Abstract

? ? This mentored Research Career Development (K08) proposal describes the 5-year training program for Dr. Kibbe. This proposal builds upon the Candidate's strengths and prior research skills and takes advantage of the research scientists at Northwestern University and the National Cancer Institute. Through the mentorship of Drs. David Dean and William Pearce and a structured didactic component, the Candidate's ability to perform hypothesis driven research will be advanced to a fully independent surgeon scientist The broad, long-term objective of this project is to prevent the development of neointimal hyperplasia following arterial injury and vascular bypass surgery. Currently, no effective therapy exists to prevent the development of neointimal hyperplasia. Therefore, the overall goal of this grant is to examine the mechanisms of NO-mediated inhibition of neointimal hyperplasia while also evaluating the clinical utility of biocompatible NO-eluting therapies. We hypothesize that biocompatible NO-eluting therapies will prevent the development of neointimal hyperplasia and that p53, heme oxygenase (HO), and the ubiquitin enzymes play a crucial role in this process.
Specific Aim 1 : Evaluate the effect of novel NO-eluting gels on the development of neointimal hvperplasia following arterial injury and vein bypass grafting. The rat carotid artery injury model and porcine carotid artery vein bypass model will be used to study the efficacy of the delivery vehicle, the optimal dose, toxicity, and the long-term durability of this therapy.
Specific Aim 2 : To determine the efficacy of a spontaneously releasing polymer cross-linked NO-eluting PTFE graft on the development of neointimal hvperplasia following prosthetic arterial bypass grafting. A porcine carotid artery bypass model will be used to study the efficacy of the NO-eluting PTFE graft, the optimal concentration, toxicity, and the long-term durability of this therapy.
Specific Aim 3 : Examine the mechanism by which NO induces VSMC apoptosis. Specifically, we will determine if p53 regulates HO-2 expression through post-transcriptional regulation. Additionally, we will determine which of the end products of heme metabolism by HO-2, namely carbon monoxide (CO), iron, or biliverdin, are responsible for preventing NO-induced VSMC apoptosis.
Specific Aim 4 : Examine the mechanism by which NO inhibits VSMC proliferation. Specifically, the role of the ubiquitin-activating, -conjugating, and -ligase enzymes in NO-mediated inhibition of VSMC proliferation will be evaluated. The data from this study will serve as the basis for further studies of NO-mediated inhibition of neointimal hyperplasia. (End of Abstract) ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Clinical Investigator Award (CIA) (K08)
Project #
5K08HL084203-02
Application #
7285701
Study Section
Special Emphasis Panel (ZHL1-CSR-O (F1))
Program Officer
Scott, Jane
Project Start
2006-09-15
Project End
2011-06-30
Budget Start
2007-07-01
Budget End
2008-06-30
Support Year
2
Fiscal Year
2007
Total Cost
$127,358
Indirect Cost

  Institution

Name
Northwestern University at Chicago
Department
Surgery
Type
Schools of Medicine
DUNS #
005436803
City
Chicago
State
IL
Country
United States
Zip Code
60611

  Publications

Gregory, Elaine K; Webb, Antonio; Vercammen, Janet M et al. (2018) Inhibiting intimal hyperplasia in prosthetic vascular grafts via immobilized all-trans retinoic acid. J Control Release 274:69-80
Bahnson, Edward S M; Vavra, Ashley K; Flynn, Megan E et al. (2016) Long-term effect of PROLI/NO on cellular proliferation and phenotype after arterial injury. Free Radic Biol Med 90:272-86
Bahnson, Edward S M; Koo, Nathaniel; Cantu-Medellin, Nadiezhda et al. (2015) Nitric oxide inhibits neointimal hyperplasia following vascular injury via differential, cell-specific modulation of SOD-1 in the arterial wall. Nitric Oxide 44:8-17
Rodriguez, Monica P; Emond, Zachary M; Wang, Zheng et al. (2014) Role of metabolic environment on nitric oxide mediated inhibition of neointimal hyperplasia in type 1 and type 2 diabetes. Nitric Oxide 36:67-75
Gregory, Elaine K; Webb, Antonio R; Vercammen, Janet M et al. (2014) Periadventitial atRA citrate-based polyester membranes reduce neointimal hyperplasia and restenosis after carotid injury in rats. Am J Physiol Heart Circ Physiol 307:H1419-29
Tsihlis, Nick D; Vavra, Ashley K; Martinez, Janet et al. (2013) Nitric oxide is less effective at inhibiting neointimal hyperplasia in spontaneously hypertensive rats. Nitric Oxide 35:165-74
Tsihlis, Nick D; Kapadia, Muneera R; Vavra, Ashley K et al. (2013) Nitric oxide may inhibit neointimal hyperplasia by decreasing isopeptidase T levels and activity in the vasculature. J Vasc Surg 58:179-86
Hogg, Melissa E; Vavra, Ashley K; Banerjee, Monisha N et al. (2012) The role of estrogen receptor ? and ? in regulating vascular smooth muscle cell proliferation is based on sex. J Surg Res 173:e1-10
Havelka, George E; Hogg, Melissa E; Martinez, Janet et al. (2011) Adventitial contributions of the extracellular signal-regulated kinase and Akt pathways to neointimal hyperplasia. Am J Surg 202:515-9
Oustwani, Chris S; Tsihlis, Nick D; Vavra, Ashley K et al. (2011) Nitric oxide increases lysine 48-linked ubiquitination following arterial injury. J Surg Res 170:e169-77

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