Design of novel cyanovirin-N variants by modulation of binding dynamics through distal mutations

Author:

Kazan I Can12ORCID,Sharma Prerna2,Rahman Mohammad Imtiazur2,Bobkov Andrey3,Fromme Raimund2,Ghirlanda Giovanna2ORCID,Ozkan S Banu1ORCID

Affiliation:

1. Center for Biological Physics and Department of Physics, Arizona State University

2. School of Molecular Sciences, Arizona State University

3. Sanford Burnham Prebys Medical Discovery Institute

Abstract

We develop integrated co-evolution and dynamic coupling (ICDC) approach to identify, mutate, and assess distal sites to modulate function. We validate the approach first by analyzing the existing mutational fitness data of TEM-1 β-lactamase and show that allosteric positions co-evolved and dynamically coupled with the active site significantly modulate function. We further apply ICDC approach to identify positions and their mutations that can modulate binding affinity in a lectin, cyanovirin-N (CV-N), that selectively binds to dimannose, and predict binding energies of its variants through Adaptive BP-Dock. Computational and experimental analyses reveal that binding enhancing mutants identified by ICDC impact the dynamics of the binding pocket, and show that rigidification of the binding residues compensates for the entropic cost of binding. This work suggests a mechanism by which distal mutations modulate function through dynamic allostery and provides a blueprint to identify candidates for mutagenesis in order to optimize protein function.

Funder

National Science Foundation

Gordon and Betty Moore Foundation

National Institutes of Health

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

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