Abstract

The overall goal of this grant is to understand the molecular mechanisms for insulin resistance in Type 2 diabetes and, in particular, how changes in adipose biology contribute to diabetes risk, with the long-term goal of finding new therapeutic targets for T2D. Since our discovery in 2005 that Retinol Binding Protein 4 (RBP4) is elevated in serum and white adipose tissue in many insulin-resistant states in humans, RBP4 elevation causes insulin resistance, and lowering serum RBP4 levels improves insulin sensitivity, many studies worldwide have extended these observations to show that elevated RBP4 is a biomarker and a potential cause of insulin resistance and metabolic syndrome. A breakthrough in the last grant cycle was our discovery that RBP4 causes insulin resistance by inducing a proinflammatory state in adipose tissue mediated by Toll Like Receptor 4. We also showed that overexpression of RBP4 selectively in adipose tissue has detrimental systemic metabolic effects and causes hepatic steatosis. In the next grant cycle, we will investigate novel mechanisms by which RBP4 induces adipose tissue inflammation and systemic insulin resistance including the role of lipolysis. Using ?omics? approaches in adipose tissue from the same adipose-Glut4 overexpressing and knockout mice in which we found RBP4, we discovered a novel class of endogenous lipids with anti-diabetic and anti-inflammatory effects - Branched Fatty Acid esters of Hydroxy Fatty Acids (FAHFAs). Since a subclass of FAHFAs, Palmitic Acid esters of Hydroxy Stearic Acids (PAHSAs), are low in insulin-resistant people and in RBP4-overexpressing mice and our new data show that PAHSAs can block the actions of RBP4 at the cellular level and improve insulin sensitivity in RBP4-overexpressing mice, we will investigate a possible mechanistic relationship between RBP4 and PAHSAs. We will also build on our studies to determine the molecular mechanisms for increased RBP4 retention in serum in insulin-resistant states by investigating the role of post- translational modifications of transthyretin, the serum binding partner for RBP4. Significance: These studies will provide novel insights into the mechanisms by which adipose tissue regulates systemic insulin sensitivity and glucose homeostasis. Discovering the interactions among these molecules will lead to a more comprehensive understanding of the cellular and tissue networks by which Glut4 downregulation in adipocytes increases Type 2 diabetes risk. Since RBP4 is elevated in many insulin-resistant people, understanding the mechanisms underlying RBP4-induced insulin resistance and retention of RBP4 in serum may lead to new strategies to lower RBP4 levels to prevent and treat Type 2 diabetes.

Public Health Relevance

The proposed research is relevant to public health because the discovery of the cellular and physiological mechanisms by which Retinol Binding Protein 4 activates the immune system in adipose tissue and causes systemic insulin resistance, and the mechanisms by which it is increased in insulin-resistant states, could help identify new therapeutic approaches for type 2 diabetes and the metabolic syndrome. The proposed research is relevant to the NIH's mission pertaining to developing fundamental knowledge that will help reduce the health burdens of obesity, diabetes, and maladaptive behavior, which are prominent ongoing public health and safety concerns.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK043051-26
Application #
9507810
Study Section
Integrative Physiology of Obesity and Diabetes Study Section (IPOD)
Program Officer
Laughlin, Maren R
Project Start
1992-02-01
Project End
2021-06-30
Budget Start
2018-07-01
Budget End
2019-06-30
Support Year
26
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Beth Israel Deaconess Medical Center
Department
Type
DUNS #
071723621
City
Boston
State
MA
Country
United States
Zip Code

  Publications

Hammarstedt, Ann; Syed, Ismail; Vijayakumar, Archana et al. (2018) Adipose tissue dysfunction is associated with low levels of the novel Palmitic Acid Hydroxystearic Acids. Sci Rep 8:15757
Kolar, Matthew J; Nelson, Andrew T; Chang, Tina et al. (2018) Faster Protocol for Endogenous Fatty Acid Esters of Hydroxy Fatty Acid (FAHFA) Measurements. Anal Chem 90:5358-5365
Syed, Ismail; Lee, Jennifer; Moraes-Vieira, Pedro M et al. (2018) Palmitic Acid Hydroxystearic Acids Activate GPR40, Which Is Involved in Their Beneficial Effects on Glucose Homeostasis. Cell Metab 27:419-427.e4
Nelson, Andrew T; Kolar, Matthew J; Chu, Qian et al. (2017) Stereochemistry of Endogenous Palmitic Acid Ester of 9-Hydroxystearic Acid and Relevance of Absolute Configuration to Regulation. J Am Chem Soc 139:4943-4947
Vijayakumar, Archana; Aryal, Pratik; Wen, Jennifer et al. (2017) Absence of Carbohydrate Response Element Binding Protein in Adipocytes Causes Systemic Insulin Resistance and Impairs Glucose Transport. Cell Rep 21:1021-1035
McMillin, Shawna L; Schmidt, Denise L; Kahn, Barbara B et al. (2017) GLUT4 Is Not Necessary for Overload-Induced Glucose Uptake or Hypertrophic Growth in Mouse Skeletal Muscle. Diabetes 66:1491-1500
Reno, Candace M; Puente, Erwin C; Sheng, Zhenyu et al. (2017) Brain GLUT4 Knockout Mice Have Impaired Glucose Tolerance, Decreased Insulin Sensitivity, and Impaired Hypoglycemic Counterregulation. Diabetes 66:587-597
Kolar, Matthew J; Kamat, Siddhesh S; Parsons, William H et al. (2016) Branched Fatty Acid Esters of Hydroxy Fatty Acids Are Preferred Substrates of the MODY8 Protein Carboxyl Ester Lipase. Biochemistry 55:4636-41
Smith, U; Kahn, B B (2016) Adipose tissue regulates insulin sensitivity: role of adipogenesis, de novo lipogenesis and novel lipids. J Intern Med 280:465-475
Lee, Seung-Ah; Yuen, Jason J; Jiang, Hongfeng et al. (2016) Adipocyte-specific overexpression of retinol-binding protein 4 causes hepatic steatosis in mice. Hepatology 64:1534-1546

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