Abstract

Angiogensis is essential for wound healing. Deficient or exuberant angiogenesis, however, contributes to pathogenesis of cutaneous ulcers, ischemic injury, psoriasis, arthritis, vascular sclerosis, as well as the ocular and non-ocular complications of diabetes. Several proteolytic systems regulate the angiogenic process. Gene knockout and reconstitution studies have identified plasminogen activator inhibitor type-I (PAI-I), the major physiologic regulator of plasmin activation, as essential for neovascularization. PAI-I protects the stroma from excessive proteolysis, facilitates endothelial cell locomotion via regulation of cell-to-matrix adhesion and stabilizes nascent vessel structure. PAI-I transcription during endothelial cell activation and in vitro angiogenesis requires mitogen/ extracelIular-regulated kinase (MEK) activity and involves binding of the helix-loop-helix transcription factor USF-1 to an E box motif (CACGTG). We propose to test the hypothesis that mitogen-activated protein (MAP) kinase-mediated USF-1 phosphorylation stimulates E box-dependent DNA binding and regulates PAI-I transcription as part of the switch to angiogenic phenotype. The following Aims will be addressed: 1. We will determine the requirements (i.e., USF-1 transcript expression, protein synthesis, nuclear translocation, phosphorylation) for USF-1 occupancy of the PAI-I box site and induced PAI-I transcription during endothelial growth activation and, migration. 2. We will clarify the MAP kinase type-specificity for USF-1 binding/ phosphorylation and identify the specific residues in USF-I that are phosphorylated by MAP kinases. 3. We will ascertain if the PAI-I E box is an expression """"""""modulating"""""""" motif acting as a platform for replacement of the PAI-I transcriptional inhibitor USF-2a with a USF-1 containing complex during the switch from a quiescent to activated endothelial phenotype. 4. We will utilize genetic constructs that target PAI-I transcripts and modulate USF-1 function to assess effects of PAI-I expression perturbation on endothelial cell migration, proliferation and capillary structure. This work will provide information necessary to fashion targeted therapeutic strategies to treat pathologic angiogenesis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM057242-05
Application #
6542776
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Program Officer
Ikeda, Richard A
Project Start
1998-05-01
Project End
2006-06-30
Budget Start
2002-07-01
Budget End
2003-06-30
Support Year
5
Fiscal Year
2002
Total Cost
$316,000
Indirect Cost

  Institution

Name
Albany Medical College
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
City
Albany
State
NY
Country
United States
Zip Code
12208

  Publications

Higgins, Stephen P; Tang, Yi; Higgins, Craig E et al. (2018) TGF-?1/p53 signaling in renal fibrogenesis. Cell Signal 43:1-10
Anorga, Sandybell; Overstreet, Jessica M; Falke, Lucas L et al. (2018) Deregulation of Hippo-TAZ pathway during renal injury confers a fibrotic maladaptive phenotype. FASEB J 32:2644-2657
Tang, Jiaqi; Gifford, Cody C; Samarakoon, Rohan et al. (2018) Deregulation of Negative Controls on TGF-?1 Signaling in Tumor Progression. Cancers (Basel) 10:
Samarakoon, Rohan; Rehfuss, Alexandra; Khakoo, Nidah S et al. (2016) Loss of expression of protein phosphatase magnesium-dependent 1A during kidney injury promotes fibrotic maladaptive repair. FASEB J 30:3308-3320
Samarakoon, Rohan; Helo, Sevann; Dobberfuhl, Amy D et al. (2015) Loss of tumour suppressor PTEN expression in renal injury initiates SMAD3- and p53-dependent fibrotic responses. J Pathol 236:421-32
Overstreet, Jessica M; Samarakoon, Rohan; Cardona-Grau, Diana et al. (2015) Tumor suppressor ataxia telangiectasia mutated functions downstream of TGF-?1 in orchestrating profibrotic responses. FASEB J 29:1258-68
Higgins, Paul J; Shahzad, Aamir; Kennedy, Jeffrey (2015) Accredited translational medicine centre: Human renal fibrotic disease: Translational research at the Center for Cell Biology and Cancer Research (CCBCR), Albany Medical College, Albany, NY. New Horiz Transl Med 2:51-54
Simone, Tessa M; Higgins, Stephen P; Archambeault, Jaclyn et al. (2015) A small molecule PAI-1 functional inhibitor attenuates neointimal hyperplasia and vascular smooth muscle cell survival by promoting PAI-1 cleavage. Cell Signal 27:923-33
Simone, Tessa M; Higgins, Stephen P; Higgins, Craig E et al. (2014) Chemical Antagonists of Plasminogen Activator Inhibitor-1: Mechanisms of Action and Therapeutic Potential in Vascular Disease. J Mol Genet Med 8:
Simone, Tessa M; Higgins, Paul J (2014) Small Molecule PAI-1 Functional Inhibitor Attenuates Vascular Smooth Muscle Cell Migration and Survival: Implications for the Therapy of Vascular Disease. New Horiz Transl Med 2:16-19

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