Abstract

We will extend our studies of the cellular and molecular mechanisms that are responsible for increased permeability of the lung vasculature. This increase in lung vascular permeability results in an array of pathological conditions including Adult Respiratory Distress Syndrome. The studies proposed here are based on the hypothesis that the VEcadherin- containing adherens junctions (AJs) of endothelial cells are critical determinants in both the increased permeability response of the endothelium and its time-dependent reversal. The dynamic AJ affects cell shape through the interaction of VE-cadherin with catenins that in turn associate with the actin cytoskeleton. The proposed studies will characterize the mechanisms by which AJs disassemble in response to thrombin and subsequently reassemble in a time-dependent manner. We will identify the phosphorylation and dephosphorylation """"""""switches"""""""", present in the VEcadherin/ eatenin complexes, which are responsible for regulating endothelial permeability. This project has the following Aims: (i) to identify the signaling mechanisms mediating the loss of homotypic VE-cadherin binding, the disassembly of AJs, and the resultant increased permeability of the endothelium, (ii), to characterize the signaling mechanisms responsible for re-assembly of AJs and reversal of this increased permeability response, and (iii) to characterize the mechanism of angiopoietin-1-induced AJ stabilization and its role in inhibiting the loss of endothelial barrier function. The studies will be carried out both in endothelial cells and in vivo with intact mice. We will exploit a variety of methodologies including cell imaging, expression of mutant constructs, gene transfer, and the evaluation of transgenic mouse models. By more fully understanding mechanisms of increased vascular permeability and the reversal of this process, we will be in a position to develop novel strategies directed against components of the AJ complex that will prevent vascular leakiness and the formation of pulmonary edema.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
2R01HL045638-16
Application #
6729481
Study Section
Special Emphasis Panel (ZRG1-SSS-8 (03))
Program Officer
Denholm, Elizabeth M
Project Start
1993-06-11
Project End
2008-06-30
Budget Start
2004-07-01
Budget End
2005-06-30
Support Year
16
Fiscal Year
2004
Total Cost
$389,675
Indirect Cost

  Institution

Name
University of Illinois at Chicago
Department
Pharmacology
Type
Schools of Medicine
DUNS #
098987217
City
Chicago
State
IL
Country
United States
Zip Code
60612

  Publications

Komarova, Yulia; Kruse, Kevin J; Mehta, Dolly et al. (2017) Response by Komarova et al to Letter Regarding Article, ""Protein Interactions at Endothelial Junctions and Signaling Mechanisms Regulating Endothelial Permeability"". Circ Res 120:e28
Soni, Dheeraj; Regmi, Sushil C; Wang, Dong-Mei et al. (2017) Pyk2 phosphorylation of VE-PTP downstream of STIM1-induced Ca2+ entry regulates disassembly of adherens junctions. Am J Physiol Lung Cell Mol Physiol 312:L1003-L1017
Jiang, Chunling; Liu, Zheng; Hu, Rong et al. (2017) Inactivation of Rab11a GTPase in Macrophages Facilitates Phagocytosis of Apoptotic Neutrophils. J Immunol 198:1660-1672
Cheng, Kwong Tai; Xiong, Shiqin; Ye, Zhiming et al. (2017) Caspase-11-mediated endothelial pyroptosis underlies endotoxemia-induced lung injury. J Clin Invest 127:4124-4135
Marsboom, Glenn; Chen, Zhenlong; Yuan, Yang et al. (2017) Aberrant caveolin-1-mediated Smad signaling and proliferation identified by analysis of adenine 474 deletion mutation (c.474delA) in patient fibroblasts: a new perspective on the mechanism of pulmonary hypertension. Mol Biol Cell 28:1177-1185
Yamada, Kaori H; Kang, Hojin; Malik, Asrar B (2017) Antiangiogenic Therapeutic Potential of Peptides Derived from the Molecular Motor KIF13B that Transports VEGFR2 to Plasmalemma in Endothelial Cells. Am J Pathol 187:214-224
Komarova, Yulia A; Kruse, Kevin; Mehta, Dolly et al. (2017) Protein Interactions at Endothelial Junctions and Signaling Mechanisms Regulating Endothelial Permeability. Circ Res 120:179-206
Cantelmo, Anna Rita; Conradi, Lena-Christin; Brajic, Aleksandra et al. (2016) Inhibition of the Glycolytic Activator PFKFB3 in Endothelium Induces Tumor Vessel Normalization, Impairs Metastasis, and Improves Chemotherapy. Cancer Cell 30:968-985
Klomp, Jennifer E; Huyot, Vincent; Ray, Anne-Marie et al. (2016) Mimicking transient activation of protein kinases in living cells. Proc Natl Acad Sci U S A 113:14976-14981
Mittal, Manish; Tiruppathi, Chinnaswamy; Nepal, Saroj et al. (2016) TNF?-stimulated gene-6 (TSG6) activates macrophage phenotype transition to prevent inflammatory lung injury. Proc Natl Acad Sci U S A 113:E8151-E8158

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