Multiscale analysis of enantioselectivity in enzyme-catalysed ‘lethal synthesis’ using projector-based embedding

Author:

Zhang Xinglong1ORCID,Bennie Simon J.2,van der Kamp Marc W.23,Glowacki David R.24ORCID,Manby Frederick R.2,Mulholland Adrian J.2

Affiliation:

1. Physical and Theoretical Chemistry Laboratory, University of Oxford, South Parks Road, Oxford OX1 3QZ, UK

2. Centre for Computational Chemistry, School of Chemistry, University of Bristol, Bristol BS8 1TS, UK

3. School of Biochemistry, University of Bristol, Bristol BS8 1TD, UK

4. Department of Computer Science, Merchant Venturers Building, Woodland Road, Bristol BS8 1UB, UK

Abstract

The action of fluoroacetate as a broad-spectrum mammalian pesticide depends on the ‘lethal synthesis’ of fluorocitrate by citrate synthase, through a subtle enantioselective enolization of fluoroacetyl-coenzyme A. In this work, we demonstrate how a projection-based embedding method can be applied to calculate coupled cluster (CCSD(T)) reaction profiles from quantum mechanics/molecular mechanics optimized pathways for this enzyme reaction. Comparison of pro- R and pro- S proton abstraction in citrate synthase at the CCSD(T)-in-DFT//MM level yields the correct enantioselectivity. We thus demonstrate the potential of projection-based embedding for determining stereoselectivity in enzymatic systems. We further show that the method is simple to apply, eliminates variability due to the choice of density functional theory functional and allows the efficient calculation of CCSD(T) quality enzyme reaction barriers.

Funder

Engineering and Physical Sciences Research Council

Royal Society

Biotechnology and Biological Sciences Research Council

Publisher

The Royal Society

Subject

Multidisciplinary

Reference42 articles.

1. The Citrate Enzymes: Their Structures, Mechanisms, and Biological Functions

2. Fluoroacetate and fluorocitrate: Mechanism of action

3. Studies with specific enzyme inhibitors XII. Resolution of DL–erythm–fluorocitric acid into optically active isomers;Dumel RJ;J. Biol. Chem.,1969

4. Absolute configuration of the isomer of fluorocitrate that inhibits aconitase

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