Abstract

Inflammation is the major mechanism of diseases mediated by blood cells and plasma proteins. Inflammatory responses underlies a variety of human diseases including atherosclerosis, coronary and peripheral arterial disorders exemplified by Kawasaki disease and systemic lupus (SLE), acute and chronic lung diseases (asthma, acute respiratory distress syndrome, interstitial lung disease), and a variety of vascular diseases including vasooclusive crises in sickle cell anemia. The overall goals of the proposed Program are (i) to conduct genome-wide mutagenesis to select novel genes involved in inflammatory response; (ii) to analyze novel genes at the level of blood lineage specific expression and stimulus-response coupling; (iii) to analyze novel genes in animal models and stimulus-response coupling; (iii) to analyze novel genes in animal models of systemic and localized inflammatory response; and (iv) to determine the function of novel genes in development and signaling of phagocytic and mast cells, T lymphocyte subsets, and B lymphocytes. The currently available resources such as the library of the murine embryonal stem (ES) cell clones with disrupted genes (approximately 600) will be expanded using a new generation of vectors. The Program is a tightly knit organization of highly interactive and cohesive projects and cores: Genetic & Proteomic Analysis of Inflammation; Phagocytosis-Based Functional Genomics of Inflammation; T Lymphocyte-Based Functional of Inflammation; B Lymphocyte-Based Functional Genomics; the Microarrays Core to develop a mutant library microarrays and a new pro-inflammatory gene expression microarrays; the Animal Models Core to screen and analyze phenotype of mutant mice; the Bioinformatics Core to develop a new inflammatory gene database; and the Administrative Core will coordinate this Program to generate, analyze, and share new quality data on genetics and proteomics of inflammation to advance new diagnostic and therapeutic approaches to the diseases of cardiovascular, pulmonary, and blood systems mediated by inflammatory response.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL068744-02
Application #
6620657
Study Section
Heart, Lung, and Blood Initial Review Group (HLBP)
Program Officer
Hasan, Ahmed AK
Project Start
2001-12-10
Project End
2006-11-30
Budget Start
2002-12-01
Budget End
2003-11-30
Support Year
2
Fiscal Year
2003
Total Cost
$1,956,405
Indirect Cost

  Institution

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

  Publications

Hawiger, J; Veach, R A; Zienkiewicz, J (2015) New paradigms in sepsis: from prevention to protection of failing microcirculation. J Thromb Haemost 13:1743-56
Lin, Qing; Liu, Yan; Moore, Daniel J et al. (2012) Cutting edge: the ""death"" adaptor CRADD/RAIDD targets BCL10 and suppresses agonist-induced cytokine expression in T lymphocytes. J Immunol 188:2493-7
Guo, Changying; Gerasimova, Tatiana; Hao, Haiping et al. (2011) Two forms of loops generate the chromatin conformation of the immunoglobulin heavy-chain gene locus. Cell 147:332-43
Farley, Adam R; Powell, David W; Weaver, Connie M et al. (2011) Assessing the components of the eIF3 complex and their phosphorylation status. J Proteome Res 10:1481-94
Olivares-Villagómez, Danyvid; Van Kaer, Luc (2010) TL and CD8??: Enigmatic partners in mucosal immunity. Immunol Lett 134:1-6
Moore, Daniel J; Zienkiewicz, Jozef; Kendall, Peggy L et al. (2010) In vivo islet protection by a nuclear import inhibitor in a mouse model of type 1 diabetes. PLoS One 5:e13235
Liu, Danya; Zienkiewicz, Jozef; DiGiandomenico, Antonio et al. (2009) Suppression of acute lung inflammation by intracellular peptide delivery of a nuclear import inhibitor. Mol Ther 17:796-802
DiGiandomenico, Antonio; Wylezinski, Lukasz S; Hawiger, Jacek (2009) Intracellular delivery of a cell-penetrating SOCS1 that targets IFN-gamma signaling. Sci Signal 2:ra37
Arnett, Diana R; Jennings, Jennifer L; Tabb, David L et al. (2008) A proteomics analysis of yeast Mot1p protein-protein associations: insights into mechanism. Mol Cell Proteomics 7:2090-106
Burg, John S; Powell, David W; Chai, Raymond et al. (2008) Insig regulates HMG-CoA reductase by controlling enzyme phosphorylation in fission yeast. Cell Metab 8:522-31

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