Broad substrate scope C-C oxidation in cyclodipeptides catalysed by a flavin-dependent filament

Emmajay Sutherland; Christopher J. Harding; Tancrede du Monceau de Bergendal; Gordon J. Florence; Katrin Ackermann; Bela E. Bode; Silvia Synowsky; Ramasburamanian Sundaramoorthy; Clarissa Melo Czekster

doi:10.1038/S41467-025-56127-Y

Broad substrate scope C-C oxidation in cyclodipeptides catalysed by a flavin-dependent filament

Emmajay Sutherland, Christopher J. Harding, Tancrede du Monceau de Bergendal, Gordon J. Florence, Katrin Ackermann, Bela E. Bode, Silvia Synowsky, Ramasburamanian Sundaramoorthy^*, Clarissa Melo Czekster^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

Abstract

Cyclic dipeptides are produced by organisms across all domains of life, with many exhibiting anticancer and antimicrobial properties. Oxidations are often key to their biological activities, particularly C-C bond oxidation catalysed by tailoring enzymes including cyclodipeptide oxidases. These flavin-dependent enzymes are underexplored due to their intricate three-dimensional arrangement involving multiple copies of two distinct small subunits, and mechanistic details underlying substrate selection and catalysis are lacking. Here, we determined the structure and mechanism of the cyclodipeptide oxidase from the halophile Nocardiopsis dassonvillei (NdasCDO), a component of the biosynthetic pathway for nocazine natural products. We demonstrated that NdasCDO forms filaments in solution, with a covalently bound flavin mononucleotide (FMN) cofactor at the interface between three distinct subunits. The enzyme exhibits promiscuity, processing various cyclic dipeptides as substrates in a distributive manner. The reaction is optimal at high pH and involves the formation of a radical intermediate. Pre-steady-state kinetics, a significant solvent kinetic isotope effect, and the absence of viscosity effects suggested that a step linked to FMN regeneration controlled the reaction rate. Our work elucidates the complex mechanistic and structural characteristics of this dehydrogenation reaction, positioning NdasCDO as a promising biocatalyst and expanding the FMN-dependent oxidase family to include enzyme filaments.

Original language	English
Article number	995
Number of pages	14
Journal	Nature Communications
Volume	16
DOIs	https://doi.org/10.1038/S41467-025-56127-Y
Publication status	Published - 24 Jan 2025

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Clarissa Czekster ISSF3 round 6: Clarissa Czekster ISSF3 round 6
Melo Czekster, C. (PI)
The Wellcome Trust
1/04/21 → 31/03/22
Project: Standard
Cryogen-free arbitrary waveform EPR: Cryogen-free arbitrary waveform EPR for structural Biology and Biophysics
Bode, B. E. (PI), Lovett, J. E. (CoI), Pliotas, C. (CoI), Schwarz-Linek, U. (CoI), Smith, G. M. (CoI), Stewart, A. J. (CoI) & White, M. (CoI)
1/05/18 → 30/04/19
Project: Standard
ISSF3 Invest People - Czekster: ISSF3 Czekster
Melo Czekster, C. (PI)
The Wellcome Trust
1/09/17 → 31/08/18
Project: Standard

Figure S3. LC-MS analysis of oxidised CDP substrates
Sutherland, E. (Creator) & Czekster, C. M. (Creator), Figshare, 2024
DOI: 10.6084/m9.figshare.25556850.v1
Dataset
Broad substrate scope C-C oxidation in cyclodipeptides catalysed by a flavin-dependent filament (EPR dataset)
Ackermann, K. (Creator) & Bode, B. E. (Creator), University of St Andrews, 6 Jan 2025
DOI: 10.17630/2e946d01-0753-45ad-aaf3-87572eef9ec0
Dataset

File

Cite this

@article{f5b4cd2a29cd459b9b40e4c78d1068f4,

title = "Broad substrate scope C-C oxidation in cyclodipeptides catalysed by a flavin-dependent filament",

abstract = "Cyclic dipeptides are produced by organisms across all domains of life, with many exhibiting anticancer and antimicrobial properties. Oxidations are often key to their biological activities, particularly C-C bond oxidation catalysed by tailoring enzymes including cyclodipeptide oxidases. These flavin-dependent enzymes are underexplored due to their intricate three-dimensional arrangement involving multiple copies of two distinct small subunits, and mechanistic details underlying substrate selection and catalysis are lacking. Here, we determined the structure and mechanism of the cyclodipeptide oxidase from the halophile Nocardiopsis dassonvillei (NdasCDO), a component of the biosynthetic pathway for nocazine natural products. We demonstrated that NdasCDO forms filaments in solution, with a covalently bound flavin mononucleotide (FMN) cofactor at the interface between three distinct subunits. The enzyme exhibits promiscuity, processing various cyclic dipeptides as substrates in a distributive manner. The reaction is optimal at high pH and involves the formation of a radical intermediate. Pre-steady-state kinetics, a significant solvent kinetic isotope effect, and the absence of viscosity effects suggested that a step linked to FMN regeneration controlled the reaction rate. Our work elucidates the complex mechanistic and structural characteristics of this dehydrogenation reaction, positioning NdasCDO as a promising biocatalyst and expanding the FMN-dependent oxidase family to include enzyme filaments.",

author = "Emmajay Sutherland and Harding, {Christopher J.} and {du Monceau de Bergendal}, Tancrede and Florence, {Gordon J.} and Katrin Ackermann and Bode, {Bela E.} and Silvia Synowsky and Ramasburamanian Sundaramoorthy and {Melo Czekster}, Clarissa",

note = "Funding: The authors thank the University of Dundee Cryo-EM facility for access to the instrumentation, funded by Wellcome (223816/Z/21/Z) and MRC (MRC World Class Laboratories PO 4050845509). They thank electron Bio-Imaging Centre (eBIC) facility, Diamond light source Ltd, UK for collection of 300kV electron microscope data. E.S. was funded by the Cunningham Trust (PhD-CT-18-41), C.M.C. is funded by the Wellcome Trust (210486/Z/18/Z and [204821/Z/16/Z] to the University of St Andrews), B.E.B. acknowledges equipment funding by BBSRC (BB/R013780/1), R.S. is funded by the Wellcome Trust (223816/Z/21/Z). ",

