Your search keyword '"Coleen A. McNamara"' showing total 4 results

1. Hyperlipemia and Oxidation of LDL Induce Vascular Smooth Muscle Cell Growth: An Effect Mediated by the HLH Factor Id3

Author

Sarah C. Rutherford, Coleen A. McNamara, Ian J. Sarembock, Angela M. Taylor, Feng Li, Scott Forrest, Ross G. Gerrity, and Pushpa Thimmalapura

Subjects

Cyclin-Dependent Kinase Inhibitor p21, Male, medicine.medical_specialty, Vascular smooth muscle, Swine, Physiology, Blotting, Western, Hypercholesterolemia, Cell, Biology, Article, Muscle, Smooth, Vascular, S Phase, Mice, chemistry.chemical_compound, Mediator, Internal medicine, medicine, Animals, Humans, Transcription factor, Cell Proliferation, DNA synthesis, Cholesterol, Cell growth, Helix-Loop-Helix Motifs, musculoskeletal system, Lipoproteins, LDL, Endocrinology, medicine.anatomical_structure, chemistry, cardiovascular system, Inhibitor of Differentiation Proteins, lipids (amino acids, peptides, and proteins), Cardiology and Cardiovascular Medicine, Lipoprotein

Abstract

Hyperlipemia and oxidized LDL (ox-LDL) are important independent cardiovascular risk factors. Ox-LDL has been shown to stimulate vascular smooth muscle cell (VSMC) proliferation. However, the effects of hyperlipemia and the molecular mechanisms mediating hyperlipemia and ox-LDL effects on VSMC growth are poorly understood. The helix-loop-helix (HLH) transcription factor, Id3, is a redox-sensitive gene expressed in VSMC in response to mitogen stimulation and vascular injury. Accordingly, we hypothesize that Id3 is an important mediator of ox-LDL and hyperlipemia-induced VSMC growth. Aortas harvested from hyperlipemic pigs demonstrated significantly more Id3 than normolipemic controls. Primary VSMC were stimulated with ox-LDL, native LDL, sera from hyperlipemic pigs, or normolipemic pigs. VSMC exposed to hyperlipemic sera demonstrated increased Id3 expression, VSMC growth and S-phase entry and decreased p21cip1 expression and transcription. Cells stimulated with ox-LDL demonstrated similar findings of increased growth and Id3 expression and decreased p21cip1 expression. Moreover, the effects of ox-LDL on growth were abolished in cells devoid of the Id3 gene. Results provide evidence that the HLH factor Id3 mediates the mitogenic effect of hyperlipemic sera and ox-LDL in VSMC via inhibition of p21cip1 expression, subsequently increasing DNA synthesis and proliferation.

Published

2006

2. Local adenovirus-mediated delivery of hirudin in a rabbit arterial injury model

Author

Coleen A. McNamara, Lawrence W. Gimple, Sean Hesselbacher, Gary K. Owens, John A. McPherson, Eric R. Powers, John E. Humphries, Gregory G. Bishop, Salah Din, Pete Wiegman, Ian J. Sarembock, David Dickek, John M. Sanders, Marie-Louise Hammarskjold, Michael Ragosta, and Michael J. Feldman

Subjects

Physiology, Arteriosclerosis, Genetic Vectors, Hirudin, Inflammation, Femoral artery, Pharmacology, medicine.disease_cause, Antithrombins, Restenosis, Hirudin Therapy, medicine.artery, medicine, Animals, Humans, Lagomorpha, biology, business.industry, Adenoviruses, Human, Gene Transfer Techniques, Thrombin, Hirudins, biology.organism_classification, medicine.disease, Adenoviridae, Femoral Artery, Disease Models, Animal, medicine.anatomical_structure, Anesthesia, Circulatory system, Rabbits, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Angioplasty, Balloon, medicine.drug, Blood vessel

