Imaging Diffusion and Stability of Single‐Chain Polymeric Nanoparticles in a Multi‐Gel Tumor‐on‐a‐Chip Microfluidic Device

Author:

Deng Linlin12ORCID,Olea Alis R.3,Ortiz‐Perez Ana24ORCID,Sun Bingbing25ORCID,Wang Jianhong25,Pujals Silvia6ORCID,Palmans Anja R. A.12ORCID,Albertazzi Lorenzo24ORCID

Affiliation:

1. Laboratory for Macromolecular and Organic Chemistry Department of Chemical Engineering and Chemistry Eindhoven University of Technology P.O. Box 513 Eindhoven 5600 MB The Netherlands

2. Institute for Complex Molecular Systems Eindhoven University of Technology P.O. Box 513 Eindhoven 5600 MB The Netherlands

3. Institute for Bioengineering of Catalonia (IBEC) The Barcelona Institute of Science and Technology Baldiri Reixac 15–21 Barcelona 08028 Spain

4. Molecular Biosensing for Medical Diagnostics Department of Biomedical Engineering Eindhoven University of Technology P.O. Box 513 Eindhoven 5600 MB The Netherlands

5. Bio‐Organic Chemistry Department of Chemical Engineering and Chemistry Eindhoven University of Technology P.O. Box 513 Eindhoven 5600 MB The Netherlands

6. Institute for Advanced Chemistry of Catalonia (IQAC) Barcelona 08034 Spain

Abstract

AbstractThe performance of single‐chain polymeric nanoparticles (SCPNs) in biomedical applications highly depends on their conformational stability in cellular environments. Until now, such stability studies are limited to 2D cell culture models, which do not recapitulate the 3D tumor microenvironment well. Here, a microfluidic tumor‐on‐a‐chip model is introduced that recreates the tumor milieu and allows in‐depth insights into the diffusion, cellular uptake, and stability of SCPNs. The chip contains Matrigel/collagen‐hyaluronic acid as extracellular matrix (ECM) models and is seeded with cancer cell MCF7 spheroids. With this 3D platform, it is assessed how the polymer's microstructure affects the SCPN's behavior when crossing the ECM, and evaluates SCPN internalization in 3D cancer cells. A library of SCPNs varying in microstructure is prepared. All SCPNs show efficient ECM penetration but their cellular uptake/stability behavior depends on the microstructure. Glucose‐based nanoparticles display the highest spheroid uptake, followed by charged nanoparticles. Charged nanoparticles possess an open conformation while nanoparticles stabilized by internal hydrogen bonding retain a folded structure inside the tumor spheroids. The 3D microfluidic tumor‐on‐a‐chip platform is an efficient tool to elucidate the interplay between polymer microstructure and SCPN's stability, a key factor for the rational design of nanoparticles for targeted biological applications.

Funder

H2020 Marie Skłodowska-Curie Actions

Publisher

Wiley

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