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Adenylate Kinase Fused to Spidroin as a Catalyst for Decreasing Leakage out of 3D-Bioprinted Hydrogels and for ATP Regeneration

Authors :
Liu, Changjun
Song, Yanmin
Hu, Tianhao
Wang, Shan
Yi, Ke
Wang, Jianjie
Yan, Qing
Wei, Li’an
Zhang, Zheyang
Li, Huimin
Luo, Yutao
Wu, Lei
Zhang, Dongyi
Meng, Er
Source :
Biomacromolecules; 20230101, Issue: Preprints
Publication Year :
2023

Abstract

Numerous metabolic reactions and pathways use adenosine 5′-triphosphate (ATP) as an energy source and as a phosphorous or pyrophosphorous donor. Based on three-dimensional (3D)-printing, enzyme immobilization can be used to improve ATP regeneration and operability and reduce cost. However, due to the relatively large mesh size of 3D-bioprinted hydrogels soaked in a reaction solution, the lower-molecular-weight enzymes cannot avoid leaking out of the hydrogels readily. Here, a chimeric adenylate-kinase-spidroin (ADK-RC) is created, with ADK serving as the N-terminal domain. The chimera is capable of self-assembling to form micellar nanoparticles at a higher molecular scale. Although fused to spidroin (RC), ADK-RC remains relatively consistent and exhibits high activity, thermostability, pH stability, and organic solvent tolerance. Considering different surface-to-volume ratios, three shapes of enzyme hydrogels are designed, 3D bioprinted, and measured. In addition, a continuous enzymatic reaction demonstrates that ADK-RC hydrogels have higher specific activity and substrate affinity but a lower reaction rate and catalytic power compared to free enzymes in solution. With ATP regeneration, the ADK and ADK-RC hydrogels significantly increase the production of d-glucose-6-phosphate and obtain an efficient usage frequency. In conclusion, enzymes fused to spidroin might be an efficient strategy for maintaining activity and reducing leakage in 3D-bioprinted hydrogels under mild conditions.

Details

Language :
English
ISSN :
15257797 and 15264602
Issue :
Preprints
Database :
Supplemental Index
Journal :
Biomacromolecules
Publication Type :
Periodical
Accession number :
ejs62496317
Full Text :
https://doi.org/10.1021/acs.biomac.2c01445