Obesity and type 2 diabetes and are increasing dramatically worldwide. The increasing rates of obesity and type 2 diabetes have increased the importance of elucidating the molecular basis for obesity, as well as determining potential therapeutic treatments for this condition. Brown adipose tissue (BAT) is a thermogenic tissue that contains large amounts of mitochondria to dissipate chemical energy as heat. BAT has a high capacity for both glucose and lipid oxidation, making BAT a potential target to decrease plasma glucose and lipids, and a potential target to protect against obesity and lower the risk of diabetes. Transplantation of BAT improves glucose homeostasis in normal chow-fed mice, in a model of diet-induced obesity, and in a model of type 1 diabetes, and these improvements in glucose homeostasis are mediated by increases in circulating IL-6 and FGF21. An increase in brown-adipocytes in white adipose tissue (WAT) through environmental (i.e. cold, exercise) or genetic manipulation results in increased energy expenditure, improved glucose tolerance, and protection against weight gain. It is currently unclear if BAT transplantation confers metabolic benefits due to certain cell types being transplanted, or whether the mature brown adipocytes are required as appears to be the case with `browning' of WAT. Our exciting preliminary data show that transplantation of isolated human progenitor cells differentiated into brown adipocytes decreases body weight and improves insulin sensitivity and a mouse model. We have also shown that transplantation of the total stromal vascular fraction (SVF) of mouse BAT improves glucose tolerance, suggesting that the SVF of BAT is essential to the improvement in metabolic homeostasis after transplantation, although the mechanism for this improvement, and the cell-type responsible for this improved glucose homeostasis, are unclear. We have also generated preliminary data that demonstrate that the cell distribution of the SVF compartment of BAT is altered with exercise-training, although the functional consequence of this change is not understood. There are two specific aims: 1) Determine if transplantation of the specific cell-types of BAT SVF improve glucose homeostasis, if a specific cell-type is required for this effect, and whether IL-6 or FGF21 are required for this effect; and 2) Determine if the metabolic function of the SVF population of BAT is altered after exercise-training. This project will establish the role of specific components of the BAT SVF in improvements in glucose metabolism, how these components function to mediate the beneficial effects of BAT on glucose homeostasis, and if exercise improves the metabolic capacity of specific components of the SVF. These studies have the potential to lead to the development of a novel cell-based therapy to combat type 2 diabetes and obesity and, if translatable to humans, have great therapeutic implications.

Public Health Relevance

While the incidence of type 2 diabetes continues to escalate worldwide, the need for developing potential therapeutics to combat this disease is increasing. The goal of this research application is to determine how specific components of brown adipose tissue (BAT) improve whole body glucose metabolism upon transplantation, and if exercise modifies these components. Elucidation of these components, and their mechanism of action, could provide novel therapeutic options for the treatment of obesity and type 2 diabetes.

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Scientist Development Award - Research & Training (K01)
Project #
1K01DK105109-01
Application #
8869588
Study Section
Kidney, Urologic and Hematologic Diseases D Subcommittee (DDK)
Program Officer
Spain, Lisa M
Project Start
2015-04-01
Project End
2015-07-31
Budget Start
2015-04-01
Budget End
2015-07-31
Support Year
1
Fiscal Year
2015
Total Cost
Indirect Cost
Name
Joslin Diabetes Center
Department
Type
DUNS #
071723084
City
Boston
State
MA
Country
United States
Zip Code
Stanford, Kristin I; Rasmussen, Morten; Baer, Lisa A et al. (2018) Paternal Exercise Improves Glucose Metabolism in Adult Offspring. Diabetes 67:2530-2540
Lehnig, Adam C; Stanford, Kristin I (2018) Exercise-induced adaptations to white and brown adipose tissue. J Exp Biol 221:
Harris, Johan E; Baer, Lisa A; Stanford, Kristin I (2018) Maternal Exercise Improves the Metabolic Health of Adult Offspring. Trends Endocrinol Metab 29:164-177
Stanford, Kristin I; Goodyear, Laurie J (2018) Muscle-Adipose Tissue Cross Talk. Cold Spring Harb Perspect Med 8:
Stanford, Kristin I; Lynes, Matthew D; Takahashi, Hirokazu et al. (2018) 12,13-diHOME: An Exercise-Induced Lipokine that Increases Skeletal Muscle Fatty Acid Uptake. Cell Metab 27:1111-1120.e3
Stanford, Kristin I; Lynes, Matthew D; Takahashi, Hirokazu et al. (2018) 12,13-diHOME: An Exercise-Induced Lipokine that Increases Skeletal Muscle Fatty Acid Uptake. Cell Metab 27:1357
Lynes, Matthew D; Leiria, Luiz O; Lundh, Morten et al. (2017) The cold-induced lipokine 12,13-diHOME promotes fatty acid transport into brown adipose tissue. Nat Med 23:631-637
VandeKopple, Matthew J; Wu, Jinghai; Baer, Lisa A et al. (2017) Stress-responsive HILPDA is necessary for thermoregulation during fasting. J Endocrinol 235:27-38
Stanford, Kristin I; Takahashi, Hirokazu; So, Kawai et al. (2017) Maternal Exercise Improves Glucose Tolerance in Female Offspring. Diabetes 66:2124-2136
May, Francis J; Baer, Lisa A; Lehnig, Adam C et al. (2017) Lipidomic Adaptations in White and Brown Adipose Tissue in Response to Exercise Demonstrate Molecular Species-Specific Remodeling. Cell Rep 18:1558-1572

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