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Rational design of a cyclohexanone dehydrogenase for enhanced α,β-desaturation and substrate specificity

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Version 2 2024-09-13, 14:16
Version 1 2024-04-23, 10:25
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posted on 2024-09-13, 14:16 authored by Warispreet SinghWarispreet Singh, Nicola Brown, Hannah V McCue, Sophie R Marriott, Richard C Wilson, Justin PerryJustin Perry, Johan P. Turkenburg, Kshatresh Dutta Dubey, Stephen H. Prior, Andrew J Carnell, Edward TaylorEdward Taylor, Gary W. Black
<p dir="ltr">The selective α,β-desaturation of cyclic carbonyl compounds, which are found in the core of many steroid and bioactive molecules, using green chemistry is highly desirable. To achieve this task, we have for the first time described and solved the <i>de novo</i> structure of a member of the cyclohexanone dehydrogenase class of enzymes. The breadth of substrate specificity was investigated by assaying the cyclohexanone dehydrogenase, from <i>Alicycliphilus denitrificans</i>, against several cyclic ketones, lactones and lactams. To investigate substrate binding, a catalytic variant, Y195F, was generated and used to obtain a crystallographic complex with the natural substrate, cyclohexanone. This revealed substrate–active site interactions, as well as the proximity of the cofactor, flavin adenine dinucleotide, and enabled us to propose a mechanistic function to key amino acids. We then used molecular dynamic simulations to guide design to add functionality to the cyclohexanone dehydrogenase enzyme. The resulting W113A variant had overall improved enzyme activity and substrate scope, <i>i.e.</i>, accepting the bulkier carbonyl compound, dihydrocoumarin. Structural analysis of the W113A variant revealed a broader, more open active site, which helped explain the modified substrate specificity. This work paves the way for future bespoke regioselective α,β-desaturation in the synthesis of important bioactive molecules <i>via</i> rational enzyme engineering.</p>

History

School affiliated with

  • Department of Life Sciences (Research Outputs)
  • College of Health and Science (Research Outputs)

Publication Title

Chemical Science

Volume

15

Issue

13

Publisher

Royal Society of Chemistry

ISSN

2041-6520

eISSN

2041-6539

Date Submitted

2023-08-01

Date Accepted

2024-02-08

Date of First Publication

2024-02-21

Date of Final Publication

2024-04-07

Funder

WS acknowledge the support by Research England's Expanding Excellence in England (E3) Fund. KDD acknowledges the Department of Biotechnology, Govt. of India for the Ramalingaswami Re-entry research grant (BT/RLF/Re-entry/10/2017). GWB acknowledges support by the BBSRC Networks in Industrial Biotechnology and Bioenergy BIOCATNET Proof-of-Concept Fund (part of BB/L013649/12017)

Open Access Status

  • Open Access

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