Computational characterization of enzyme-bound thiamin diphosphate reveals a surprisingly stable tricyclic state: implications for catalysis

Computational characterization of enzyme-bound thiamin diphosphate reveals a surprisingly stable tricyclic state: implications for catalysis

Thiamin diphosphate (ThDP)-dependent enzymes constitute a large class of enzymes that catalyze a diverse range of reactions. Many are involved in stereospecific carbon–carbon bond formation and, consequently, have found increasing interest and utility as chiral catalysts in various biocatalytic appl...

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Main Authors: Ferran Planas, Michael J. McLeish, Fahmi Himo
Format: Article
Language:English
Published: Beilstein-Institut 2019-01-01
Series:Beilstein Journal of Organic Chemistry
Subjects:
binding site
DFT
enzyme mechanism
quantum chemical calculations
ThDP-dependent
Online Access:https://doi.org/10.3762/bjoc.15.15
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spelling doaj-17c8c6f8cfc64fb1b78a4f658af4c8f82021-02-02T00:18:41ZengBeilstein-InstitutBeilstein Journal of Organic Chemistry1860-53972019-01-0115114515910.3762/bjoc.15.151860-5397-15-15Computational characterization of enzyme-bound thiamin diphosphate reveals a surprisingly stable tricyclic state: implications for catalysisFerran Planas0Michael J. McLeish1Fahmi Himo2Department of Organic Chemistry, Arrhenius Laboratory, Stockholm University, SE-10691 Stockholm, SwedenDepartment of Chemistry and Chemical Biology, Indiana University-Purdue University Indianapolis, Indianapolis IN 46202, USADepartment of Organic Chemistry, Arrhenius Laboratory, Stockholm University, SE-10691 Stockholm, SwedenThiamin diphosphate (ThDP)-dependent enzymes constitute a large class of enzymes that catalyze a diverse range of reactions. Many are involved in stereospecific carbon–carbon bond formation and, consequently, have found increasing interest and utility as chiral catalysts in various biocatalytic applications. All ThDP-catalyzed reactions require the reaction of the ThDP ylide (the activated state of the cofactor) with the substrate. Given that the cofactor can adopt up to seven states on an enzyme, identifying the factors affecting the stability of the pre-reactant states is important for the overall understanding of the kinetics and mechanism of the individual reactions.In this paper we use density functional theory calculations to systematically study the different cofactor states in terms of energies and geometries. Benzoylformate decarboxylase (BFDC), which is a well characterized chiral catalyst, serves as the prototypical ThDP-dependent enzyme. A model of the active site was constructed on the basis of available crystal structures, and the cofactor states were characterized in the presence of three different ligands (crystallographic water, benzoylformate as substrate, and (R)-mandelate as inhibitor). Overall, the calculations reveal that the relative stabilities of the cofactor states are greatly affected by the presence and identity of the bound ligands. A surprising finding is that benzoylformate binding, while favoring ylide formation, provided even greater stabilization to a catalytically inactive tricyclic state. Conversely, the inhibitor binding greatly destabilized the ylide formation. Together, these observations have significant implications for the reaction kinetics of the ThDP-dependent enzymes, and, potentially, for the use of unnatural substrates in such reactions.https://doi.org/10.3762/bjoc.15.15binding siteDFTenzyme mechanismquantum chemical calculationsThDP-dependent
collection DOAJ
language English
format Article
sources DOAJ
author Ferran Planas
Michael J. McLeish
Fahmi Himo
spellingShingle Ferran Planas
Michael J. McLeish
Fahmi Himo
Computational characterization of enzyme-bound thiamin diphosphate reveals a surprisingly stable tricyclic state: implications for catalysis
Beilstein Journal of Organic Chemistry
binding site
DFT
enzyme mechanism
quantum chemical calculations
ThDP-dependent
author_facet Ferran Planas
Michael J. McLeish
Fahmi Himo
author_sort Ferran Planas
title Computational characterization of enzyme-bound thiamin diphosphate reveals a surprisingly stable tricyclic state: implications for catalysis
title_short Computational characterization of enzyme-bound thiamin diphosphate reveals a surprisingly stable tricyclic state: implications for catalysis
title_full Computational characterization of enzyme-bound thiamin diphosphate reveals a surprisingly stable tricyclic state: implications for catalysis
title_fullStr Computational characterization of enzyme-bound thiamin diphosphate reveals a surprisingly stable tricyclic state: implications for catalysis
title_full_unstemmed Computational characterization of enzyme-bound thiamin diphosphate reveals a surprisingly stable tricyclic state: implications for catalysis
title_sort computational characterization of enzyme-bound thiamin diphosphate reveals a surprisingly stable tricyclic state: implications for catalysis
publisher Beilstein-Institut
series Beilstein Journal of Organic Chemistry
issn 1860-5397
publishDate 2019-01-01
description Thiamin diphosphate (ThDP)-dependent enzymes constitute a large class of enzymes that catalyze a diverse range of reactions. Many are involved in stereospecific carbon–carbon bond formation and, consequently, have found increasing interest and utility as chiral catalysts in various biocatalytic applications. All ThDP-catalyzed reactions require the reaction of the ThDP ylide (the activated state of the cofactor) with the substrate. Given that the cofactor can adopt up to seven states on an enzyme, identifying the factors affecting the stability of the pre-reactant states is important for the overall understanding of the kinetics and mechanism of the individual reactions.In this paper we use density functional theory calculations to systematically study the different cofactor states in terms of energies and geometries. Benzoylformate decarboxylase (BFDC), which is a well characterized chiral catalyst, serves as the prototypical ThDP-dependent enzyme. A model of the active site was constructed on the basis of available crystal structures, and the cofactor states were characterized in the presence of three different ligands (crystallographic water, benzoylformate as substrate, and (R)-mandelate as inhibitor). Overall, the calculations reveal that the relative stabilities of the cofactor states are greatly affected by the presence and identity of the bound ligands. A surprising finding is that benzoylformate binding, while favoring ylide formation, provided even greater stabilization to a catalytically inactive tricyclic state. Conversely, the inhibitor binding greatly destabilized the ylide formation. Together, these observations have significant implications for the reaction kinetics of the ThDP-dependent enzymes, and, potentially, for the use of unnatural substrates in such reactions.
topic binding site
DFT
enzyme mechanism
quantum chemical calculations
ThDP-dependent
url https://doi.org/10.3762/bjoc.15.15
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AT michaeljmcleish computationalcharacterizationofenzymeboundthiamindiphosphaterevealsasurprisinglystabletricyclicstateimplicationsforcatalysis
AT fahmihimo computationalcharacterizationofenzymeboundthiamindiphosphaterevealsasurprisinglystabletricyclicstateimplicationsforcatalysis
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