Mechanism of erosion of nanostructured porous silicon drug carriers in neoplastic tissues

Author(s)

Tzur-Balter, Adi; Shatsberg, Zohar; Beckerman, Margarita; Segal, Ester; Artzi, Natalie

Abstract

Nanostructured porous ​silicon (PSi) is emerging as a promising platform for drug delivery owing to its biocompatibility, degradability and high surface area available for drug loading. The ability to control PSi structure, size and porosity enables programming its in vivo retention, providing tight control over embedded drug release kinetics. In this work, the relationship between the in vitro and in vivo degradation of PSi under (pre)clinically relevant conditions, using breast cancer mouse model, is defined. We show that PSi undergoes enhanced degradation in diseased environment compared with healthy state, owing to the upregulation of reactive oxygen species (ROS) in the tumour vicinity that oxidize the silicon scaffold and catalyse its degradation. We further show that PSi degradation in vitro and in vivo correlates in healthy and diseased states when ROS-free or ROS-containing media are used, respectively. Our work demonstrates that understanding the governing mechanisms associated with specific tissue microenvironment permits predictive material performance.

Date issued

2015-02

URI

http://hdl.handle.net/1721.1/96408

Department

Massachusetts Institute of Technology. Institute for Medical Engineering & Science

Journal

Nature Communications

Publisher

Nature Publishing Group

Citation

Tzur-Balter, Adi, Zohar Shatsberg, Margarita Beckerman, Ester Segal, and Natalie Artzi. “Mechanism of Erosion of Nanostructured Porous Silicon Drug Carriers in Neoplastic Tissues.” Nature Communications 6 (February 11, 2015): 6208.

Version: Final published version

ISSN

2041-1723