causes anhedonia and depressive-like behavior. Saccharin preference testing 24h post hypoglycemia showed that mice receiving insulin (0.8 units/kg) had saccharin aversion (62% vs 90.5% of total fluid consumption). In addition, mice administered insulin had increased immobility in the forced swim test that took 48h to rectify. Insulin at 0.8units/kg increased plasma corticosterone (325±23pg/ml vs. 119±32pg/ml), Epi (814±254pg/ml vs. 350±40pg/ml), and NE (541±155pg/ml vs. 265±28pg/ml) at 24h post insulin treatment. Importantly, blocking of the adrenergic receptors with phentolamine, metoprolol and butoxamine, or treatment with the anti-depressants (fluoxetine and desipramine) ablated the insulin-induced saccharin aversion and increased immobility in forced swim test. Taken together, these data indicate that anhedonia and depressive-like behaviors are induced by hypoglycemia and those behaviors are dependent on catecholamines in an adrenergic receptor-mediated manner.
- Graduation Semester
- 2010-08
- Permalink
- http://hdl.handle.net/2142/17052
- Copyright and License Information
- Copyright 2010 Min Jung Park
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Graduate Dissertations and Theses at Illinois PRIMARY
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