PLGA nanodepots co-encapsulating prostratin and anti-CD25 enhance primary natural killer cell antiviral and antitumor function

Authors

Elizabeth E. Sweeney, The George Washington University
Preethi B. Balakrishnan, The George Washington University
Allison B. Powell, Childrens National Health System
Allan Bowen, The George Washington University
Indra Sarabia, The George Washington University
Rachel A. Burga, The George Washington University
R. Brad Jones, Weill Cornell Medicine
Alberto Bosque, The George Washington University
C. Russell Y. Cruz, The George Washington University
Rohan Fernandes, The George Washington University

Document Type

Journal Article

Publication Date

3-1-2020

Journal

Nano Research

Volume

13

Issue

3

DOI

10.1007/s12274-020-2684-1

Keywords

antibody; cancer; human immunodeficiency virus (HIV); latency-reversing agent; natural killer (NK) cells; poly(lactic-co-glycolic acid) (PLGA) nanodepots

Abstract

© 2020, Tsinghua University Press and Springer-Verlag GmbH Germany, part of Springer Nature. Natural killer (NK) cells are attractive effector cells of the innate immune system against human immunodeficiency virus (HIV) and cancer. However, NK cell therapies are limited by the fact that target cells evade NK cells, for example, in latent reservoirs (in HIV) or through upregulation of inhibitory signals (in cancer). To address this limitation, we describe a biodegradable nanoparticlebased “priming” approach to enhance the cytotoxic efficacy of peripheral blood mononuclear cell-derived NK cells. We present poly(lactic-co-glycolic acid) (PLGA) nanodepots (NDs) that co-encapsulate prostratin, a latency-reversing agent, and anti-CD25 (aCD25), a cell surface binding antibody, to enhance primary NK cell function against HIV and cancer. We utilize a nanoemulsion synthesis scheme to encapsulate both prostratin and aCD25 within the PLGA NDs (termed Pro-aCD25-NDs). Physicochemical characterization studies of the NDs demonstrated that our synthesis scheme resulted in stable and monodisperse Pro-aCD25- NDs. The NDs successfully released both active prostratin and anti-CD25, and with controllable release kinetics. When Pro-aCD25-NDs were administered in an in vitro model of latent HIV and acute T cell leukemia using J-Lat 10.6 cells, the NDs were observed to prime J-Lat cells resulting in significantly increased NK cell-mediated cytotoxicity compared to free prostratin plus anti-CD25, and other controls. These findings demonstrate the feasibility of using our Pro-aCD25-NDs to prime target cells for enhancing the cytotoxicity of NK cells as antiviral or antitumor agents. [Figure not available: see fulltext.]

APA Citation

Sweeney, E., Balakrishnan, P., Powell, A., Bowen, A., Sarabia, I., Burga, R., Jones, R., Bosque, A., Cruz, C., & Fernandes, R. (2020). PLGA nanodepots co-encapsulating prostratin and anti-CD25 enhance primary natural killer cell antiviral and antitumor function. Nano Research, 13 (3). http://dx.doi.org/10.1007/s12274-020-2684-1