| Literature DB >> 24829311 |
Wijnand K den Dekker1, Dennie Tempel1, Lambert Speelman2, Jeroen Huizingh1, Allan Ramos1, Frank J Gijsen2, Jolanda J Wentzel2, Caroline Cheng3, Henricus J Duckers4.
Abstract
Previously, we created an experimental murine model for the induction of vulnerable plaque (VP). Although this murine model offers the opportunity to study the different molecular biological pathways that regulate plaque destabilization, the size of the animals severely limits the use of the model for in vivo diagnostics and percutaneous interventions. This study aimed to create a VP model in the rabbit, based on the murine model, to aid the assessment and development of novel diagnostic and interventional tools. New Zealand white rabbits were fed on a 2% cholesterol diet. After 1 week, a shear stress-altering device was implanted around the right carotid artery. Twelve weeks after cast placement, the carotid artery was isolated and processed for (immuno-)histological analysis to evaluate the presence of a VP phenotype. Atherosclerotic plaques with high lipid and macrophage content, low vascular smooth muscle cell content and intimal neovascularization were located upstream and downstream of the cast. The plaques lacked a significant necrotic core. In conclusion, we were able to create atherosclerotic plaques with a phenotype beyond that of a fatty streak, with a high percentage of lipids and macrophages, a thick cap with some vascular smooth muscle cells and neovascularization. However, as there was only a small necrotic core, the overall phenotype seems less vulnerable as compared to the thin fibrous cap atheroma in patients.Entities:
Keywords: angiogenesis; atherosclerosis; endothelium; hypercholesterolemia; rabbit; vulnerable plaque
Year: 2014 PMID: 24829311 DOI: 10.1177/1358863X14529006
Source DB: PubMed Journal: Vasc Med ISSN: 1358-863X Impact factor: 3.239