Multiscale computation delivers organophosphorus reactivity and stereoselectivity to immunoglobulin scavengers

Author:

Mokrushina Yuliana A.ORCID,Golovin Andrey V.,Smirnov Ivan V.ORCID,Chatziefthimiou Spyros D.ORCID,Stepanova Anastasia V.ORCID,Bobik Tatyana V.,Zalevsky Arthur O.ORCID,Zlobin Alexander S.ORCID,Konovalov Kirill A.ORCID,Terekhov Stanislav S.,Stepanov Alexey V.ORCID,Pipiya Sofiya O.ORCID,Shamborant Olga G.ORCID,Round Ekaterina,Belogurov Alexey A.ORCID,Bourenkov GlebORCID,Makarov Alexander A.,Wilmanns MatthiasORCID,Xie Jia,Blackburn G. Michael,Gabibov Alexander G.,Lerner Richard A.ORCID

Abstract

Quantum mechanics/molecular mechanics (QM/MM) maturation of an immunoglobulin (Ig) powered by supercomputation delivers novel functionality to this catalytic template and facilitates artificial evolution of biocatalysts. We here employ density functional theory-based (DFT-b) tight binding and funnel metadynamics to advance our earlier QM/MM maturation of A17 Ig-paraoxonase (WTIgP) as a reactibody for organophosphorus toxins. It enables regulation of biocatalytic activity for tyrosine nucleophilic attack on phosphorus. The single amino acid substitution l-Leu47Lys results in 340-fold enhanced reactivity for paraoxon. The computed ground-state complex shows substrate-induced ionization of the nucleophilic l-Tyr37, now H-bonded to l-Lys47, resulting from repositioning of l-Lys47. Multiple antibody structural homologs, selected by phenylphosphonate covalent capture, show contrasting enantioselectivities for a P-chiral phenylphosphonate toxin. That is defined by crystallographic analysis of phenylphosphonylated reaction products for antibodies A5 and WTIgP. DFT-b analysis using QM regions based on these structures identifies transition states for the favored and disfavored reactions with surprising results. This stereoselection analysis is extended by funnel metadynamics to a range of WTIgP variants whose predicted stereoselectivity is endorsed by experimental analysis. The algorithms used here offer prospects for tailored design of highly evolved, genetically encoded organophosphorus scavengers and for broader functionalities of members of the Ig superfamily, including cell surface-exposed receptors.

Funder

Russian Foundation for Basic Research

Russian Science Foundation

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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