DUGiDocsEnzymatic Control over Reactive Intermediates Enables Direct Oxidation of Alkenes to Carbonyls by a P450 Iron-Oxo Species
dc.contributor.author
dc.date.accessioned
2022-09-23T06:20:55Z
dc.date.available
2022-09-23T06:20:55Z
dc.date.issued
2022-08-23
dc.identifier.issn
0002-7863
dc.identifier.uri
dc.description.abstract
The aerobic oxidation of alkenes to carbonyls is an important and challenging transformation in synthesis. Recently, a new P450-based enzyme (aMOx) has been evolved in the laboratory to directly oxidize styrenes to their corresponding aldehydes with high activity and selectivity. The enzyme utilizes a heme-based, high-valent iron-oxo species as a catalytic oxidant that normally epoxidizes alkenes, similar to other catalysts. How the evolved aMOx enzyme suppresses the commonly preferred epoxidation and catalyzes direct carbonyl formation is currently not well understood. Here, we combine computational modelling together with mechanistic experiments to study the reaction mechanism and unravel the molecular basis behind the selectivity achieved by aMOx. Our results describe that although both pathways are energetically accessible diverging from a common covalent radical intermediate, intrinsic dynamic effects determine the strong preference for epoxidation. We discovered that aMOx overrides these intrinsic preferences by controlling the accessible conformations of the covalent radical intermediate. This disfavors epoxidation and facilitates the formation of a carbocation intermediate that generates the aldehyde product through a fast 1,2-hydride migration. Electrostatic preorganization of the enzyme active site also contributes to the stabilization of the carbocation intermediate. Computations predicted that the hydride migration is stereoselective due to the enzymatic conformational control over the intermediate species. These predictions were corroborated by experiments using deuterated styrene substrates, which proved that the hydride migration is cis- and enantioselective. Our results demonstrate that directed evolution tailored a highly specific active site that imposes strong steric control over key fleeting biocatalytic intermediates, which is essential for accessing the carbonyl forming pathway and preventing competing epoxidation
dc.description.sponsorship
This work was supported by the Spanish MICINN (Ministerio
de Ciencia e Innovación) PID2019-111300GA-I00 project and
the Ramón y Cajal program via the RYC 2020-028628-I
fellowship (M.G.B), the Generalitat de Catalunya AGAUR
Beatriu de Pinós H2020 MSCA- COFUND (grant agreement
No 801370) 2018-BP-00204 project (M.G.B.), the Spanish
MIU (Ministerio de Universidades) predoctoral FPU fellowship
FPU18/02380 (J.S.), and the Deutsche Forschungsgemeinschaft via the Emmy Noether fellowship 420112577 (S.C.H.)
Open Access funding provided thanks to the CRUE-CSIC agreement with ACS
dc.format.mimetype
application/pdf
dc.language.iso
eng
dc.publisher
American Chemical Society (ACS)
dc.relation
PID2019-111300GA-I00
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Reproducció digital del document publicat a: https://doi.org/10.1021/jacs.2c02567
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Journal of the American Chemical Society (JACS), 2022, vol. 144, núm. 35, p. 15954-15968
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Articles publicats (D-Q)
dc.rights
Attribution 4.0 International
dc.rights.uri
dc.title
Enzymatic Control over Reactive Intermediates Enables Direct Oxidation of Alkenes to Carbonyls by a P450 Iron-Oxo Species
dc.type
info:eu-repo/semantics/article
dc.rights.accessRights
info:eu-repo/semantics/openAccess
dc.relation.projectID
info:eu-repo/grantAgreement/AEI/Plan Estatal de Investigación Científica y Técnica y de Innovación 2017-2020/PID2019-111300GA-I00/ES/CARACTERIZACION MULTIESCALAR DE INTERMEDIOS REACTIVOS PARA EL DESCUBRIMIENTO Y DISEÑO DE NUEVAS ACTIVIDADES BIOCATALITICAS/
dc.type.version
info:eu-repo/semantics/publishedVersion
dc.identifier.doi
dc.identifier.idgrec
035651
dc.contributor.funder
dc.type.peerreviewed
peer-reviewed
dc.relation.FundingProgramme
dc.relation.ProjectAcronym
dc.identifier.eissn
1520-5126