Published August 6, 2025 | Version v1
Journal article Open

PANCS-Binders: A rapid, high-throughput binder discovery platform

Description

Proteins that selectively bind to a target of interest are foundational in research, diagnostics and therapeutics. Current approaches for discovering binders are laborious and time-consuming, taking months or more, and have a high failure rate. Here we establish phage-assisted noncontinuous selection of protein binders (PANCS-Binders), an in vivo selection platform that links the life cycle of M13 phage to target protein binding through proximity-dependent split RNA polymerase biosensors, allowing for comprehensive screening of whether a variant binds a target with high fidelity. We showcase PANCS-Binders by screening multiple protein libraries each against a panel of 95 separate targets, thereby individually assessing more than 1011 protein–protein interaction pairs, in 2 days. These selections yielded large, high-quality datasets and hundreds of novel binders, which can be affinity matured or directly used in mammalian cells to inhibit or degrade targets. We believe that PANCS-Binders accelerates and simplifies the binder discovery process, which will help unlock new creative potential in proteome targeting with engineered binder-based biotechnologies.

Data availability

Links to electronic vector maps are included in Supplementary Information. All physical vectors will be made available on reasonable request. Source data are provided with this paper.

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Additional details

Identifiers

DOI
10.1038/s41592-025-02740-0
Other
oai:uchicago.tind.io:15965

Funding

National Institute of General Medical Sciences
GM119840
National Institute of General Medical Sciences
F32GM147968
National Cancer Institute
P30CA014599
Camille and Henry Dreyfus Foundation
Teacher Scholar Award

UChicago Information

Division(s)
Physical Sciences Division
Department(s)
Chemistry