Solvent‐cast 3D printing with molecular weight polymer blends to decouple effects of scaffold architecture and mechanical properties on mesenchymal stromal cell fate

Author:

Tolbert John W.12,French Tyler2,Kitson Andrew2,Okpara Chiebuka3,Hammerstone Diana E.2,Lazarte Santiago4,Babuska Tomas F.56,Gonzalez‐Fernandez Tomas3ORCID,Krick Brandon A.5,Chow Lesley W.123ORCID

Affiliation:

1. Polymer Science and Engineering Program Lehigh University Bethlehem Pennsylvania USA

2. Department of Materials Science and Engineering Lehigh University Bethlehem Pennsylvania USA

3. Department of Bioengineering Lehigh University Bethlehem Pennsylvania USA

4. Department of Chemical and Biomedical Engineering, FAMU‐FSU College of Engineering Florida State University Tallahassee Florida USA

5. Department of Mechanical Engineering, FAMU‐FSU College of Engineering Florida State University Tallahassee Florida USA

6. Sandia National Laboratories Albuquerque New Mexico USA

Abstract

AbstractThe biochemical and physical properties of a scaffold can be tailored to elicit specific cellular responses. However, it is challenging to decouple their individual effects on cell‐material interactions. Here, we solvent‐cast 3D printed different ratios of high and low molecular weight (MW) poly(caprolactone) (PCL) to fabricate scaffolds with significantly different stiffnesses without affecting other properties. Ink viscosity was used to match processing conditions between inks and generate scaffolds with the same surface chemistry, crystallinity, filament diameter, and architecture. Increasing the ratio of low MW PCL resulted in a significant decrease in modulus. Scaffold modulus did not affect human mesenchymal stromal cell (hMSC) differentiation under osteogenic conditions. However, hMSC response was significantly affected by scaffold stiffness in chondrogenic media. Low stiffness promoted more stable chondrogenesis whereas high stiffness drove hMSC progression toward hypertrophy. These data illustrate how this versatile platform can be used to independently modify biochemical and physical cues in a single scaffold to synergistically enhance desired cellular response.

Funder

National Science Foundation

Lehigh University

P.C. Rossin College of Engineering and Applied Science, Lehigh University

Publisher

Wiley

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