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An optimized thermodynamics integration protocol for identifying beneficial mutations in antibody design

by Sheng, Zizhang , Guo, Yicheng , Ho, David D. , Bimela, Jude S. , Wang, Maple , Li, Zhiteng

in Accuracy / Affinity / Algorithms / Antibodies / antibody 10-40 / antibody design / Antigens / Broadly Neutralizing Antibodies / Coronaviruses / COVID-19 - genetics / COVID-19 vaccines / Energy / Free energy / Humans / Hydrophobicity / Immunology / Mean square errors / Molecular dynamics / molecular dynamics simulation / Mutagenesis / Mutation / Performance evaluation / Proteins / SARS-CoV-2 / SARS-CoV-2 - genetics / Severe acute respiratory syndrome coronavirus 2 / Simulation / Thermodynamics / thermodynamics integration

2023

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An optimized thermodynamics integration protocol for identifying beneficial mutations in antibody design

by Sheng, Zizhang , Guo, Yicheng , Ho, David D. , Bimela, Jude S. , Wang, Maple , Li, Zhiteng

2023

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An optimized thermodynamics integration protocol for identifying beneficial mutations in antibody design

by Sheng, Zizhang , Guo, Yicheng , Ho, David D. , Bimela, Jude S. , Wang, Maple , Li, Zhiteng

2023

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Journal Article

An optimized thermodynamics integration protocol for identifying beneficial mutations in antibody design

Sheng, Zizhang,

Guo, Yicheng,

Ho, David D.,

Bimela, Jude S.,

Wang, Maple,

Li, Zhiteng

2023

Overview

Accurate identification of beneficial mutations is central to antibody design. Many knowledge-based (KB) computational approaches have been developed to predict beneficial mutations, but their accuracy leaves room for improvement. Thermodynamic integration (TI) is an alchemical free energy algorithm that offers an alternative technique for identifying beneficial mutations, but its performance has not been evaluated. In this study, we developed an efficient TI protocol with high accuracy for predicting binding free energy changes of antibody mutations. The improved TI method outperforms KB methods at identifying both beneficial and deleterious mutations. We observed that KB methods have higher accuracies in predicting deleterious mutations than beneficial mutations. A pipeline using KB methods to efficiently exclude deleterious mutations and TI to accurately identify beneficial mutations was developed for high-throughput mutation scanning. The pipeline was applied to optimize the binding affinity of a broadly sarbecovirus neutralizing antibody 10-40 against the circulating severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) omicron variant. Three identified beneficial mutations show strong synergy and improve both binding affinity and neutralization potency of antibody 10-40. Molecular dynamics simulation revealed that the three mutations improve the binding affinity of antibody 10-40 through the stabilization of an altered binding mode with increased polar and hydrophobic interactions. Above all, this study presents an accurate and efficient TI-based approach for optimizing antibodies and other biomolecules.

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Frontiers Media SA,Frontiers Media S.A

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