Abstract

Intravascular delivery of an E1/E3 deleted adenovirus encoding the hirudin protein reduces neointimal formation in the rat arterial injury model. Given the interspecies variability in response to adenoviral vectors, we tested this same construct in the hirudin-sensitive cholesterol-fed rabbit arterial balloon injury model. We hypothesized that local delivery of an E1/E3-deleted adenovirus encoding hirudin (Ad-Hir) in addition to early hirudin infusion would limit neointimal formation compared to early hirudin alone. Methods and Results: Local delivery of Ad-Hir, 2.5 × 1010 PFU/ml, using a double balloon catheter [n = 6 vessels (v)] produced a 79% reduction in vessel wall thrombin activity at 48 h after balloon angioplasty (BA) compared with vehicle (Veh, n = 6v; p = 0.05). In chronic experiments, hypercholesterolemic rabbits underwent femoral BA, and received either early hirudin alone (n = 9v) or early hirudin plus locally delivered Ad-Hir (early hirudin + Ad-Hir; n = 9v), an E1/E3-deleted adenovirus encoding β-galactosidase (early hirudin + AdGal; n = 7v), or Veh (early hirudin + Veh; n = 10v). Early hirudin + Ad-Hir did not limit the arterial response to injury versus the other groups at 4 weeks after BA. Plaque area, cross-sectional luminal area narrowing by plaque, and T cell infiltration were significantly increased in the adenovirus- versus non-adenovirus-treated arteries. Plaque area correlated with T cell density. Conclusion: Following BA in cholesterol-fed rabbits, local transduction with A-Hir produced a marked reduction in vessel wall-associated thrombin activity. However, this strategy increased rather than decreased the arterial response to BA injury. Our results suggest that the lack of therapeutic effect resulted from adenovirus-stimulated plaque formation, possibly resulting from a T cell-mediated inflammatory response.

Published

1999

3. Editorial: The JVR Internet Discussion Forum

Author

Ian J. Sarembock, John A. McPherson, Derek L. Connolly, B. Risberg, D. Guelfi, Enzo Porteri, L.E. Olson, K. Messmer, John M. Sanders, Allison W. Miller, Gary K. Owens, Coleen A. McNamara, Damiano Rizzoni, Lawrence Magliola, David Manka, John E. Humphries, Kerry L. Tyson, Jane K. Osbourn, Peter L. Weissberg, C.M. Almgren, A. Veihelmann, John Sanders, Catherine M. Shanahan, Sean Hesselbacher, R C Webb, Giancarlo Pasini, Eric R. Powers, Alfonso Piccoli, David Dickek, Pete Wiegman, Lawrence W. Gimple, Michael J. Feldman, Samuel A. Green, Maria Lorenza Muiesan, Salah Din, Maurizio Castellano, Prasad V. G. Katakam, Michael R. Ujhelyi, Fritz Krombach, Gregory G. Bishop, Peter Wiegman, H. J. Refior, Enrico Agabiti Rosei, Marie-Louise Hammarskjold, Nathaniel R.B. Cary, H. Karaki, Allan W. Jones, Michael Ragosta, Peter Agre, and Klaus Ley

Subjects

Physiology, business.industry, Medicine, Library science, The Internet, Cardiology and Cardiovascular Medicine, business

Published

1999

4. Selected Comments on and Replies to the Article

Author

David Manka, Coleen A. McNamara, Jane K. Osbourn, Samuel A. Green, Maria Lorenza Muiesan, Allison W. Miller, Alfonso Piccoli, Gary K. Owens, D. Guelfi, Damiano Rizzoni, Lawrence Magliola, C.M. Almgren, Prasad V. G. Katakam, Eric R. Powers, Sean Hesselbacher, Ian J. Sarembock, R C Webb, Michael J. Feldman, L.E. Olson, Peter Agre, Derek L. Connolly, John M. Sanders, Klaus Ley, John Sanders, John E. Humphries, Peter L. Weissberg, John A. McPherson, Pete Wiegman, B. Risberg, Peter Wiegman, Michael R. Ujhelyi, Enzo Porteri, A. Veihelmann, Catherine M. Shanahan, Fritz Krombach, David Dickek, Gregory G. Bishop, Allan W. Jones, Kerry L. Tyson, Michael Ragosta, Enrico Agabiti Rosei, Marie-Louise Hammarskjold, Nathaniel R.B. Cary, H. J. Refior, H. Karaki, Giancarlo Pasini, Lawrence W. Gimple, Maurizio Castellano, Salah Din, and K. Messmer

Subjects

Physiology, Cardiology and Cardiovascular Medicine

Published

1999