Immune cell screening of a nanoparticle library improves atherosclerosis therapy

Author:

Tang JunORCID,Baxter Samantha,Menon Arjun,Alaarg Amr,Sanchez-Gaytan Brenda L.,Fay Francois,Zhao Yiming,Ouimet Mireille,Braza Mounia S.,Longo Valerie A.,Abdel-Atti Dalya,Duivenvoorden Raphael,Calcagno Claudia,Storm Gert,Tsimikas Sotirios,Moore Kathryn J.,Swirski Filip K.,Nahrendorf Matthias,Fisher Edward A.,Pérez-Medina Carlos,Fayad Zahi A.,Reiner Thomas,Mulder Willem J. M.

Abstract

Immunological complexity in atherosclerosis warrants targeted treatment of specific inflammatory cells that aggravate the disease. With the initiation of large phase III trials investigating immunomodulatory drugs for atherosclerosis, cardiovascular disease treatment enters a new era. We here propose a radically different approach: implementing and evaluating in vivo a combinatorial library of nanoparticles with distinct physiochemical properties and differential immune cell specificities. The library’s nanoparticles are based on endogenous high-density lipoprotein, which can preferentially deliver therapeutic compounds to pathological macrophages in atherosclerosis. Using the apolipoprotein E-deficient (Apoe−/−) mouse model of atherosclerosis, we quantitatively evaluated the library’s immune cell specificity by combining immunological techniques and in vivo positron emission tomography imaging. Based on this screen, we formulated a liver X receptor agonist (GW3965) and abolished its liver toxicity while still preserving its therapeutic function. Screening the immune cell specificity of nanoparticles can be used to develop tailored therapies for atherosclerosis and other inflammatory diseases.

Funder

DH | National Institute for Health Research

Foundation for the National Institutes of Health

HHS | NIH | National Cancer Institute

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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