Hyaluronan Nanoparticles Selectively Target Plaque-Associated Macrophages and Improve Plaque Stability in Atherosclerosis

被引:157
作者
Beldman, Thijs J. [1 ]
Senders, Max L. [1 ]
Alaarg, Amr [3 ,5 ]
Perez-Medina, Carlos [3 ]
Tang, Jun [3 ,4 ]
Zhao, Yiming [3 ]
Fay, Francois [3 ]
Deichmoller, Jacqueline [6 ,8 ]
Born, Benjamin [6 ]
Desclos, Emilie [2 ]
van der Wel, Nicole N. [2 ]
Hoebe, Ron A. [2 ]
Kohen, Fortune [6 ]
Kartvelishvily, Elena [7 ]
Neeman, Michal [6 ]
Reiner, Thomas [4 ,9 ]
Calcagno, Claudia [3 ]
Fayad, Zahi A. [3 ]
de Winther, Menno P. J. [1 ,10 ]
Lutgens, Esther [1 ,10 ]
Mulder, Willem J. M. [1 ,3 ]
Kluza, Ewelina [1 ]
机构
[1] Acad Med Ctr, Expt Vasc Biol, Dept Med Biochem, NL-1105 AZ Amsterdam, Netherlands
[2] Acad Med Ctr, Cellular Imaging, AMC Core Facil, NL-1105 AZ Amsterdam, Netherlands
[3] Mt Sinai Sch Med, Dept Radiol, New York, NY 10029 USA
[4] Mem Sloan Kettering Canc Ctr, Dept Radiol, New York, NY 10065 USA
[5] Univ Twente, MIRA Inst Biomed Technol & Tech Med, Dept Biomat Sci & Technol, NL-7522 NB Enschede, Netherlands
[6] Weizmann Inst Sci, Dept Biol Regulat, IL-7610001 Rehovot, Israel
[7] Weizmann Inst Sci, Dept Chem Res Support, IL-7610001 Rehovot, Israel
[8] Ruhr Univ Bochum, Phys Chem 2, D-44801 Bochum, Germany
[9] Weill Cornell Med Coll, Dept Radiol, New York, NY 10065 USA
[10] Ludwig Maximilians Univ Munchen, Inst Cardiovasc Prevent, D-80336 Munich, Germany
基金
美国国家卫生研究院;
关键词
hyaluronan nanoparticles; atherosclerosis; inflammation; PET imaging anti-inflammatory effects; antiatherogenic therapy; IN-VIVO PET; PHYSICOCHEMICAL PROPERTIES; MONOCLONAL-ANTIBODIES; ACID NANOPARTICLES; RECEPTOR; CANCER; PATHOGENESIS; CLEARANCE; MURINE; CD44;
D O I
10.1021/acsnano.7b01385
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Hyaluronan is a biologically active polymer, which can be formulated into nanoparticles. In our study, we aimed to probe atherosclerosis-associated inflammation by using hyaluronan nanoparticles and to determine whether they can ameliorate atherosclerosis. Hyaluronan nanoparticles (HA-NPs) were prepared by reacting amine-functionalized oligomeric hyaluronan (HA) with cholanic ester and labeled with a fluorescent or radioactive label. HA-NPs were characterized in vitro by several advanced microscopy methods. The targeting properties and biodistribution of HA-NPs were studied in apoe(-/-) mice, which received either fluorescent or radiolabeled HA-NPs and were examined ex vivo by flow cytometry or nuclear techniques. Furthermore, three atherosclerotic rabbits received Zr-89-HA-NPs and were imaged by PET/MRI. The therapeutic effects of HA-NPs were studied in apoe(-/-) mice, which received weekly doses of 50 mg/kg HA-NPs during a 12-week high-fat diet feeding period. Hydrated HA-NPs were ca. 90 nm in diameter and displayed very stable morphology under hydrolysis conditions. Flow cytometry revealed a 6- to 40-fold higher uptake of Cy7-HA-NPs by aortic macrophages compared to normal tissue macrophages. Interestingly, both local and systemic HA-NP immune cell interactions significantly decreased over the disease progression. Zr-89-HA-NPs-induced radioactivity in atherosclerotic aortas was 30% higher than in wild-type controls. PET imaging of rabbits revealed 6-fold higher standardized uptake values compared to the muscle. The plaques of HA-NP-treated mice contained 30% fewer macrophages compared to control and free HA-treated group. In conclusion, we show favorable targeting properties of HA-NPs, which can be exploited for PET imaging of atherosclerosis-associated inflammation. Furthermore, we demonstrate the anti-inflammatory effects of HA-NPs in atherosclerosis.
引用
收藏
页码:5785 / 5799
页数:15
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