Mechanism of the Oxidative Ring-Closure Reaction During the Gliotoxin Biosynthesis by Cytochrome P450 GliF

Muizz Qureshi, Thirakorn Mokkawes, Yuanxin Cao, Samuel De Visser

Research output: Contribution to journalArticlepeer-review

Abstract

During the gliotoxin biosynthesis in fungi the cytochrome P450 GliF enzyme catalyzes an
unusual C−N ring-closure step while also an aromatic ring is hydroxylated in the same reaction cycle, which may have relevance to drug synthesis reactions in biotechnology. However, as the details of the reaction mechanism are still controversial, no applications have been developed yet. To resolve the mechanism of gliotoxin biosynthesis and gain insight into the steps leading to ring-closure, we ran a combination of molecular dynamics and density functional theory calculations on the structure and reactivity of P450 GliF and tested a range of possible reaction mechanisms, pathways and models. The calculations show that rather than hydrogen atom transfer from substrate to Com- pound I, an initial proton transfer transition state is followed by a fast electron transfer en route to the radical intermediate and hence a non-synchronous hydrogen atom abstraction takes place. The radical intermediate then reacts by OH rebound to the aromatic ring to form a biradical in the substrate that through ring-closure between the radical centers gives gliotoxin products. Interestingly, the structure and energetics of the reaction mechanisms appear little effected by the addition of polar groups to the model and hence we predict that the reaction can be catalyzed by other P450 isozymes that also bind the same substrate. Alternative pathways such as a pathway starting with an electrophilic attack on the arene to form an epoxide are high in energy and are ruled out.
Original languageEnglish
Article number8567
JournalInternational Journal of Molecular Sciences
Volume25
Issue number16
DOIs
Publication statusPublished - 6 Aug 2024

Keywords

  • density functional theory
  • enzyme catalysis
  • inorganic reaction mechanisms
  • cyto- 24 chrome P450 enzymes
  • mono-oxygenases

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