PDMS Nano-Modified Scaffolds for Improvement of Stem Cells Proliferation and Differentiation in Microfluidic Platform

Hadi Hashemzadeh; Abdollah Allahverdi; Mosslim Sedghi; Zahra Vaezi; Tahereh Tohidi Moghadam; Mario Rothbauer; Michael Bernhard Fischer; Peter Ertl; Hossein Naderi-Manesh

doi:10.3390/nano10040668

PDMS Nano-Modified Scaffolds for Improvement of Stem Cells Proliferation and Differentiation in Microfluidic Platform

Nanomaterials (Basel). 2020 Apr 2;10(4):668. doi: 10.3390/nano10040668.

Authors

Hadi Hashemzadeh¹, Abdollah Allahverdi², Mosslim Sedghi², Zahra Vaezi², Tahereh Tohidi Moghadam¹, Mario Rothbauer³, Michael Bernhard Fischer⁴, Peter Ertl³, Hossein Naderi-Manesh^{1

2}

Affiliations

¹ Department of Nanobiotechnology, Faculty of Biological Science, Tarbiat Modares University, Tehran 14115-154, Iran.
² Department of Biophysics, Faculty of Biological Science, Tarbiat Modares University, Tehran 14115-154, Iran.
³ Vienna University of Technology, Faculty of Technical Chemistry, Institute of Applied Synthetic Chemistry & Institute of Chemical Technologies and Analytics, Getreidemarkt 9, 1060 Vienna, Austria.
⁴ Department of Health Science and Biomedicine, Danube University Krems, 3500 Vienna, Austria.

Abstract

Microfluidics cell-based assays require strong cell-substrate adhesion for cell viability, proliferation, and differentiation. The intrinsic properties of PDMS, a commonly used polymer in microfluidics systems, regarding cell-substrate interactions have limited its application for microfluidics cell-based assays. Various attempts by previous researchers, such as chemical modification, plasma-treatment, and protein-coating of PDMS revealed some improvements. These strategies are often reversible, time-consuming, short-lived with either cell aggregates formation, not cost-effective as well as not user- and eco-friendly too. To address these challenges, cell-surface interaction has been tuned by the modification of PDMS doped with different biocompatible nanomaterials. Gold nanowires (AuNWs), superparamagnetic iron oxide nanoparticles (SPIONs), graphene oxide sheets (GO), and graphene quantum dot (GQD) have already been coupled to PDMS as an alternative biomaterial enabling easy and straightforward integration during microfluidic fabrication. The synthesized nanoparticles were characterized by corresponding methods. Physical cues of the nanostructured substrates such as Young's modulus, surface roughness, and nanotopology have been carried out using atomic force microscopy (AFM). Initial biocompatibility assessment of the nanocomposites using human amniotic mesenchymal stem cells (hAMSCs) showed comparable cell viabilities among all nanostructured PDMS composites. Finally, osteogenic stem cell differentiation demonstrated an improved differentiation rate inside microfluidic devices. The results revealed that the presence of nanomaterials affected a 5- to 10-fold increase in surface roughness. In addition, the results showed enhancement of cell proliferation from 30% (pristine PDMS) to 85% (nano-modified scaffolds containing AuNWs and SPIONs), calcification from 60% (pristine PDMS) to 95% (PDMS/AuNWs), and cell surface marker expression from 40% in PDMS to 77% in SPION- and AuNWs-PDMS scaffolds at 14 day. Our results suggest that nanostructured composites have a very high potential for stem cell studies and future therapies.

Keywords: PDMS functionalization; microfluidics material; nano biointerface; nanomaterials; nanoparticle-polymer composites; nanotopography; osteogenic differentiation; stem cells.