An in Vivo Platform to Select and Evolve Aggregation-resistant Proteins

Overview

Journal Nat Commun

Specialty Biology

Date 2020 Apr 15

PMID 32286330

Citations 18

Authors

Jessica S Ebo

Janet C Saunders

Paul W A Devine

Alice M Gordon

Amy S Warwick

Bob Schiffrin

Stacey E Chin

Elizabeth England

James D Button

Christopher Lloyd

Nicholas J Bond

Alison E Ashcroft

Sheena E Radford

David C Lowe

David J Brockwell

Affiliations

Soon will be listed here.

Abstract

Protein biopharmaceuticals are highly successful, but their utility is compromised by their propensity to aggregate during manufacture and storage. As aggregation can be triggered by non-native states, whose population is not necessarily related to thermodynamic stability, prediction of poorly-behaving biologics is difficult, and searching for sequences with desired properties is labour-intensive and time-consuming. Here we show that an assay in the periplasm of E. coli linking aggregation directly to antibiotic resistance acts as a sensor for the innate (un-accelerated) aggregation of antibody fragments. Using this assay as a directed evolution screen, we demonstrate the generation of aggregation resistant scFv sequences when reformatted as IgGs. This powerful tool can thus screen and evolve 'manufacturable' biopharmaceuticals early in industrial development. By comparing the mutational profiles of three different immunoglobulin scaffolds, we show the applicability of this method to investigate protein aggregation mechanisms important to both industrial manufacture and amyloid disease.

Citing Articles

AggNet: Advancing protein aggregation analysis through deep learning and protein language model.

He W, Xu X, Li H, Zhou J, Gao X Protein Sci. 2025; 34(2):e70031.

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Biophysical Analysis of Therapeutic Antibodies in the Early Development Pipeline.

Willis L, Kapur N, Radford S, Brockwell D Biologics. 2024; 18:413-432.

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Rationalizing mAb Candidate Screening Using a Single Holistic Developability Parameter.

Willis L, Trayton I, Saunders J, Bruque M, Davis Birch W, Westhead D Mol Pharm. 2024; 22(1):181-195.

PMID: 39681988 PMC: 11707744. DOI: 10.1021/acs.molpharmaceut.4c00829.

Enzymatically catalyzed molecular aggregation.

Wang W, Zhang R, Zhang L, Hao L, Cai X, Wu Q Nat Commun. 2024; 15(1):9999.

PMID: 39557870 PMC: 11574095. DOI: 10.1038/s41467-024-54291-1.

Aggrescan4D: A comprehensive tool for pH-dependent analysis and engineering of protein aggregation propensity.

Zalewski M, Iglesias V, Barcenas O, Ventura S, Kmiecik S Protein Sci. 2024; 33(10):e5180.

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