Caveolin-1 Regulates Atherogenesis by Attenuating Low-Density Lipoprotein Transcytosis and Vascular Inflammation Independently of Endothelial Nitric Oxide Synthase Activation.
| Citation | . “Caveolin-1 Regulates Atherogenesis By Attenuating Low-Density Lipoprotein Transcytosis And Vascular Inflammation Independently Of Endothelial Nitric Oxide Synthase Activation.”. Circulation, pp. 225-239. |
| Center | Yale University |
| Author | Cristina M Ramírez, Xinbo Zhang, Chirosree Bandyopadhyay, Noemi Rotllan, Michael G Sugiyama, Binod Aryal, Xinran Liu, Shun He, Jan R Kraehling, Victoria Ulrich, Chin Sheng Lin, Heino Velazquez, Miguel A Lasunción, Guangxin Li, Yajaira Suárez, George Tellides, Filip K Swirski, Warren L Lee, Martin A Schwartz, William C Sessa, Carlos Fernández-Hernando |
| Keywords | atherosclerosis, caveolae, Extracellular matrix, fibronectins, inflammation, nitric oxide synthase type III, transcytosis |
| Abstract |
BACKGROUND: Atherosclerosis is driven by synergistic interactions between pathological, biomechanical, inflammatory, and lipid metabolic factors. Our previous studies demonstrated that absence of caveolin-1 (Cav1)/caveolae in hyperlipidemic mice strongly inhibits atherosclerosis, which was attributed to activation of endothelial nitric oxide (NO) synthase (eNOS) and increased production of NO and reduced inflammation and low-density lipoprotein trafficking. However, the contribution of eNOS activation and NO production in the athero-protection of Cav1 and the exact mechanisms by which Cav1/caveolae control the pathogenesis of diet-induced atherosclerosis are still not clear. METHODS: Triple-knockout mouse lacking expression of eNOS, Cav1, and Ldlr were generated to explore the role of NO production in Cav1-dependent athero-protective function. The effects of Cav1 on lipid trafficking, extracellular matrix remodeling, and vascular inflammation were studied both in vitro and in vivo with a mouse model of diet-induced atherosclerosis. The expression of Cav1 and distribution of caveolae regulated by flow were analyzed by immunofluorescence staining and transmission electron microscopy. RESULTS: We found that absence of Cav1 significantly suppressed atherogenesis in LdlreNOS mice, demonstrating that athero-suppression is independent of increased NO production. Instead, we find that the absence of Cav1/caveolae inhibited low-density lipoprotein transport across the endothelium and proatherogenic fibronectin deposition and disturbed flow-mediated endothelial cell inflammation. Consistent with the idea that Cav1/caveolae may play a role in early flow-dependent inflammatory priming, distinct patterns of Cav1 expression and caveolae distribution were observed in athero-prone and athero-resistant areas of the aortic arch even in wild-type mice. CONCLUSIONS: These findings support a role for Cav1/caveolae as a central regulator of atherosclerosis that links biomechanical, metabolic, and inflammatory pathways independently of endothelial eNOS activation and NO production. |
| Year of Publication |
2019
|
| Journal |
Circulation
|
| Volume |
140
|
| Issue |
3
|
| Number of Pages |
225-239
|
| Date Published |
12/2019
|
| ISSN Number |
1524-4539
|
| DOI |
10.1161/CIRCULATIONAHA.118.038571
|
| Alternate Journal |
Circulation
|
| PMID |
31154825
|
| PMCID |
PMC6778687
|
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