Forced protein unfolding leads to highly elastic and tough protein hydrogels

Jie Fang; Alexander Mehlich; Nobuyasu Koga; Jiqing Huang; Rie Koga; Xiaoye Gao; Chunguang Hu; Chi Jin; Matthias Rief; Juergen Kast; David Baker; Hongbin Li

doi:10.1038/ncomms3974

Forced protein unfolding leads to highly elastic and tough protein hydrogels

Jie Fang, Alexander Mehlich, Nobuyasu Koga, Jiqing Huang, Rie Koga, Xiaoye Gao, Chunguang Hu, Chi Jin, Matthias Rief, Juergen Kast, David Baker, Hongbin Li

Chair of Biophysics

Research output: Contribution to journal › Article › peer-review

154 Scopus citations

Abstract

Protein-based hydrogels usually do not exhibit high stretchability or toughness, significantly limiting the scope of their potential biomedical applications. Here we report the engineering of a chemically cross-linked, highly elastic and tough protein hydrogel using a mechanically extremely labile, de novo-designed protein that assumes the classical ferredoxin-like fold structure. Due to the low mechanical stability of the ferredoxin-like fold structure, swelling of hydrogels causes a significant fraction of the folded domains to unfold. Subsequent collapse and aggregation of unfolded ferredoxin-like domains leads to intertwining of physically and chemically cross-linked networks, entailing hydrogels with unusual physical and mechanical properties: a negative swelling ratio, high stretchability and toughness. These hydrogels can withstand an average strain of 450% before breaking and show massive energy dissipation. Upon relaxation, refolding of the ferredoxin-like domains enables the hydrogel to recover its massive hysteresis. This novel biomaterial may expand the scope of hydrogel applications in tissue engineering.

Original language	English
Article number	2974
Journal	Nature Communications
Volume	4
DOIs	https://doi.org/10.1038/ncomms3974
State	Published - 19 Dec 2013

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title = "Forced protein unfolding leads to highly elastic and tough protein hydrogels",

abstract = "Protein-based hydrogels usually do not exhibit high stretchability or toughness, significantly limiting the scope of their potential biomedical applications. Here we report the engineering of a chemically cross-linked, highly elastic and tough protein hydrogel using a mechanically extremely labile, de novo-designed protein that assumes the classical ferredoxin-like fold structure. Due to the low mechanical stability of the ferredoxin-like fold structure, swelling of hydrogels causes a significant fraction of the folded domains to unfold. Subsequent collapse and aggregation of unfolded ferredoxin-like domains leads to intertwining of physically and chemically cross-linked networks, entailing hydrogels with unusual physical and mechanical properties: a negative swelling ratio, high stretchability and toughness. These hydrogels can withstand an average strain of 450% before breaking and show massive energy dissipation. Upon relaxation, refolding of the ferredoxin-like domains enables the hydrogel to recover its massive hysteresis. This novel biomaterial may expand the scope of hydrogel applications in tissue engineering.",

author = "Jie Fang and Alexander Mehlich and Nobuyasu Koga and Jiqing Huang and Rie Koga and Xiaoye Gao and Chunguang Hu and Chi Jin and Matthias Rief and Juergen Kast and David Baker and Hongbin Li",

note = "Funding Information: We thank anonymous reviewers for their constructive suggestions and Dr. Zheng Yang for his technical assistance. This work is supported by Canadian Institutes of Health Research, Canada Research Chair program, Canada Foundation for Innovation, Michael Smith Foundation for Health Research and Natural Science Engineering Research Council of Canada. M.R. acknowledges funding through an SFB863 grant of Deutsche Forschungsgemeinschaft. H.L. is a Canada Research Chair and Michael Smith Foundation for Health Research Career Investigator. H.L. acknowledges the support of an Alexander von Humboldt fellowship.",

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AU - Mehlich, Alexander

AU - Koga, Nobuyasu

AU - Huang, Jiqing

AU - Koga, Rie

AU - Gao, Xiaoye

AU - Hu, Chunguang

AU - Jin, Chi

AU - Rief, Matthias

AU - Kast, Juergen

AU - Baker, David

AU - Li, Hongbin

N1 - Funding Information: We thank anonymous reviewers for their constructive suggestions and Dr. Zheng Yang for his technical assistance. This work is supported by Canadian Institutes of Health Research, Canada Research Chair program, Canada Foundation for Innovation, Michael Smith Foundation for Health Research and Natural Science Engineering Research Council of Canada. M.R. acknowledges funding through an SFB863 grant of Deutsche Forschungsgemeinschaft. H.L. is a Canada Research Chair and Michael Smith Foundation for Health Research Career Investigator. H.L. acknowledges the support of an Alexander von Humboldt fellowship.

PY - 2013/12/19

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N2 - Protein-based hydrogels usually do not exhibit high stretchability or toughness, significantly limiting the scope of their potential biomedical applications. Here we report the engineering of a chemically cross-linked, highly elastic and tough protein hydrogel using a mechanically extremely labile, de novo-designed protein that assumes the classical ferredoxin-like fold structure. Due to the low mechanical stability of the ferredoxin-like fold structure, swelling of hydrogels causes a significant fraction of the folded domains to unfold. Subsequent collapse and aggregation of unfolded ferredoxin-like domains leads to intertwining of physically and chemically cross-linked networks, entailing hydrogels with unusual physical and mechanical properties: a negative swelling ratio, high stretchability and toughness. These hydrogels can withstand an average strain of 450% before breaking and show massive energy dissipation. Upon relaxation, refolding of the ferredoxin-like domains enables the hydrogel to recover its massive hysteresis. This novel biomaterial may expand the scope of hydrogel applications in tissue engineering.

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Forced protein unfolding leads to highly elastic and tough protein hydrogels

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