De novo design of high-affinity binders of bioactive helical peptides

被引:0
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作者
Susana Vázquez Torres
Philip J. Y. Leung
Preetham Venkatesh
Isaac D. Lutz
Fabian Hink
Huu-Hien Huynh
Jessica Becker
Andy Hsien-Wei Yeh
David Juergens
Nathaniel R. Bennett
Andrew N. Hoofnagle
Eric Huang
Michael J. MacCoss
Marc Expòsit
Gyu Rie Lee
Asim K. Bera
Alex Kang
Joshmyn De La Cruz
Paul M. Levine
Xinting Li
Mila Lamb
Stacey R. Gerben
Analisa Murray
Piper Heine
Elif Nihal Korkmaz
Jeff Nivala
Lance Stewart
Joseph L. Watson
Joseph M. Rogers
David Baker
机构
[1] University of Washington,Department of Biochemistry
[2] University of Washington,Institute for Protein Design
[3] University of Washington,Graduate Program in Biological Physics, Structure and Design
[4] University of Washington,Graduate Program in Molecular Engineering
[5] University of Washington,Department of Bioengineering
[6] University of Copenhagen,Department of Drug Design and Pharmacology
[7] University of Washington,Department of Laboratory Medicine and Pathology
[8] University of Washington,Department of Genome Sciences
[9] University of Washington,School of Computer Science and Engineering
[10] University of Washington,Molecular Engineering and Sciences Institute
[11] University of Washington,Howard Hughes Medical Institute
来源
Nature | 2024年 / 626卷
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摘要
Many peptide hormones form an α-helix on binding their receptors1–4, and sensitive methods for their detection could contribute to better clinical management of disease5. De novo protein design can now generate binders with high affinity and specificity to structured proteins6,7. However, the design of interactions between proteins and short peptides with helical propensity is an unmet challenge. Here we describe parametric generation and deep learning-based methods for designing proteins to address this challenge. We show that by extending RFdiffusion8 to enable binder design to flexible targets, and to refining input structure models by successive noising and denoising (partial diffusion), picomolar-affinity binders can be generated to helical peptide targets by either refining designs generated with other methods, or completely de novo starting from random noise distributions without any subsequent experimental optimization. The RFdiffusion designs enable the enrichment and subsequent detection of parathyroid hormone and glucagon by mass spectrometry, and the construction of bioluminescence-based protein biosensors. The ability to design binders to conformationally variable targets, and to optimize by partial diffusion both natural and designed proteins, should be broadly useful.
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页码:435 / 442
页数:7
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