Systemic targeted delivery of antisense with perflourobutane gas microbubble carrier reduced neointimal formation in the porcine coronary restenosis model

The antisense phosphorodiamidate morpholino oligomer (PMO), AVI-4126, has been effective in reducing neointimal formation in animal models following delivery by pluronic gels, local delivery catheters and coated stents. Greater flexibility of repeated-dosage regimens and reduced procedure complexity...

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Published in:Cardiovascular radiation medicine 2003-07, Vol.4 (3), p.152-159
Main Authors: Kipshidze, Nicholas N., Porter, Thomas R., Dangas, George, Yazdi, Hamid, Tio, Fermin, Xie, Feng, Hellinga, David, Fournadjiev, Jana, Wolfram, Roswitha, Seabron, Rufus, Waksman, Ron, Abizaid, Alexander, Roubin, Gary, Iyer, Sriram, Leon, Martin B., Moses, Jeffrey W., Iversen, Patrick
Format: Article
Language:English
Subjects:
Animals
Antisense
Blood Vessel Prosthesis Implantation
Blotting, Western
Coronary Restenosis - etiology
Coronary Restenosis - metabolism
Coronary Restenosis - pathology
Disease Models, Animal
Female
Fluorocarbons - pharmacokinetics
Genes, myc - drug effects
Infusion Pumps, Implantable
Male
Microbubbles
Models, Cardiovascular
Morpholines - pharmacokinetics
Morpholinos
Nanoparticles
Oligonucleotides, Antisense - pharmacokinetics
Restenosis
Stents
Swine
Tunica Intima - drug effects
Tunica Intima - metabolism
Tunica Intima - pathology
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Summary:The antisense phosphorodiamidate morpholino oligomer (PMO), AVI-4126, has been effective in reducing neointimal formation in animal models following delivery by pluronic gels, local delivery catheters and coated stents. Greater flexibility of repeated-dosage regimens and reduced procedure complexity may be provided by systemic injection of AVI-4126 bound to perfluorobutane gas microbubble carriers. The purpose of this study was to investigate the effects of perfluorocarbon gas microbubble carrier (PGMC)-based systemic delivery of AVI-4126 on expression of the c- myc in vascular tissue and restenosis after stent implantation. Seven pigs underwent stent implantation (3 stents/animal). Five pigs received IV injection of PGMC and 2 mg of AVI-4126 (AVI BioPharma). Two served as control. Four hours postprocedure, 3 pigs were sacrificed and stented segments analyzed by high-performance liquid chromatography (HPLC) and Western blot. In chronic experiments, 4 pigs (12 stent sites) were sacrificed at 28 days. HPLC analysis of plasma samples of treated animals showed minimal presence of AVI-4126. HPLC of the treated arteries demonstrated easily detected concentrations of AVI-4126. Western blot analysis of the stented vessels demonstrated modest inhibition of c- myc. Morphometry showed that the neointimal area was significantly reduced in the AVI-4126/PGMC group compared with control (2.63±1.99 vs. 4.77±.1.71 mm 2, respectively, P
ISSN:1522-1865
DOI:10.1016/S1522-1865(03)00184-7