Abstract

In the current grant cycle, we identified null mutations in a novel gene, Lpin1 (lipin), as the cause of lipodystrophy in the fatty liver dystrophy (fld) mouse. The fld mouse is a model of generalized lipodystrophy, with a lack of normal adipose tissue, insulin resistance, and susceptibility to atherosclerosis. We have established that lipin is abundantly expressed in adipose tissue and skeletal muscle. In the adipocyte, lipin is induced at two distinct time points-first, shortly after initiation of differentiation, acting upstream of the PPARgamma transcriptional regulator, and later, in mature adipocytes. The requirement for lipin in differentiation accounts for the lipodystrophy observed in lipin-deficient mice. Furthermore, transgenic mice with enhanced lipin expression specifically in mature adipocytes become obese, suggesting a specific role for lipin after differentiation. Lipin also has an important role in muscle. Using both lipin-deficient and lipin transgenic mice, we have demonstrated that lipin expression levels in muscle are a determinant of energy metabolism, with null expression causing increased energy expenditure, and enhanced expression causing reduced energy expenditure, leading to obesity. Thus, lipin is unique among known factors in its ability to cause the absolute extremes of adiposity-ranging from lipodystrophy to obesity-depending on its expression levels in peripheral tissues. The proposed studies seek to further elucidate the cellular and molecular functions of lipin in adipose tissue and muscle biology. These studies will also provide the first evaluation of genetic variation in human lipin gene structure and expression and its potential association with features of the metabolic syndrome. Using a combination of genetic, molecular, and biochemical approaches, we will address the following questions: (1) What is the role of lipin in differentiating and mature adipocytes?; (2) How do lipin levels in muscle modulate energy expenditure?; (3) What is the identity of lipin-protein interacting proteins?; and (4) Are variations in human lipin gene sequence or expression levels associated with clinical aspects of the metabolic syndrome?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL028481-22
Application #
7312437
Study Section
Heart, Lung, and Blood Initial Review Group (HLBP)
Project Start
2006-02-01
Project End
2010-01-31
Budget Start
2006-02-01
Budget End
2007-01-31
Support Year
22
Fiscal Year
2006
Total Cost
$440,154
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Type
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Orozco, Luz D; Farrell, Colin; Hale, Christopher et al. (2018) Epigenome-wide association in adipose tissue from the METSIM cohort. Hum Mol Genet 27:1830-1846
Chella Krishnan, Karthickeyan; Kurt, Zeyneb; Barrere-Cain, Rio et al. (2018) Integration of Multi-omics Data from Mouse Diversity Panel Highlights Mitochondrial Dysfunction in Non-alcoholic Fatty Liver Disease. Cell Syst 6:103-115.e7
Freund, Malika Kumar; Burch, Kathryn S; Shi, Huwenbo et al. (2018) Phenotype-Specific Enrichment of Mendelian Disorder Genes near GWAS Regions across 62 Complex Traits. Am J Hum Genet 103:535-552
Pan, David Z; Garske, Kristina M; Alvarez, Marcus et al. (2018) Integration of human adipocyte chromosomal interactions with adipose gene expression prioritizes obesity-related genes from GWAS. Nat Commun 9:1512
Small, Kerrin S; Todor?evi?, Marijana; Civelek, Mete et al. (2018) Regulatory variants at KLF14 influence type 2 diabetes risk via a female-specific effect on adipocyte size and body composition. Nat Genet 50:572-580
Mangul, Serghei; Yang, Harry Taegyun; Strauli, Nicolas et al. (2018) ROP: dumpster diving in RNA-sequencing to find the source of 1 trillion reads across diverse adult human tissues. Genome Biol 19:36
Cantor, Rita; Navarro, Linda; Pan, Calvin (2018) Identifying fenofibrate responsive CpG sites. BMC Proc 12:43
Rahmani, Elior; Schweiger, Regev; Shenhav, Liat et al. (2018) BayesCCE: a Bayesian framework for estimating cell-type composition from DNA methylation without the need for methylation reference. Genome Biol 19:141
Goldberg, Ira J; Reue, Karen; Abumrad, Nada A et al. (2018) Deciphering the Role of Lipid Droplets in Cardiovascular Disease: A Report From the 2017 National Heart, Lung, and Blood Institute Workshop. Circulation 138:305-315
Hui, Simon T; Kurt, Zeyneb; Tuominen, Iina et al. (2018) The Genetic Architecture of Diet-Induced Hepatic Fibrosis in Mice. Hepatology 68:2182-2196

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