Abstract

The long-term goal of the proposed studies is to understand the signal transduction mechanisms governing the development and function of the cardiovascular system. In the previous funding period, we focused on the role and mechanisms of focal adhesion kinase (FAK) signaling in ECs during embryonic angiogenesis and FAK- family interacting protein of 200 kDa (FIP200) in cardiac development. Using a functional reconstitution approach based on isolated primary FAK-null ECs, we identified a novel role for S732 phosphorylation of FAK in promoting EC proliferation and angiogenesis by the regulation of centrosome functions during mitosis. We have also created two different FAK mutant knockin mouse models. Using the EC-specific FAK kinase- defective (KD) mutant knockin mouse model, we demonstrated the role of kinase-independent and -dependent functions of FAK in EC survival and barrier function, respectively, during embryonic development. In addition to these and several others published studies that show the role of FAK and FIP200 in cardiac development, this grant also supported our studies on the role and mechanisms of FIP200 in fetal hematopoietic stem cells. In preliminary studies, we established new mouse models with the inducible EC-specific FAK knockout (KO) and KD mutant knockin mice and showed a role of FAK and its kinase activity in adult angiogenesis. Moreover, we observed increased Notch signaling upon FAK deletion or loss of its kinase activity, suggesting a potentially novel mechanism of FAK in the regulation of angiogenesis through the critical Notch pathway. We also generated and analyzed both embryonic and inducible EC-specific KO of TSC1 (tuberous sclerosis complex 1), which provided the first direct evidence for a role of TSC/mTOR signaling in the embryonic vascular development and angiogenesis of adult organisms in mouse models in vivo. Despite these progresses, still relatively little is known about the role and mechanisms o FAK signaling in the regulation of angiogenesis in adult organism in vivo. Likewise, the mechanisms of TSC/mTOR signaling in ECs during embryonic and adult angiogenesis have not been assessed directly in vivo. Based on our previous and preliminary studies, we propose to 1). Analyze the role and mechanism of FAK and its kinase activity in the regulation of Notch signaling in postnatal angiogenesis by using inducible EC-specific FAK KO and KD mutant knockin mouse models, 2). Investigate the role and mechanisms of TSC/mTOR signaling in vascular development and angiogenesis by using an EC-specific TSC1 KO mouse model, and 3). Study the role and mechanisms of TSC/mTOR signaling and its regulation of VEGF expression in postnatal angiogenesis. These studies will generate significant insights into the mechanisms of intracellular signaling in the regulation of angiogenesis in vivo and may also provide critical information for potential development of novel therapies for angiogenesis related diseases.

Public Health Relevance

Angiogenesis plays an essential role in embryogenesis, homeostasis of adult organism, and contributes to various diseases including coronary heart disease, age-related macular degeneration, diabetes and cancer when it is not properly regulated. Analysis of molecular and cellular mechanisms by which key signaling molecules and their associated pathways regulate angiogenesis using mouse models in vivo will significantly advance our understanding of the basic mechanisms of angiogenesis that may contribute to novel therapies for cardiovascular and other diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL073394-12
Application #
8856304
Study Section
Intercellular Interactions (ICI)
Program Officer
Schramm, Charlene A
Project Start
2003-04-01
Project End
2017-03-31
Budget Start
2015-04-01
Budget End
2016-03-31
Support Year
12
Fiscal Year
2015
Total Cost
$389,382
Indirect Cost
$143,132

  Institution

Name
University of Cincinnati
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
041064767
City
Cincinnati
State
OH
Country
United States
Zip Code
45221

  Publications

Chen, Song; Wang, Chenran; Yeo, Syn et al. (2016) Distinct roles of autophagy-dependent and -independent functions of FIP200 revealed by generation and analysis of a mutant knock-in mouse model. Genes Dev 30:856-69
Wang, Chenran; Chen, Song; Yeo, Syn et al. (2016) Elevated p62/SQSTM1 determines the fate of autophagy-deficient neural stem cells by increasing superoxide. J Cell Biol 212:545-60
Sun, Shaogang; Chen, Song; Liu, Fei et al. (2015) Constitutive Activation of mTORC1 in Endothelial Cells Leads to the Development and Progression of Lymphangiosarcoma through VEGF Autocrine Signaling. Cancer Cell 28:758-772
Fang, Fang; Sun, Shaogang; Wang, Li et al. (2015) Neural Crest-Specific TSC1 Deletion in Mice Leads to Sclerotic Craniofacial Bone Lesion. J Bone Miner Res 30:1195-205
Chen, Xiao Lei; Nam, Ju-Ock; Jean, Christine et al. (2012) VEGF-induced vascular permeability is mediated by FAK. Dev Cell 22:146-57
Fan, Huaping; Guan, Jun-Lin (2011) Compensatory function of Pyk2 protein in the promotion of focal adhesion kinase (FAK)-null mammary cancer stem cell tumorigenicity and metastatic activity. J Biol Chem 286:18573-82
Peng, Xu; Guan, Jun-Lin (2011) Focal adhesion kinase: from in vitro studies to functional analyses in vivo. Curr Protein Pept Sci 12:52-67
Zhao, Xiaofeng; Guan, Jun-Lin (2011) Focal adhesion kinase and its signaling pathways in cell migration and angiogenesis. Adv Drug Deliv Rev 63:610-5
Li, Xiao-Yan; Zhou, Xiaoming; Rowe, R Grant et al. (2011) Snail1 controls epithelial-mesenchymal lineage commitment in focal adhesion kinase-null embryonic cells. J Cell Biol 195:729-38
Wang, Chenran; Yoo, Youngdong; Fan, Huaping et al. (2010) Regulation of Integrin ? 1 recycling to lipid rafts by Rab1a to promote cell migration. J Biol Chem 285:29398-405

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