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  5. Low-N Protein Activity Optimization with FolDE.

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Article
en
2025

Low-N Protein Activity Optimization with FolDE.

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en
2025
pubmed.ncbi.nlm.nih.gov/41281216

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Jay D Keasling
Jay D Keasling

University of California, Berkeley

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Jacob B. Roberts
Chunpeng Ji
Isaac Donnell
+13 more

Abstract

Proteins are traditionally optimized through the costly construction and measurement of many mutants. Active Learning-assisted Directed Evolution (ALDE) alleviates that cost by predicting the best improvements and iteratively testing mutants to inform predictions. However, existing ALDE methods face a critical limitation: selecting the highest-predicted mutants in each round yields homogeneous training data insufficient for accurate prediction models in subsequent rounds. Here we present FolDE, an ALDE method designed to maximize end-of-campaign success. In simulations across 20 protein targets, FolDE discovers 23% more top 10% mutants than the best baseline method (p=0.005) and is 55% more likely to find top 1% mutants. FolDE achieves this primarily through naturalness-based warm-starting, which augments limited activity measurements with protein language model outputs to improve activity prediction. We also introduce a constant-liar batch selector, which improves batch diversity; this is important in multi-mutation campaigns but had limited effect in our benchmarks. The complete workflow is freely available as open-source software, making efficient protein optimization accessible to any laboratory.

How to cite this publication

Jacob B. Roberts, Chunpeng Ji, Isaac Donnell, Thomas D. Young, Allison N. Pearson, Graham A. Hudson, Leah S. Keiser, Mia Wesselkamper, Peter H. Winegar, JA Ludwig, Sarah H. Klass, Isha V Sheth, Ezechinyere C Ukabiala, M. Astolfi, Benjamin Eysenbach, Jay D Keasling (2025). Low-N Protein Activity Optimization with FolDE..

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Publication Details

Type

Article

Year

2025

Authors

16

Datasets

0

Total Files

0

Language

en

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