What does this research mean for the field?

Gelatin methacrylate/gellan gum hydrogels can be optimized to balance mechanical strength and cell viability for soft tissue engineering applications in the central nervous system. Novelty: ClaimNovelty.INCREMENTAL. Consensus alignment: ConsensusAlignment.NEUTRAL.

What question did this study set out to answer?

This research aims to develop bioink for soft tissue engineering by optimizing gelatin methacrylate and gellan gum formulations.

March 5, 2026Open Access

Balancing Strength and Cell Viability in Gelatin Methacrylate/Gellan Gum Bioink Formulations

Key Points

This research aims to develop bioink for soft tissue engineering by optimizing gelatin methacrylate and gellan gum formulations.
Developed bioink formulations combining gelatin methacrylate and gellan gum.
Characterized rheological and mechanical properties through compression testing.
Conducted biodegradation and cell viability assays, including live/dead fluorescence microscopy.
Tested multiple concentrations of gelatin and gellan gum to evaluate their effects.
Bioinks achieved over 98% cell viability after one day of culture.
Increasing gellan gum concentration enhances stiffness and Young's modulus for both gelatin formulations.
Higher gellan gum content decreased biodegradation and cell viability after 14 days of culture.
Certain formulations maintained above 85% cell viability over extended culture periods.

Abstract

Soft tissue injuries resulting from trauma or degeneration are challenging to treat due to limited regenerative capacity, particularly in complex tissues, such as the central nervous system (CNS), nerves, and cartilage, where biomechanical and biochemical factors hinder effective repair. In these cases, tissue engineering presents a promising approach by combining biomaterials, cells, and bioactive signals to enhance soft tissue regeneration; however, its success relies on the compatibility between implanted materials and native tissue. Among the advances in this field, 3D bioprinting enables precise spatial control of the scaffold architecture and cell positioning, making it well-suited for developing constructs that mimic native tissue. In this study, we developed and characterized a series of bioink formulations based on a dual network system of gelatin methacrylate (GelMA) combined with gellan gum (GG). The GelMA/GG hydrogels were evaluated using rheological and compression testing as well as biodegradation and cell viability assays, including live/dead fluorescence microscopy. Formulations containing two different concentrations of GelMA (2.5 and 4.0% w/w) and GG (0.25 and 0.50% w/w) were tested, and the rheological results showed a strong dependence of the elastic component (G′) on GG concentration. For the 2.5% GelMA formulations, increasing the GG content significantly enhanced the Young’s modulus. In 4.0% GelMA formulations, stiffness increased as the GG concentration rose. Higher GG content decreased biodegradation over 14 days in phosphate-buffered saline and reduced cell viability due to the hydrogel’s increased stiffness. The bioinks demonstrated suitable rheological properties for bioprinting, achieving over 98% cell viability after 1 day. Additionally, formulations such as 4.0% GelMA with 0.25% GG and 2.5% GelMA with 0.5% GG exhibited high cell viability (above 85%) when maintained even after longer culture periods, such as 14 days. These results indicate that GelMA/GG hydrogels have great potential as versatile, tunable bioinks for soft-tissue engineering in the CNS. Future research will focus on modifying the hydrogel network’s rigidity to enhance cell viability further and refine its application in bioprinting strategies for regenerating soft tissues in the central nervous system.

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Cite This Study

Backes et al. (Tue,) studied this question.

synapsesocial.com/papers/69a91e2cd6127c7a504c1e33 https://doi.org/https://doi.org/10.1021/acsomega.5c09665

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