Bottom-up de novo design of functional proteins with complex structural features

被引:0
|
作者
Che Yang
Fabian Sesterhenn
Jaume Bonet
Eva A. van Aalen
Leo Scheller
Luciano A. Abriata
Johannes T. Cramer
Xiaolin Wen
Stéphane Rosset
Sandrine Georgeon
Theodore Jardetzky
Thomas Krey
Martin Fussenegger
Maarten Merkx
Bruno E. Correia
机构
[1] École Polytechnique Fédérale de Lausanne (EPFL),Institute of Bioengineering
[2] Swiss Institute of Bioinformatics,Laboratory of Chemical Biology and Institute for Complex Molecular Systems, Department of Biomedical Engineering
[3] Eindhoven University of Technology,Department of Biosystems Science and Engineering
[4] ETH Zurich,Institute of Virology
[5] Hannover Medical School,Department of Structural Biology
[6] Stanford University School of Medicine,undefined
[7] German Center for Infection Research (DZIF),undefined
来源
Nature Chemical Biology | 2021年 / 17卷
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摘要
De novo protein design has enabled the creation of new protein structures. However, the design of functional proteins has proved challenging, in part due to the difficulty of transplanting structurally complex functional sites to available protein structures. Here, we used a bottom-up approach to build de novo proteins tailored to accommodate structurally complex functional motifs. We applied the bottom-up strategy to successfully design five folds for four distinct binding motifs, including a bifunctionalized protein with two motifs. Crystal structures confirmed the atomic-level accuracy of the computational designs. These de novo proteins were functional as components of biosensors to monitor antibody responses and as orthogonal ligands to modulate synthetic signaling receptors in engineered mammalian cells. Our work demonstrates the potential of bottom-up approaches to accommodate complex structural motifs, which will be essential to endow de novo proteins with elaborate biochemical functions, such as molecular recognition or catalysis.
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页码:492 / 500
页数:8
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