Abstract

In this application for an exploratory/development grant (R21), the PI proposes to study the role of applied electrical potentials on angiogenesis, the growth, migration, and formation of new capillaries by endothelial cells (ECs). The PI reports the new observation that exposure of capillary ECs to low-level applied electrical potentials significantly increased EC growth over several days, suggesting that this treatment might be useful to improve wound healing. Although electric field effects have been previously reported in wound healing studies, the mechanism(s) of these effects, particularly with respect to angiogenesis, are unknown. The PI has found that direct current (DC) negative potentials stimulated while positive potentials inhibited EC growth or caused necrosis. In vitro and in vivo angiogenesis models are proposed.
The Specific Aims are to: 1) determine the optimal potential conditions for EC stimulation;
This aim will use DC, pulse wave DC, and AC current approaches. 2) determine the mechanism of EC growth stimulation;
This aim will examine whther an electrochemical process at the electrode generate a chemical species (which could be detected in the media) which affects EC growth. These experiments will use cyclic voltammetry to evaluate the media for the presence of these putative species. The second part of these experiments will examine whether negative potential stimulates EC production, release, or activation of FGF or VEG-F. These experiments will use various molecular techniques to determine wether these growth factors are mobilized into the media by negative potential from EC cytoplasm, cell surfaces, or extracellular matrix. These latter experiments will be performed using cell-free extracellular matrix derived from electric potential-treated cultures, and subsequently exposed to normal ECs. 3) to determine the influence of negative potential in vitro (using a scrape wound healing assay, SWA) and in vivo (using a chorioallantoic membrane (CAM) assay). The SWA will be performed directly on optically transparent ITO glass substrate, and numbers of ECs entering the denuded areas monitored. CAMs will be sham- treated or treated with negative potential, and then density and number of vessels quantified. These experiments may lead to new adjunct therapies to promote angiogenesis in a variety of clinical situations.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Exploratory/Developmental Grants (R21)
Project #
1R21GM058583-01
Application #
2745530
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Project Start
1999-01-01
Project End
2000-12-31
Budget Start
1999-01-01
Budget End
1999-12-31
Support Year
1
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Massachusetts Lowell
Department
Type
Schools of Arts and Sciences
DUNS #
956072490
City
Lowell
State
MA
Country
United States
Zip Code
01854

  Publications

Zhou, Tiean; Marx, Kenneth A; Dewilde, Abiche H et al. (2012) Dynamic cell adhesion and viscoelastic signatures distinguish normal from malignant human mammary cells using quartz crystal microbalance. Anal Biochem 421:164-71
Marx, Kenneth A; Zhou, Tiean; McIntosh, Donna et al. (2009) Electropolymerized tyrosine-based thin films: selective cell binding via peptide recognition to novel electropolymerized biomimetic tyrosine RGDY films. Anal Biochem 384:86-95
Marx, Kenneth A; Zhou, Tiean; Montrone, Anne et al. (2007) A comparative study of the cytoskeleton binding drugs nocodazole and taxol with a mammalian cell quartz crystal microbalance biosensor: different dynamic responses and energy dissipation effects. Anal Biochem 361:77-92
Marx, Kenneth A; Zhou, Tiean; Montrone, Anne et al. (2005) Quartz crystal microbalance biosensor study of endothelial cells and their extracellular matrix following cell removal: Evidence for transient cellular stress and viscoelastic changes during detachment and the elastic behavior of the pure matrix. Anal Biochem 343:23-34
Marx, Kenneth A; Zhou, Tiean; Long, Dang (2005) Electropolymerized films formed from the amphiphilic decyl esters of D- and L-tyrosine compared to L-tyrosine using the electrochemical quartz crystal microbalance. Biomacromolecules 6:1698-706
Marx, Kenneth A; Zhou, Tiean; Warren, Michael et al. (2003) Quartz crystal microbalance study of endothelial cell number dependent differences in initial adhesion and steady-state behavior: evidence for cell-cell cooperativity in initial adhesion and spreading. Biotechnol Prog 19:987-99
Marx, Kenneth A (2003) Quartz crystal microbalance: a useful tool for studying thin polymer films and complex biomolecular systems at the solution-surface interface. Biomacromolecules 4:1099-120
Marx, K A; Zhou, T; Montrone, A et al. (2001) A quartz crystal microbalance cell biosensor: detection of microtubule alterations in living cells at nM nocodazole concentrations. Biosens Bioelectron 16:773-82
Zhou, T; Marx, K A; Warren, M et al. (2000) The quartz crystal microbalance as a continuous monitoring tool for the study of endothelial cell surface attachment and growth. Biotechnol Prog 16:268-77
Marx, K A; Zhou, T; Sarma, R (1999) Quartz crystal microbalance measurement of self-assembled micellar tubules of the amphiphilic decyl ester of D-tyrosine and their enzymatic polymerization. Biotechnol Prog 15:522-8