Abstract

Carbohydrate and lipid metabolism are under tight hormonal control by insulin, glucagon and the autonomic nervous system. Following a chronic stress, such as infection, carbohydrate and lipid metabolism are markedly accelerated with associated changes in insulin, glucagon, the sympathetic nervous system and other hormones. This increase in carbohydrate metabolism is not readily suppressed by exogenous nutritional support. Although in vivo studies suggest that gluconeogenesis is increased in infection, in vitro data suggest that hepatic gluconeogenic potential is decreased. An explanation for this paradox is that the hormonal and substrate changes commonly seen in infection may compensate for the hepatic impairment. Glucagon and insulin are potent regulators of glucose metabolism and they have been implicated in directing the increase in glucose production seen in sepsis. The first goal of this proposal is to determine if sepsis alters hepatic insulin sensitivity and the role of basal insulin in regulating hepatic glucose production. The second goal is to determine what role the hyperglucagonemia seen in sepsis plays in directing the gluconeogenic response to infection. The third goal of this proposal is to determine whether the capacity of the liver to remove and metabolize glucose is altered by infection. Experiments will be carried out in dogs which have received either a sterile or an E-coli-containing fibrinogen clot in the peritoneum 36 hrs prior to the study. Hormone levels will be controlled both by surgical (pancreatectomy) and pharmacological (somatostatin) methods. Hepatic glucose metabolism (glycogenolysis, gluconeogenesis, glucose uptake) will be measured using combined tracer and A-V difference techniques. This proposal is a first step in defining some of the many factors that are responsible for the acceleration of gluconeogenesis in stressful situations, more specifically in the infectious state. In addition, it will determine if infection modifies the ability of the liver to take up glucose or to respond to factors, which normally play an important role in stimulating hepatic glucose uptake. The combination of both tracer and balance techniques will allow assessment of the rates of hepatic glucose uptake, glycogenolysis and gluconeogenesis and the factors that are important in determining their relative rates. A knowledge of the factors that regulate hepatic metabolism in infection and the identification of the processes involved will contribute to our understanding of the role they might play in directing the metabolic response to infection and the metabolic fate of nutritional support.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
First Independent Research Support & Transition (FIRST) Awards (R29)
Project #
1R29DK043748-01A1
Application #
3464444
Study Section
Metabolism Study Section (MET)
Project Start
1992-02-01
Project End
1997-01-31
Budget Start
1992-02-01
Budget End
1993-01-31
Support Year
1
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
Vanderbilt University Medical Center
Department
Type
Schools of Medicine
DUNS #
004413456
City
Nashville
State
TN
Country
United States
Zip Code
37212

  Publications

Dooley, James; Garcia-Perez, Josselyn E; Sreenivasan, Jayasree et al. (2016) The microRNA-29 Family Dictates the Balance Between Homeostatic and Pathological Glucose Handling in Diabetes and Obesity. Diabetes 65:53-61
House 2nd, Lawrence M; Morris, Robert T; Barnes, Tammy M et al. (2015) Tissue inflammation and nitric oxide-mediated alterations in cardiovascular function are major determinants of endotoxin-induced insulin resistance. Cardiovasc Diabetol 14:56
Cyphert, Travis J; Morris, Robert T; House, Lawrence M et al. (2015) NF-?B-dependent airway inflammation triggers systemic insulin resistance. Am J Physiol Regul Integr Comp Physiol 309:R1144-52
Chen, Sheng-Song; Otero, Yolanda F; Mulligan, Kimberly X et al. (2014) Liver, but not muscle, has an entrainable metabolic memory. PLoS One 9:e86164
Otero, Yolanda F; Stafford, John M; McGuinness, Owen P (2014) Pathway-selective insulin resistance and metabolic disease: the importance of nutrient flux. J Biol Chem 289:20462-9
Barnes, Tammy M; Otero, Yolanda F; Elliott, Amicia D et al. (2014) Interleukin-6 amplifies glucagon secretion: coordinated control via the brain and pancreas. Am J Physiol Endocrinol Metab 307:E896-905
Pound, Lynley D; Oeser, James K; O'Brien, Tracy P et al. (2013) G6PC2: a negative regulator of basal glucose-stimulated insulin secretion. Diabetes 62:1547-56
Ye, Jianping; McGuinness, Owen P (2013) Inflammation during obesity is not all bad: evidence from animal and human studies. Am J Physiol Endocrinol Metab 304:E466-77
Mulligan, Kimberly X; Morris, R Tyler; Otero, Yolanda F et al. (2012) Disassociation of muscle insulin signaling and insulin-stimulated glucose uptake during endotoxemia. PLoS One 7:e30160
Pound, Lynley D; Sarkar, Suparna A; Ustione, Alessandro et al. (2012) The physiological effects of deleting the mouse SLC30A8 gene encoding zinc transporter-8 are influenced by gender and genetic background. PLoS One 7:e40972

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