Abstract

The focal development of atherosclerosis involves the complex interplay of mechanical forces & chemical mediators impinging on endothelial (ECs) & smooth muscle cells (SMC) & their interactions with extracellular matrix (ECM). This program is designed to explore how these factors interact, playing specific attention to two issues; the modulation of signalling responses to humoral mediators by mechanical forces & the cell to regional heterogeneity of such interactions in the vasculature. Several humoral factors influence the adhesive interactions between endothelial & circulating cells, so characteristic of the early stages of activated receptors; PARs) G protein coupled receptors; tyrosine kinase receptors (Eph kinases) & integrins (alphaIIbbeta3 & alphaVbeta3), platelets with ECs, & cholesterol export, properties that may limit atherogenesis. Cyclooxygenase (COX)-2 is a major source of these observations will be addressed in Proj. 1, using selective inhibitors of COX-2 in humans, in conventional & novel mouse models of atherosclerosis & in genetic crosses of these models with mice lacking COX-2 or the PGI2 receptor. We shall investigate specifically how mechanical forces modulate expression of the biosynthetic & signaling pathways of PGI2 in vascular cells. Thrombin, by contrast, enhances adhesive interactions & stimulates cellular proliferation. It is a recognized ligand for some PARs but little is known of the diversity of PARs & their distinct functions in vascular cells. In Proj. 2, the mechanisms of activation, processing & regulation of PARs & the functional importance, distribution & signaling pathways activated by the noel Eph kinases will be investigated. The structural motifs which discriminate affinity for osteopontin amongst beta3 integrins will be examined in Proj. 3. We shall also determine the structural basis for selection by this adhesive ligand amongst its several receptors on platelets, examine the role of mechanical shear on the interaction, & examine the interactions or other signaling pathways outlined above (PGI2, thrombin) on regulating the activation of beta3 integrins. Since the ECM is likely to play a major role in conditioning the response of VSMCs to humoral and mechanical factors, Proj. 4 will explore the role of distinct ECM proteins interacting with mechanical forces on these interactions will also be examine din this project. Finally, Proj. 5 will address the hypothesis that differences in surface geometry amongst apparently similar endothelial cells results in differences in regulated expression of elements of the signaling pathways explored in Projects 1- 4 in response to mechanical forces. These observations will be integrated with comparisons of data derived from regions of flow separation, both in vitro & ex vivo, using mouse models & human atherosclerotic tissue. This program will take an integrated approach to the study of humoral and mechanical signaling in vascular cells. Factors which underlie the cell to cell heterogeneity of this interaction are likely to contribute to the focal nature of atherogenesis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL062250-03
Application #
6390271
Study Section
Heart, Lung, and Blood Initial Review Group (HLBP)
Program Officer
Tolunay, Eser
Project Start
1999-04-07
Project End
2004-03-31
Budget Start
2001-04-01
Budget End
2002-03-31
Support Year
3
Fiscal Year
2001
Total Cost
$1,354,173
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Pharmacology
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Paschos, Georgios K; Tang, Soon Yew; Theken, Katherine N et al. (2018) Cold-Induced Browning of Inguinal White Adipose Tissue Is Independent of Adipose Tissue Cyclooxygenase-2. Cell Rep 24:809-814
Davies, Peter F; Manduchi, Elisabetta; Jiménez, Juan M et al. (2017) Biofluids, cell mechanics and epigenetics: Flow-induced epigenetic mechanisms of endothelial gene expression. J Biomech 50:3-10
Davies, Peter F; Manduchi, Elisabetta; Stoeckert, Christian J et al. (2016) SY 15-2 ENDOTHELIAL EPIGENETICS AND ITS ROLE IN MEDIATING BIOMECHANICAL STRESS OF HYPERTENSION. J Hypertens 34 Suppl 1 - IS:e371
Bae, Yong Ho; Liu, Shu-Lin; Byfield, Fitzroy J et al. (2016) Measuring the Stiffness of Ex Vivo Mouse Aortas Using Atomic Force Microscopy. J Vis Exp :
Tang, Soon Yew; Monslow, James; R Grant, Gregory et al. (2016) Cardiovascular Consequences of Prostanoid I Receptor Deletion in Microsomal Prostaglandin E Synthase-1-Deficient Hyperlipidemic Mice. Circulation 134:328-38
Sweet, Daniel T; Jiménez, Juan M; Chang, Jeremy et al. (2015) Lymph flow regulates collecting lymphatic vessel maturation in vivo. J Clin Invest 125:2995-3007
Jiang, Yi-Zhou; Manduchi, Elisabetta; Stoeckert Jr, Christian J et al. (2015) Arterial endothelial methylome: differential DNA methylation in athero-susceptible disturbed flow regions in vivo. BMC Genomics 16:506
Hsu, Bernadette Y; Bae, Yong Ho; Mui, Keeley L et al. (2015) Apolipoprotein E3 Inhibits Rho to Regulate the Mechanosensitive Expression of Cox2. PLoS One 10:e0128974
Han, Jingyan; Shuvaev, Vladimir V; Davies, Peter F et al. (2015) Flow shear stress differentially regulates endothelial uptake of nanocarriers targeted to distinct epitopes of PECAM-1. J Control Release 210:39-47
Jiang, Yi-Zhou; Manduchi, Elisabetta; Jiménez, Juan M et al. (2015) Endothelial epigenetics in biomechanical stress: disturbed flow-mediated epigenomic plasticity in vivo and in vitro. Arterioscler Thromb Vasc Biol 35:1317-26

Showing the most recent 10 out of 163 publications