Improving folding properties of computationally designed proteins

Author:

Bjerre Benjamin1,Nissen Jakob1,Madsen Mikkel1,Fahrig-Kamarauskaitė Jūratė1,Norrild Rasmus K1,Holm Peter C1,Nordentoft Mathilde K1,O’Shea Charlotte1,Willemoës Martin1,Johansson Kristoffer E1,Winther Jakob R1

Affiliation:

1. The Linderstrøm-Lang Centre for Protein Science, Section for Biomolecular Sciences, Department of Biology, University for Copenhagen, Ole Maaloes Vej 5, DK-2200 Copenhagen N, Denmark

Abstract

Abstract While the field of computational protein design has witnessed amazing progression in recent years, folding properties still constitute a significant barrier towards designing new and larger proteins. In order to assess and improve folding properties of designed proteins, we have developed a genetics-based folding assay and selection system based on the essential enzyme, orotate phosphoribosyl transferase from Escherichia coli. This system allows for both screening of candidate designs with good folding properties and genetic selection of improved designs. Thus, we identified single amino acid substitutions in two failed designs that rescued poorly folding and unstable proteins. Furthermore, when these substitutions were transferred into a well-structured design featuring a complex folding profile, the resulting protein exhibited native-like cooperative folding with significantly improved stability. In protein design, a single amino acid can make the difference between folding and misfolding, and this approach provides a useful new platform to identify and improve candidate designs.

Funder

Novo-Nordisk Foundation and the Independent Research Fund Denmark

Publisher

Oxford University Press (OUP)

Subject

Molecular Biology,Biochemistry,Bioengineering,Biotechnology

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