Unlocking the potential of bio-inspired bioinks: A collective breakthrough in mammalian tissue bioprinting
Author:
Marquette Christophe A.1, Chastagnier Laura1, Sousa Benjamin Da1, Chocarro-Wrona Carlos1, Courtial Edwin-Joffrey1, Rae Elea1, Thomann Céline1, Carre Albane1, Essayan Lucie1, Pasuch Ana J.1, Mosnier Alizée1, Devillard Chloé1, Petiot Emma1, Lemarié Lucas2, Matera Eva-Laure3, Simoes Meigge3, Dumontet Charles3, Martin Cristina Cuella4, Pechtimaldjian Léa4, Pécheur Eve-Isabelle4, Maguer-Satta Véronique4, Michelet Maude5, Plissonnier Marie-Laure5, Archer Fabienne6, Moreau Karen7, Dufaud Marjorie8, Zaupa Cécile9, Balloul Jean-Marc9, Pruvost Quentin10, Dauphin Thibaud10, Mosser Mathilde10, Pragnère Sarah11
Affiliation:
1. 3d.FAB - Université Lyon1 2. SEGULA technologies 3. Oncopharmacologie, Centre de Recherche en Cancérologie de Lyon (CRCL) 4. CITI, Centre de Recherche en Cancérologie de Lyon (CRCL) 5. Hepatitis Viruses and Pathobiology of Chronic Liver Disease, Centre de Recherche en Cancérologie de Lyon (CRCL) 6. IVPC UMR754, INRAE, Universite Claude Bernard Lyon 1 7. CIRI, Centre International de Recherche en Infectiologie, Inserm U1111, Universite Claude Bernard Lyon 1 8. IRMB 9. Transgene 10. ONIRIS VetAgroBio Nantes, INRAE 11. Laboratory of Tribology and System Dynamics UMR-CNRS 5513, Ecole Centrale de Lyon
Abstract
Abstract
The composition of soft tissues in mammals can be simplified as approximately 60–65% water, 16% protein, 16% fat, 1% carbohydrate, and trillions of cells. This report brings together the collaborative efforts of 10 research groups over the past five years, all dedicated to producing mammalian tissues through extrusion-based bioprinting. What unified these studies was a common approach, with a shared bioink composition consisting of gelatin, alginate, and fibrinogen, and a post-printing consolidation strategy involving transglutaminase crosslinking, calcium chelation, and thrombin-mediated fibrin production. By consolidating the findings of these studies, it was conclusively demonstrated that bioprinting and culturing all 19 cells tested from 14 different organs was indeed achievable. These remarkable outcomes were attributed not only to the bio-inspired nature of the common bioink but also to its unique rheological properties, such as significant shear-thinning and a sufficiently high static yield stress. The majority of these cells exhibited behaviours consistent with their natural in vivo environments. Clearly identifiable microstructures and organizations showcased intricate morphogenesis mechanisms resulting in the formation of micro-tubules, micro-vessels, and micro-acini. It is now evident that microextrusion bioprinting, especially when using bio-inspired bioink formulations, represents a promising avenue for generating a wide range of mammalian soft tissues.
Publisher
Springer Science and Business Media LLC
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