Probing nanoparticle translocation across the permeable endothelium in experimental atherosclerosis

YongTae Kim(Georgia Institute of Technology), Mark E. Lobatto(Amsterdam UMC Location University of Amsterdam), Tomohiro Kawahara(Kyushu Institute of Technology), Bomy Lee Chung(Allen Institute), Aneta J. Mieszawska(Imaging Center), Brenda L. Sánchez-Gaytán(Imaging Center), François Fay(Imaging Center), Max L. Senders(Imaging Center), Claudia Calcagno(Imaging Center), Jacob Becraft(Biological E (India)), May Tun Saung(Boston University), Ronald E. Gordon(Mount Sinai Hospital), Erik S.G. Stroes(Amsterdam UMC Location University of Amsterdam), Mingming Ma(Allen Institute), Omid C. Farokhzad(Brigham and Women's Hospital), Zahi A. Fayad(Imaging Center), Willem J. M. Mulder(Amsterdam UMC Location University of Amsterdam), Róbert Langer(Harvard–MIT Division of Health Sciences and Technology)
Proceedings of the National Academy of Sciences
January 6, 2014
Cited by 188Open Access
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Abstract

Therapeutic and diagnostic nanomaterials are being intensely studied for several diseases, including cancer and atherosclerosis. However, the exact mechanism by which nanomedicines accumulate at targeted sites remains a topic of investigation, especially in the context of atherosclerotic disease. Models to accurately predict transvascular permeation of nanomedicines are needed to aid in design optimization. Here we show that an endothelialized microchip with controllable permeability can be used to probe nanoparticle translocation across an endothelial cell layer. To validate our in vitro model, we studied nanoparticle translocation in an in vivo rabbit model of atherosclerosis using a variety of preclinical and clinical imaging methods. Our results reveal that the translocation of lipid-polymer hybrid nanoparticles across the atherosclerotic endothelium is dependent on microvascular permeability. These results were mimicked with our microfluidic chip, demonstrating the potential utility of the model system.


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