Abstract

The primary goal of this project is to characterize the intracellular signal transduction mechanisms activated by fluid flow in endothelial cells (BC). This information will then be used to define the plasma membrane components by which endothelial cells sense their hemodynamic environment. This knowledge is important to our understanding of a wide variety of biological processes that are modulated by physical forces, such as bone growth, muscle hypertrophy, hair cell sound transduction, etc. The major hypothesis underlying the proposal is that fluid shear stress activates receptor-like signal events in BC. If this hypothesis is correct, it would follow that intracellular kinases (e.g., calcium- calmodulin dependent, protein kinase C (PKC), and a newly defined family termed mitogen activated protein kinases (MAPK)) should be activated by fluid shear stress. Our preliminary data provide strong support for a major role of the MAPK in the BC response to flow. To characterize the nature of the MAPK response to fluid shear stress and to identify other molecules that transmit the mechanical signal from plasma membrane to MAPK we will use immunological and biochemical techniques to study cultured human and bovine BC. These cells will be exposed to defined fluid shear stress in a parallel plate flow chamber. We will first characterize the MAPK response to flow by studying its dependence on shear stress, and its regulation by calcium, protein kinases (C kinase and tyrosine kinases), G proteins, and integrins. Next, we will study the differences in activation of MAPK by different flow patterns (steady, pulsatile and oscillatory). Finally, we will study the long-term alterations in these signal molecules in models (both in vivo and in vitro) of altered flow conditions. These studies should define the temporal and functional interactions of MAPK with other intracellular mediators activated by flow. Ultimately, the results will allow us to characterize and identify the plasma membrane components (i.e., the """"""""shear stress receptor"""""""") responsible for the modulation of BC function by hemodynamic forces.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL018645-23S1
Application #
2823768
Study Section
Project Start
Project End
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
23
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
University of Washington
Department
Type
DUNS #
135646524
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Wight, Thomas N (2018) A role for proteoglycans in vascular disease. Matrix Biol 71-72:396-420
Kocarnik, Beverly M; Boyko, Edward J; Matsumoto, Alvin M et al. (2016) Baseline estradiol concentration in community-dwelling Japanese American men is not associated with intra-abdominal fat accumulation over 10 years. Obes Res Clin Pract 10:624-632
Nishizawa, Tomohiro; Kanter, Jenny E; Kramer, Farah et al. (2014) Testing the role of myeloid cell glucose flux in inflammation and atherosclerosis. Cell Rep 7:356-365
Wight, Thomas N; Kinsella, Michael G; Evanko, Stephen P et al. (2014) Versican and the regulation of cell phenotype in disease. Biochim Biophys Acta 1840:2441-51
Kang, Inkyung; Yoon, Dong Won; Braun, Kathleen R et al. (2014) Expression of versican V3 by arterial smooth muscle cells alters tumor growth factor ? (TGF?)-, epidermal growth factor (EGF)-, and nuclear factor ?B (NF?B)-dependent signaling pathways, creating a microenvironment that resists monocyte adhesion. J Biol Chem 289:15393-404
Ruppert, S M; Hawn, T R; Arrigoni, A et al. (2014) Tissue integrity signals communicated by high-molecular weight hyaluronan and the resolution of inflammation. Immunol Res 58:186-92
Wight, Thomas N; Kang, Inkyung; Merrilees, Mervyn J (2014) Versican and the control of inflammation. Matrix Biol 35:152-61
Tsubota, Yoshiaki; Frey, Jeremy M; Tai, Phillip W L et al. (2013) Monocyte ADAM17 promotes diapedesis during transendothelial migration: identification of steps and substrates targeted by metalloproteinases. J Immunol 190:4236-44
Cieslewicz, Maryelise; Tang, Jingjing; Yu, Jonathan L et al. (2013) Targeted delivery of proapoptotic peptides to tumor-associated macrophages improves survival. Proc Natl Acad Sci U S A 110:15919-24
Lund, Susan Amanda; Wilson, Carole L; Raines, Elaine W et al. (2013) Osteopontin mediates macrophage chemotaxis via ?4 and ?9 integrins and survival via the ?4 integrin. J Cell Biochem 114:1194-202

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