Rapid biosensor development using plant hormone receptors as reprogrammable scaffolds

被引:0
|
作者
Jesús Beltrán
Paul J. Steiner
Matthew Bedewitz
Shuang Wei
Francis C. Peterson
Zongbo Li
Brigid E. Hughes
Zachary Hartley
Nicholas R. Robertson
Angélica V. Medina-Cucurella
Zachary T. Baumer
Alison C. Leonard
Sang-Youl Park
Brian F. Volkman
Dmitri A. Nusinow
Wenwan Zhong
Ian Wheeldon
Sean R. Cutler
Timothy A. Whitehead
机构
[1] University of California,Department of Botany and Plant Sciences
[2] Riverside,Institute for Integrative Genome Biology
[3] University of California,Department of Chemical and Biological Engineering
[4] Riverside,Department of Biochemistry
[5] University of Colorado Boulder,Department of Biochemistry
[6] University of California,Department of Chemistry
[7] Riverside,Department of Bioengineering
[8] Medical College of Wisconsin,Department of Chemical Engineering and Materials Science
[9] University of California,Department of Chemical and Environmental Engineering
[10] Riverside,Center for Plant Cell Biology
[11] University of California,undefined
[12] Riverside,undefined
[13] Michigan State University,undefined
[14] Donald Danforth Plant Science Center,undefined
[15] University of California,undefined
[16] Riverside,undefined
[17] University of California,undefined
[18] Riverside,undefined
来源
Nature Biotechnology | 2022年 / 40卷
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摘要
A general method to generate biosensors for user-defined molecules could provide detection tools for a wide range of biological applications. Here, we describe an approach for the rapid engineering of biosensors using PYR1 (Pyrabactin Resistance 1), a plant abscisic acid (ABA) receptor with a malleable ligand-binding pocket and a requirement for ligand-induced heterodimerization, which facilitates the construction of sense–response functions. We applied this platform to evolve 21 sensors with nanomolar to micromolar sensitivities for a range of small molecules, including structurally diverse natural and synthetic cannabinoids and several organophosphates. X-ray crystallography analysis revealed the mechanistic basis for new ligand recognition by an evolved cannabinoid receptor. We demonstrate that PYR1-derived receptors are readily ported to various ligand-responsive outputs, including enzyme-linked immunosorbent assay (ELISA)-like assays, luminescence by protein-fragment complementation and transcriptional circuits, all with picomolar to nanomolar sensitivity. PYR1 provides a scaffold for rapidly evolving new biosensors for diverse sense–response applications.
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页码:1855 / 1861
页数:6
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