Abstract

Our previous studies provide direct evidence that gap junction communication between endothelial cells and the mesenchymal cells that they recruit, via Cx43-containing channels, mediates the activation of TGF-beta, which is required for endothelial-induced mural cell differentiation during blood vessel assembly. In the proposed studies, we focus on elucidating the mechanism(s) by which gap junction communication regulates these processes. To gain insight into the mechanism(s), we will determine whether other Cx proteins expressed in the vasculature (Cx45, Cx40, Cx37), which exhibit distinct selectivity and regulatory properties, are capable of supporting these processes. Our Preliminary data, to date, demonstrate that Cx40 does not. Thus, our overall hypothesis, based on Preliminary data and the phenotypes of mice lacking specific Cx proteins, is that only Cx43- and Cx45-containing gap junction channels between endothelial and mesenchymal cells can mediate TGF-beta activation and endothelial-induced mural cell differentiation. We further hypothesize that TGF-beta activation is mediated either via the exchange of cytoplasmic signals through Cx43- and Cx45- containing channels that are excluded by other channel types (Cx40 and Cx37), or via signaling events involving the regulation of the unique cytoplasmic domains of Cx43 and Cx45 proteins. To address these issues, we will measure differences in the selectivity of gap junction channels that mediate TGF-beta activation and endothelial-induced mural cell differentiation (Cx43-containing) vs. those that do not (Cx40-containing). We will examine the role of the cytoplasmic, regulatory region of Cx43 in the activation of TGF-beta via testing the ability of Cx43-/- mesenchymal cell transfectants that express Cx43 lacking the entire cytoplasmic, regulatory region or containing specific point mutations within that region, to form functional gap junction channels with endothelial cells, and mediate TGF-beta activation and endothelial-induced mural cell differentiation. Finally, using the information obtained in the aforementioned studies we will examine the signaling events supported by gap junctions that lead to TGF-b activation. Our studies will reveal the mechanism(s) by which gap junction communication regulates blood vessel assembly. Insights gained from these studies will be applicable to ex vivo vascular tissue engineering and will aid in the development of strategies to promote or suppress vessel formation for the treatment of prevalent pathologies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
1R01HL077675-01
Application #
6816105
Study Section
Vascular Cell and Molecular Biology Study Section (VCMB)
Program Officer
Rabadan-Diehl, Cristina
Project Start
2004-07-01
Project End
2008-04-30
Budget Start
2004-07-01
Budget End
2005-04-30
Support Year
1
Fiscal Year
2004
Total Cost
$314,705
Indirect Cost

  Institution

Name
Baylor College of Medicine
Department
Pediatrics
Type
Schools of Medicine
DUNS #
051113330
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Co?kun, Süleyman; Chao, Hsu; Vasavada, Hema et al. (2014) Development of the fetal bone marrow niche and regulation of HSC quiescence and homing ability by emerging osteolineage cells. Cell Rep 9:581-90
Goldberg, Joshua S; Vadakkan, Tegy J; Hirschi, Karen K et al. (2013) A computational approach to detect gap junction plaques and associate them with cells in fluorescent images. J Histochem Cytochem 61:283-93
Marcelo, Kathrina L; Goldie, Lauren C; Hirschi, Karen K (2013) Regulation of endothelial cell differentiation and specification. Circ Res 112:1272-87
Fang, Jennifer S; Dai, Cuiping; Kurjiaka, David T et al. (2013) Connexin45 regulates endothelial-induced mesenchymal cell differentiation toward a mural cell phenotype. Arterioscler Thromb Vasc Biol 33:362-8
Marcelo, Kathrina L; Sills, Tiffany M; Coskun, Suleyman et al. (2013) Hemogenic endothelial cell specification requires c-Kit, Notch signaling, and p27-mediated cell-cycle control. Dev Cell 27:504-15
Ek-Vitorin, Jose F; Burt, Janis M (2013) Structural basis for the selective permeability of channels made of communicating junction proteins. Biochim Biophys Acta 1828:51-68
Kienstra, Kirsten A; Hirschi, Karen K (2012) Studying vascular progenitor cells in a neonatal mouse model. Methods Mol Biol 904:235-42
Good, Miranda E; Ek-Vitorín, José F; Burt, Janis M (2012) Extracellular loop cysteine mutant of cx37 fails to suppress proliferation of rat insulinoma cells. J Membr Biol 245:369-80
Gemel, Joanna; Nelson, Tasha K; Burt, Janis M et al. (2012) Inducible coexpression of connexin37 or connexin40 with connexin43 selectively affects intercellular molecular transfer. J Membr Biol 245:231-41
Kienstra, Kirsten A; Hirschi, Karen K (2012) Vascular progenitor cell mobilization. Methods Mol Biol 904:155-64

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