Novel Strategy to Drive the Intracellular Uptake of Lipid Nanoparticles for Photodynamic Therapy

Author:

Ho Tiffany12,Guidolin Keegan1,Makky Ali3,Valic Michael14,Ding Lili1,Bu Jiachuan1,Zheng Mark1,Cheng Miffy H. Y.1,Yau Jeremy2,Chen Juan1ORCID,Zheng Gang1245ORCID

Affiliation:

1. Princess Margaret Cancer Centre University Health Network 101 College Street, PMCRT 5-354 Toronto ON M5G1L7 Canada

2. Department of Pharmaceutical Sciences University of Toronto 144 College St. Toronto Toronto ON M5S 3M2 Canada

3. Université Paris-Saclay CNRS Institut Galien Paris-Saclay, Bâtiment Henri Moissan 91400 Orsay France

4. Institute of Biomedical Engineering University of Toronto 64 College St. Toronto ON M5S 3G9 Canada

5. Department of Medical Biophysics University of Toronto 101 College St. Toronto ON M5G 1L7 Canada

Abstract

AbstractNanoparticles’ uptake by cancer cells upon reaching the tumor microenvironment is often the rate‐limiting step in cancer nanomedicine. Herein, we report that the inclusion of aminopolycarboxylic acid conjugated lipids, such as EDTA‐ or DTPA‐hexadecylamide lipids in liposome‐like porphyrin nanoparticles (PS) enhanced their intracellular uptake by 25‐fold, which was attributed to these lipids’ ability to fluidize the cell membrane in a detergent‐like manner rather than by metal chelation of EDTA or DTPA. EDTA‐lipid‐incorporated‐PS (ePS) take advantage of its unique active uptake mechanism to achieve >95 % photodynamic therapy (PDT) cell killing compared to <5 % cell killing by PS. In multiple tumor models, ePS demonstrated fast fluorescence‐enabled tumor delineation within minutes post‐injection and increased PDT potency (100 % survival rate) compared to PS (60 %). This study offers a new nanoparticle cellular uptake strategy to overcome challenges associated with conventional drug delivery.

Funder

Terry Fox Research Institute

Canada Foundation for Innovation

Princess Margaret Cancer Foundation

Publisher

Wiley

Subject

General Chemistry,Catalysis

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