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month = jan,

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doi = "10.1038/S41467-025-56127-Y",

language = "English",

volume = "16",

journal = "Nature Communications",

issn = "2041-1723",

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TY - JOUR

T1 - Broad substrate scope C-C oxidation in cyclodipeptides catalysed by a flavin-dependent filament

AU - Sutherland, Emmajay

AU - Harding, Christopher J.

AU - du Monceau de Bergendal, Tancrede

AU - Florence, Gordon J.

AU - Ackermann, Katrin

AU - Bode, Bela E.

AU - Synowsky, Silvia

AU - Sundaramoorthy, Ramasburamanian

AU - Melo Czekster, Clarissa

N1 - Funding: The authors thank the University of Dundee Cryo-EM facility for access to the instrumentation, funded by Wellcome (223816/Z/21/Z) and MRC (MRC World Class Laboratories PO 4050845509). They thank electron Bio-Imaging Centre (eBIC) facility, Diamond light source Ltd, UK for collection of 300kV electron microscope data. E.S. was funded by the Cunningham Trust (PhD-CT-18-41), C.M.C. is funded by the Wellcome Trust (210486/Z/18/Z and [204821/Z/16/Z] to the University of St Andrews), B.E.B. acknowledges equipment funding by BBSRC (BB/R013780/1), R.S. is funded by the Wellcome Trust (223816/Z/21/Z).

PY - 2025/1/24

Y1 - 2025/1/24

N2 - Cyclic dipeptides are produced by organisms across all domains of life, with many exhibiting anticancer and antimicrobial properties. Oxidations are often key to their biological activities, particularly C-C bond oxidation catalysed by tailoring enzymes including cyclodipeptide oxidases. These flavin-dependent enzymes are underexplored due to their intricate three-dimensional arrangement involving multiple copies of two distinct small subunits, and mechanistic details underlying substrate selection and catalysis are lacking. Here, we determined the structure and mechanism of the cyclodipeptide oxidase from the halophile Nocardiopsis dassonvillei (NdasCDO), a component of the biosynthetic pathway for nocazine natural products. We demonstrated that NdasCDO forms filaments in solution, with a covalently bound flavin mononucleotide (FMN) cofactor at the interface between three distinct subunits. The enzyme exhibits promiscuity, processing various cyclic dipeptides as substrates in a distributive manner. The reaction is optimal at high pH and involves the formation of a radical intermediate. Pre-steady-state kinetics, a significant solvent kinetic isotope effect, and the absence of viscosity effects suggested that a step linked to FMN regeneration controlled the reaction rate. Our work elucidates the complex mechanistic and structural characteristics of this dehydrogenation reaction, positioning NdasCDO as a promising biocatalyst and expanding the FMN-dependent oxidase family to include enzyme filaments.

AB - Cyclic dipeptides are produced by organisms across all domains of life, with many exhibiting anticancer and antimicrobial properties. Oxidations are often key to their biological activities, particularly C-C bond oxidation catalysed by tailoring enzymes including cyclodipeptide oxidases. These flavin-dependent enzymes are underexplored due to their intricate three-dimensional arrangement involving multiple copies of two distinct small subunits, and mechanistic details underlying substrate selection and catalysis are lacking. Here, we determined the structure and mechanism of the cyclodipeptide oxidase from the halophile Nocardiopsis dassonvillei (NdasCDO), a component of the biosynthetic pathway for nocazine natural products. We demonstrated that NdasCDO forms filaments in solution, with a covalently bound flavin mononucleotide (FMN) cofactor at the interface between three distinct subunits. The enzyme exhibits promiscuity, processing various cyclic dipeptides as substrates in a distributive manner. The reaction is optimal at high pH and involves the formation of a radical intermediate. Pre-steady-state kinetics, a significant solvent kinetic isotope effect, and the absence of viscosity effects suggested that a step linked to FMN regeneration controlled the reaction rate. Our work elucidates the complex mechanistic and structural characteristics of this dehydrogenation reaction, positioning NdasCDO as a promising biocatalyst and expanding the FMN-dependent oxidase family to include enzyme filaments.

U2 - 10.1038/S41467-025-56127-Y

DO - 10.1038/S41467-025-56127-Y

M3 - Article

C2 - 39856061

SN - 2041-1723

VL - 16

JO - Nature Communications

JF - Nature Communications

M1 - 995

ER -

Broad substrate scope C-C oxidation in cyclodipeptides catalysed by a flavin-dependent filament

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Projects

Clarissa Czekster ISSF3 round 6: Clarissa Czekster ISSF3 round 6

Cryogen-free arbitrary waveform EPR: Cryogen-free arbitrary waveform EPR for structural Biology and Biophysics

ISSF3 Invest People - Czekster: ISSF3 Czekster

Datasets

Figure S3. LC-MS analysis of oxidised CDP substrates

Broad substrate scope C-C oxidation in cyclodipeptides catalysed by a flavin-dependent filament (EPR dataset)

Cite this