Abstract

We are in the midst of a worldwide epidemic of obesity and related metabolic diseases. It is now known that the incidence type 2 diabetes, NASH, cardiovascular disorders and even cancer are increased with obesity. This represents a huge burden upon the health and health care system of the United States and much of the rest of the world. While education concerning diet and exercise are critical components to a solution for these problems, there is a huge need to improve both our basic understanding of and therapeutic options for all of these conditions. Two key parts of organismal energy balance are food intake and energy expenditure. The latter includes physical activity and brown fat-mediated thermogenesis. Our work under this grant (over several years) discovered the PGC1 transcriptional coactivators and their role in various pathways of mitochondrial biogenesis and oxidative metabolism. In the last grant cycle we identified 3 new proteins encoded by the PGC1? gene; PGC1?4, in particular, has interesting and powerful activities in muscle and brown fat. PGC1?4 does not stimulate mitochondrial biogenesis in muscle, but rather increases muscle hypertrophy, strength and resistance to cancer cachexia. Preliminary data here shows that it affects UCP1 and other themogenic genes in fat but again, does not stimulate mitochondrial biogenesis. PGC1?4 also increases expression of a novel myokine, meteorin-like (METRNL), that is a powerful stimulator of adipose tissue browning through modulation of the immune cells within fat tissue. The new cycle of this grant will explore the full range of biologicl functions of METRNL in cellular and systemic metabolism, using knock-out mice already breeding in our lab. Preliminary data has identified a clonal fat cell line that has a molecular response to METRNL and we will use these cells (3T3-F442A) to clone and characterize the METRNL receptor. Isolation of this receptor will be through protein purifications, using tagged MERTNL and advanced protein Mass Spectrometry methods, specifically isobaric tagging. It is expected that the receptor identification will also lead us to new tissues and pathways where METRNL may function in important ways. Lastly, we will return to a key mechanistic problem: how can PGC1?4, a shorter form of the canonical PGC1? protein, regulate such a different set of genes in both muscle and brown fat. Because the PGC1s are coregulatory proteins, this must involve, at least in part, differential interactions with partner transcription factors and other proteins. To investigate this, we will use purifications of the PGC1? complexes, followed by comparative and quantitative Mass Spectrometry. The function of these new factors in the PGC1 complexes will be studied by genetic and (potentially) pharmacological methods.

Public Health Relevance

Energy expenditure, through exercise and brown fat, uses chemical energy and fights obesity and diabetes. This project explores in molecular detail several molecules that have been shown to be regulated by physical activity in animals and to improve metabolic health. Detailed studies may open up new avenues for treatment of metabolic disorders as well as improve our understanding of why physical activity is so beneficial to humans.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK061562-16
Application #
9263929
Study Section
Integrative Physiology of Obesity and Diabetes Study Section (IPOD)
Program Officer
Laughlin, Maren R
Project Start
2002-06-01
Project End
2019-04-30
Budget Start
2017-05-01
Budget End
2018-04-30
Support Year
16
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
Dana-Farber Cancer Institute
Department
Type
DUNS #
076580745
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Kim, Hyeonwoo; Wrann, Christiane D; Jedrychowski, Mark et al. (2018) Irisin Mediates Effects on Bone and Fat via ?V Integrin Receptors. Cell 175:1756-1768.e17
Long, Jonathan Z; Roche, Alexander M; Berdan, Charles A et al. (2018) Ablation of PM20D1 reveals N-acyl amino acid control of metabolism and nociception. Proc Natl Acad Sci U S A 115:E6937-E6945
Rao, Rajesh R; Long, Jonathan Z; White, James P et al. (2014) Meteorin-like is a hormone that regulates immune-adipose interactions to increase beige fat thermogenesis. Cell 157:1279-91
White, James P; Wrann, Christiane D; Rao, Rajesh R et al. (2014) G protein-coupled receptor 56 regulates mechanical overload-induced muscle hypertrophy. Proc Natl Acad Sci U S A 111:15756-61
Boström, Pontus; Wu, Jun; Jedrychowski, Mark P et al. (2012) A PGC1-?-dependent myokine that drives brown-fat-like development of white fat and thermogenesis. Nature 481:463-8
Ruas, Jorge L; White, James P; Rao, Rajesh R et al. (2012) A PGC-1? isoform induced by resistance training regulates skeletal muscle hypertrophy. Cell 151:1319-31
Wu, Jun; Ruas, Jorge L; Estall, Jennifer L et al. (2011) The unfolded protein response mediates adaptation to exercise in skeletal muscle through a PGC-1?/ATF6? complex. Cell Metab 13:160-9
Lustig, Yaniv; Ruas, Jorge L; Estall, Jennifer L et al. (2011) Separation of the gluconeogenic and mitochondrial functions of PGC-1{alpha} through S6 kinase. Genes Dev 25:1232-44
Devarakonda, Srikripa; Gupta, Kushol; Chalmers, Michael J et al. (2011) Disorder-to-order transition underlies the structural basis for the assembly of a transcriptionally active PGC-1?/ERR? complex. Proc Natl Acad Sci U S A 108:18678-83
Rasbach, Kyle A; Gupta, Rana K; Ruas, Jorge L et al. (2010) PGC-1alpha regulates a HIF2alpha-dependent switch in skeletal muscle fiber types. Proc Natl Acad Sci U S A 107:21866-71

Showing the most recent 10 out of 35 publications