| Literature DB >> 11825339 |
Rainer Voisard1, Eva Kucharczyk, Ute Deininger, Regine Baur, Vinzenz Hombach.
Abstract
BACKGROUND: Strictly intravascular approaches for the treatment of postangioplasty restenosis are effective in the intima and the inner parts of the media but may be insufficient to control redundant pathways in the more outer parts of the media and the adventitia. An inverse situation may occur subsequently to a strictly extravascular approach, like the recently suggested pericardial approach in pigs. We hypothesized that simultaneous intra/extravascular administration of anti-restenotic agents inhibits restenosis by blocking all stimulatory pathways in the entire arterial wall.Entities:
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Year: 2002 PMID: 11825339 PMCID: PMC65511 DOI: 10.1186/1471-2261-2-2
Source DB: PubMed Journal: BMC Cardiovasc Disord ISSN: 1471-2261 Impact factor: 2.298
Figure 1Effect of simultaneous intra/extravascular administration of high dose diltiazem (50 μg/mL) for 1 – 7 days on time course of cells undergoing DNA synthesis in coronary organ cultures 7 (A) and 28 days (B) after ex vivo ballooning. The number of cells in the neointima with positive bromodeoxyuridine incorporation is depicted in relation to the total cell number.
Figure 2Micrographs showing serial sections of porcine coronary organ cultures at day 7, staining with BrdU (avidin /biotin method): untreated control (A), ex vivo ballooning (B)and ex vivo ballooning with simultaneous intra/extravascular antiproliferative drug therapy (C). arrows = cells with positive staining against BrdU.
Figure 3Effect of simultaneous intra/extravascular administration administration of high dose diltiazem (50 μg/mL) for 1 – 7 days on neointimal thickening in porcine organ cultures 7 (A) and 28 days (B) after ballooning. Each column represents five different vessels, * = p < 0.05.
Figure 4Micrographs of sections of porcine coronoary organ cultures at day 28, staining with elastica van gieson: untreated control (A), ex vivo ballooning (B) and ex vivo ballooning with simultaneous intra/extravascular antiproliferative drug therapy (C). arrow = area of neointimal thickening.