Choice of fusion proteins, expression host, and analytics solves difficult‐to‐produce protein challenges in discovery research

Author:

Lyons‐Abbott Sally1,Abramov Ariel1,Chan Chung‐leung1,Deer Jen Running1,Fu Guangsen1,Hassouneh Wafa1,Koch Tyree1,Misquith Ayesha1,O'Neill Jason1,Simon Sandy Alexander1,Wolf Anitra1,Yeh Ronald1,Vernet Erik1ORCID

Affiliation:

1. Novo Nordisk Research Center Seattle, Inc Seattle Washington USA

Abstract

AbstractHigh quality biological reagents are a prerequisite for pharmacological research. Herein a protein production screening approach, including quality assessment methods, for protein‐based discovery research is presented. Trends from 2895 expression constructs representing 253 proteins screened in mammalian and bacterial hosts—91% of which are successfully expressed and purified—are discussed. Mammalian expression combined with the use of solubility‐promoting fusion proteins is deemed suitable for most targets. Furthermore, cases utilizing stable cell line generation and choice of fusion protein for higher yield and quality of difficult‐to‐produce proteins (Leucine‐rich repeat‐containing G‐protein coupled receptor 4 (LGR4) and Neurturin) are presented and discussed. In the case of Neurturin, choice of fusion protein impacted the target binding 80‐fold. These results highlight the need for exploration of construct designs and careful Quality Control (QC) of difficult‐to‐produce protein reagents.

Funder

Novo Nordisk

Publisher

Wiley

Subject

Molecular Medicine,Applied Microbiology and Biotechnology,General Medicine

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