| Literature DB >> 32757263 |
Julia Hauptstein1, Thomas Böck2, Michael Bartolf-Kopp2, Leonard Forster2, Philipp Stahlhut2, Ali Nadernezhad2, Gina Blahetek3, Alma Zernecke-Madsen3, Rainer Detsch4, Tomasz Jüngst2, Jürgen Groll2, Jörg Teßmar2, Torsten Blunk1.
Abstract
In 3D bioprinting, bioinks with high concentrations of polymeric materials are frequently used to enable fabrication of 3D cell-hydrogel constructs with sufficient stability. However, this is often associated with restricted cell bioactivity and an inhomogeneous distribution of newly produced extracellular matrix (ECM). Therefore, this study investigates bioink compositions based on hyaluronic acid (HA), an attractive material for cartilage regeneration, which allow for reduction of polymer content. Thiolated HA and allyl-modified poly(glycidol) in varying concentrations are UV-crosslinked. To adapt bioinks to poly(ε-caprolactone) (PCL)-supported 3D bioprinting, the gels are further supplemented with 1 wt% unmodified high molecular weight HA (hmHA) and chondrogenic differentiation of incorporated human mesenchymal stromal cells is assessed. Strikingly, addition of hmHA to gels with a low polymer content (3 wt%) results in distinct increase of construct quality with a homogeneous ECM distribution throughout the constructs, independent of the printing process. Improved ECM distribution in those constructs is associated with increased construct stiffness after chondrogenic differentiation, as compared to higher concentrated constructs (10 wt%), which only show pericellular matrix deposition. The study contributes to effective bioink development, demonstrating dual function of a supplement enabling PCL-supported bioprinting and at the same time improving biological properties of the resulting constructs.Entities:
Keywords: biofabrication; bioinks; chondrogenic differentiation; extracellular matrix; hyaluronic acid
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Year: 2020 PMID: 32757263 DOI: 10.1002/adhm.202000737
Source DB: PubMed Journal: Adv Healthc Mater ISSN: 2192-2640 Impact factor: 9.933