Anti-EGFR Targeted Multifunctional I-131 Radio-Nanotherapeutic for Treating Osteosarcoma: In Vitro 3D Tumor Spheroid Model

Suphalak Khamruang Marshall; Boonyisa Saelim; Maneerat Taweesap; Verachai Pachana; Yada Panrak; Naritsara Makchuchit; Passara Jaroenpakdee

doi:10.3390/nano12193517

Anti-EGFR Targeted Multifunctional I-131 Radio-Nanotherapeutic for Treating Osteosarcoma: In Vitro 3D Tumor Spheroid Model

Nanomaterials (Basel). 2022 Oct 8;12(19):3517. doi: 10.3390/nano12193517.

Authors

Suphalak Khamruang Marshall^{1

2}, Boonyisa Saelim¹, Maneerat Taweesap¹, Verachai Pachana¹, Yada Panrak¹, Naritsara Makchuchit¹, Passara Jaroenpakdee¹

Affiliations

¹ Department of Radiology, Faculty of Medicine, Prince of Songkla University, Songkhla 90110, Thailand.
² Molecular Imaging and Cyclotron Center, Division of Nuclear Medicine, Department of Radiology, Faculty of Medicine, Prince of Songkla University, Songkhla 90110, Thailand.

Abstract

The systemic delivery of doxorubicin (DOX) to treat osteosarcoma requires an adequate drug concentration to be effective, but in doing so, it raises the risk of increasing organ off-target toxicity and developing drug resistance. Herein, this study reveals a multiple therapeutic nanocarrier delivery platform that overcomes off-target toxicity by providing good specificity and imparting enhanced tumor penetration in a three-dimensional (3D) human MG-63 spheroid model. By synthesizing PEG-PLGA nanoparticles by the double emulsion method, encapsulating DOX and Na131I in the inner core, and conjugating with an epidermal growth factor receptor (EGFR) antibody, it is intended to specifically target human MG-63 cells. The nanocarrier is biocompatible with blood and has good stability characteristics. Na131I encapsulation efficiency was >96%, and radiochemical purity was >96% over 96 h. A DOX encapsulation efficacy of ~80% was achieved, with a drug loading efficiency of ~3%, and a sustained DOX release over 5 days. The nanocarrier EGFR antibody achieved a ~80-fold greater targeting efficacy to MG-63 cells (EGFR+) than fibroblast cells (EGFR−). The targeted multiple therapeutic DIE-NPs have a higher penetration and uptake of Na131I to the 3D model and a ~3-fold higher cytotoxicity than the DOX monotherapy (D-NPs). The co-administration of DOX and Na131I (DIE-NPs) disrupts DNA repair and generates free radicals resulting in DNA damage, triggering the activation of apoptosis pathways. This leads to inhibition of MG-63 cell proliferation and promotes cell cycle arrest in the G0/G1 phase. Furthermore, the PEGylated anti-EGFR functionalized DIE-NPs were found to be biocompatible with red blood cells and to have no adverse effects. This anti-EGFR targeted multifunctional I-131 radio-nanotherapeutic signifies a customizable specific targeted treatment for osteosarcoma.

Keywords: 3D spheroid; EGFR targeted therapy; I-131; cancer treatment; doxorubicin; epidermal growth factor receptor; multiple therapeutic; osteosarcoma; radiolabeled nanoparticles; targeted drug delivery.

Grants and funding

Grants for development of faculty staff, Faculty of Medicine, Prince of Songkla University.