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Literature DB >> 8690797

Regulation of cellular proliferation and intimal formation following balloon injury in atherosclerotic rabbit arteries.

R D Simari¹, H San, M Rekhter, T Ohno, D Gordon, G J Nabel, E G Nabel.

Abstract

Injury to atherosclerotic arteries induces the expression of growth regulatory genes that stimulate cellular proliferation and intimal formation. Intimal expansion has been reduced in vivo in nonatherosclerotic balloon-injured arteries by transfer of genes that inhibit cell proliferation. It is not known, however, whether vascular cell proliferation can be inhibited after injury in more extensively diseased atherosclerotic arteries. Accordingly, the purpose of this study was to investigate whether expression of recombinant genes in atherosclerotic arteries after balloon injury could inhibit intimal cell proliferation. To test this hypothesis, we examined the response to balloon injury in atherosclerotic rabbit arteries after gene transfer of herpesvirus thymidine kinase gene (tk) and administration of ganciclovir. Smooth muscle cells from hyperlipidemic rabbit arteries infected with adenoviral vectors encoding tk were sensitive to ganciclovir, and bystander killing was observed in vitro. In atherosclerotic arteries, a human placental alkaline phosphatase reporter gene was expressed in intimal and medial smooth muscle cells and macrophages, identifying these cells as targets for gene transfer. Expression of tk in balloon-injured hyperlipidemic rabbit arteries followed by ganciclovir treatment resulted in a 64% reduction in intimal cell proliferation 7 d after gene transfer (P = 0.004), and a 35-49% reduction in internal area 21 d after gene transfer, compared with five different control groups (P < 0.05). Replication of smooth muscle cells and macrophages was inhibited by tk expression and ganciclovir treatment. These findings indicate that transfer of a gene that inhibits cellular proliferation limits the intimal area in balloon-injured atherosclerotic arteries. Molecular approaches to the inhibition of cell proliferation in atherosclerotic arteries constitute a possible treatment for vascular proliferative diseases.

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Year: 1996 PMID： 8690797 PMCID： PMC507420 DOI： 10.1172/JCI118770

Source DB: PubMed Journal: J Clin Invest ISSN： 0021-9738 Impact factor: 14.808

43 in total

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Authors: A J Cohen; B Weiser; Q Afzal; J Fuhrer
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Authors: D P Faxon; T A Sanborn; V J Weber; C Haudenschild; S B Gottsman; W A McGovern; T J Ryan
Journal: Arteriosclerosis Date: 1984 May-Jun

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13 in total

Review 1. Nonviral gene transfer strategies for the vasculature.

Authors: Jennifer L Young; David A Dean
Journal: Microcirculation Date: 2002-01 Impact factor: 2.628

2. Requirements for enhanced transgene expression by untranslated sequences from the human cytomegalovirus immediate-early gene.

Authors: R D Simari; Z Y Yang; X Ling; D Stephan; N D Perkins; G J Nabel; E G Nabel
Journal: Mol Med Date: 1998-11 Impact factor: 6.354

10. Vascular-directed tissue factor pathway inhibitor overexpression regulates plasma cholesterol and reduces atherosclerotic plaque development.

Authors: Shuchong Pan; Thomas A White; Tyra A Witt; Anca Chiriac; Cheri S Mueske; Robert D Simari
Journal: Circ Res Date: 2009-08-27 Impact factor: 17.367

Regulation of cellular proliferation and intimal formation following balloon injury in atherosclerotic rabbit arteries.

1. Antisense c-myb oligonucleotides inhibit intimal arterial smooth muscle cell accumulation in vivo.

2. Time course of smooth muscle cell proliferation in the intima and media of arteries following experimental angioplasty.

3. Macrophage and smooth muscle cell proliferation in atherosclerotic lesions of WHHL and comparably hypercholesterolemic fat-fed rabbits.

4. Rapid colorimetric assay for cellular growth and survival: application to proliferation and cytotoxicity assays.

5. Ventricular tachycardia in two patients with AIDS receiving ganciclovir (DHPG).

6. Restenosis following transluminal angioplasty in experimental atherosclerosis.

7. Inhibition of cellular ras prevents smooth muscle cell proliferation after vascular injury in vivo.

8. Effect of lovastatin on intimal hyperplasia after balloon angioplasty: a study in an atherosclerotic hypercholesterolemic rabbit.

9. In vivo gene transfer with retroviral vector-producer cells for treatment of experimental brain tumors.

10. Genetic transformation of mouse embryos by microinjection of purified DNA.

Review 1. Nonviral gene transfer strategies for the vasculature.

2. Requirements for enhanced transgene expression by untranslated sequences from the human cytomegalovirus immediate-early gene.

3. Transcriptional targeting of replication-defective adenovirus transgene expression to smooth muscle cells in vivo.

4. 2014 Association of American Physicians George M. Kober Medal. Introduction of Elizabeth G. Nabel.

5. A Metabolic Intravascular Platform to Study FDG Uptake in Vascular Injury.

Review 6. Forging the Fate of Cellular Therapies for Cardiovascular Disease.

Review 7. Cardiovascular gene delivery: The good road is awaiting.

Review 8. Applied gene therapy in preclinical models of vascular injury.

Review 9. Gene therapy for restenosis: current status.

10. Vascular-directed tissue factor pathway inhibitor overexpression regulates plasma cholesterol and reduces atherosclerotic plaque development.