期刊
JOURNAL OF THE AMERICAN HEART ASSOCIATION
卷 4, 期 2, 页码 -出版社
WILEY-BLACKWELL
DOI: 10.1161/JAHA.114.001477
关键词
arteriosclerosis; coronary disease; darapladib; inflammation; lipoprotein-associated phospholipase A(2); peripheral vascular disease
资金
- GlaxoSmithKline
- University of Pennsylvania School of Medicine
Background-Despite systemic exposure to risk factors, the circulatory system develops varying patterns of atherosclerosis for unclear reasons. In a porcine model, we investigated the relationship between site-specific lesion development and inflammatory pathways involved in the coronary arteries (CORs) and distal abdominal aortas (AAs). Methods and Results-Diabetes mellitus (DM) and hypercholesterolemia (HC) were induced in 37 pigs with 3 healthy controls. Site-specific plaque development was studied by comparing plaque severity, macrophage infiltration, and inflammatory gene expression between CORs and AAs of 17 DM/HC pigs. To assess the role of lipoprotein-associated phospholipase A(2) (Lp-PLA(2)) in plaque development, 20 DM/HC pigs were treated with the Lp-PLA2 inhibitor darapladib and compared with the 17 DM/HC untreated pigs. DM/HC caused site-specific differences in plaque severity. In the AAs, normalized plaque area was 4.4-fold higher (P< 0.001) and there were more fibroatheromas (9 of the 17 animals had a fibroatheroma in the AA and not the COR, P= 0.004), while normalized macrophage staining area was 1.5-fold higher (P= 0.011) compared with CORs. DM/HC caused differential expression of 8 of 87 atherosclerotic genes studied, including 3 important in inflammation with higher expression in the CORs. Darapladib-induced attenuation of normalized plaque area was site-specific, as CORs responded 2.9-fold more than AAs (P= 0.045). Conclusions-While plaque severity was worse in the AAs, inflammatory genes and inflammatory pathways that use Lp-PLA(2) were more important in the CORs. Our results suggest fundamental differences in inflammation between vascular sites, an important finding for the development of novel anti-inflammatory therapeutics.
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