Issue 15, 2017

Assessing chemotherapeutic effectiveness using a paper-based tumor model

Abstract

In vitro models for screening new cancer chemotherapeutics often rely on two-dimensional cultures to predict therapeutic potential. Unfortunately, the predictive power of these models is limited, as they fail to recapitulate the complex three-dimensional environments in tumors that promote a chemoresistant phenotype. In this study, we describe the preparation and characterization of paper-based cultures (PBCs) engineered to assess chemotherapeutic effectiveness in three dimensional, diffusion-limited environments. Similar environments are found in poorly vascularized tumors. Monotonic gradients develop across these cultures, which are assembled by stacking cell-laden paper scaffolds to yield thick tissue-like structures, and provide distinct chemical environments for each scaffold. After prolonged incubation, the scaffolds can simply be peeled apart and analyzed. Through fluorescence imaging, we determined that viable and proliferative cell populations were most abundant in scaffolds close to the nutrient-rich medium. By adjusting the cell density, we modulated the spatiotemporal evolution of oxygen gradients across the cultures and correlated these environmental changes with cellular sensitivity to SN-38 exposure. From these results, we showed that differences in the oxygen gradients produced cellular populations with significantly different chemosensitivities. Through this work, we highlight PBCs ability to serve as an analytical model capable of determining chemotherapeutic effectiveness under a range of chemical environments.

Graphical abstract: Assessing chemotherapeutic effectiveness using a paper-based tumor model

Supplementary files

Article information

Article type
Paper
Submitted
15 May 2017
Accepted
05 Jul 2017
First published
06 Jul 2017

Analyst, 2017,142, 2819-2827

Assessing chemotherapeutic effectiveness using a paper-based tumor model

M. W. Boyce, G. J. LaBonia, A. B. Hummon and M. R. Lockett, Analyst, 2017, 142, 2819 DOI: 10.1039/C7AN00806F

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