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Effective atherosclerotic plaque inflammation inhibition with targeted drug delivery by hyaluronan conjugated atorvastatin nanoparticles.
Citation | “Effective Atherosclerotic Plaque Inflammation Inhibition With Targeted Drug Delivery By Hyaluronan Conjugated Atorvastatin Nanoparticles.”. Nanoscale, pp. 9541-9556. . |
Center | University of Michigan |
Author | Seyedmehdi Hossaini Nasr, Zahra Rashidijahanabad, Sherif Ramadan, Nate Kauffman, Narayanan Parameswaran, Kurt R Zinn, Chunqi Qian, Ripla Arora, Dalen Agnew, Xuefei Huang |
Abstract |
Atherosclerosis is associated with inflammation in the arteries, which is a major cause of heart attacks and strokes. Reducing the extent of local inflammation at atherosclerotic plaques can be an attractive strategy to combat atherosclerosis. While statins can exhibit direct anti-inflammatory activities, the high dose required for such a therapy renders it unrealistic due to their low systemic bioavailabilities and potential side effects. To overcome this, a new hyaluronan (HA)-atorvastatin (ATV) conjugate was designed with the hydrophobic statin ATV forming the core of the nanoparticle (HA-ATV-NP). The HA on the NPs can selectively bind with CD44, a cell surface receptor overexpressed on cells residing in atherosclerotic plaques and known to play important roles in plaque development. HA-ATV-NPs exhibited significantly higher anti-inflammatory effects on macrophages compared to ATV alone in vitro. Furthermore, when administered in an apolipoprotein E (ApoE)-knockout mouse model of atherosclerosis following a 1-week treatment regimen, HA-ATV-NPs markedly decreased inflammation in advanced atherosclerotic plaques, which were monitored through contrast agent aided magnetic resonance imaging. These results suggest CD44 targeting with HA-ATV-NPs is an attractive strategy to reduce harmful inflammation in atherosclerotic plaques. |
Year of Publication |
2020
|
Journal |
Nanoscale
|
Volume |
12
|
Issue |
17
|
Number of Pages |
9541-9556
|
Date Published |
05/2020
|
ISSN Number |
2040-3372
|
DOI |
10.1039/d0nr00308e
|
Alternate Journal |
Nanoscale
|
PMID |
32314997
|
PMCID |
PMC7234819
|
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