4.8 Article

Hydrogel Bioink with Multilayered Interfaces Improves Dispersibility of Encapsulated Cells in Extrusion Bioprinting

Journal

ACS APPLIED MATERIALS & INTERFACES
Volume 11, Issue 34, Pages 30585-30595

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acsami.9b09782

Keywords

3D bioprinting; bioink; interfacial retention; gelatin methacrylate; cell sedimentation

Funding

  1. National Key R&D Program of China [2018YFC1005002]
  2. National Natural Science Foundation of China [81772007, 81771971, 21734003, 81570422]
  3. Science and Technology Commission of Shanghai Municipality [17JC1400200, 18490740500]
  4. Shanghai Pujiang Program [17PJ1401500]
  5. Shanghai Municipal Education Commission [2017-01-07-00-07-E00027]
  6. Fudan University Human Phenome Institute Research Program

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One of the challenges for extrusion bioprinting using low-viscosity bioinks is the fast gravity-driven sedimentation of cells. Cells in a hydrogel bioink that features low viscosity tend to settle to the bottom of the bioink reservoir, and as such, their bioprintability is hindered by association with the inhomogeneous cellularized structures that are deposited. This is particularly true in cases where longer periods are required to print complex or larger tissue constructs. Increasing the bioink's viscosity efficiently retards sedimentation but gives rise to cell membranolysis or functional disruption due to increased shear stress on the cells during the extrusion process. Inspired by the rainbow cocktail, we report the development of a multilayered modification strategy for gelatin methacryloyl (GelMA) bioink to manipulate multiple liquid interfaces, providing interfacial retention to retard cell sedimentation in the bioink reservoir. Indeed, the interfacial tension in our layer-by-layer bioink system, characterized by the pendant drop method, was found to be exponentially higher than the sedimental pull (Delta(Gravity-Buoyancy) = similar to 10(-9) N) of cells, indicating that the interfacial retention is crucial for preventing cell sedimentation across the adjacent layers. It was demonstrated that the encapsulated cells displayed better dispersibility in constructs bioprinted using the multilayered GelMA bioink system than that of pristine GelMA where the index of homogeneity of the cell distribution in the multilayered bioink was 4 times that of the latter.

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