Crystal structure of ArOYE6 reveals a novel C-terminal helical extension and mechanistic insights into the distinct class III OYEs from pathogenic fungi

Yeshveer Singh; Ruby Sharma; Manasi Mishra; Praveen Kumar Verma; Ajay Kumar Saxena

doi:10.1111/febs.16445

Crystal structure of ArOYE6 reveals a novel C-terminal helical extension and mechanistic insights into the distinct class III OYEs from pathogenic fungi

FEBS J. 2022 Sep;289(18):5531-5550. doi: 10.1111/febs.16445. Epub 2022 Mar 29.

Authors

Yeshveer Singh¹, Ruby Sharma², Manasi Mishra¹, Praveen Kumar Verma^{1

3}, Ajay Kumar Saxena²

Affiliations

¹ Plant Immunity Laboratory, National Institute of Plant Genome Research, New Delhi, India.
² Rm-403/440, Structural Biology Laboratory, School of Life Science, Jawaharlal Nehru University, New Delhi, India.
³ Plant Immunity Laboratory, School of Life Science, Jawaharlal Nehru University, New Delhi, India.

PMID: 35313092
DOI: 10.1111/febs.16445

Abstract

Old yellow enzymes (OYEs) play a critical role in antioxidation, detoxification and ergot alkaloid biosynthesis processes in various organisms. The yeast- and bacteria-like OYEs have been structurally characterized earlier, however, filamentous fungal pathogens possess a novel OYE class, that is, class III, whose biochemical and structural intricacies remain unexplored to date. Here, we present the 1.6 Å X-ray structure of a class III member, OYE 6 from necrotrophic fungus Ascochyta rabiei (ArOYE6), in flavin mononucleotide (FMN)-bound form (PDB ID-7FEV) and provide mechanistic insights into their catalytic capability. We demonstrate that ArOYE6 exists as a monomer in solution, forms (β/α)₈ barrel structure harbouring non-covalently bound FMN at cofactor binding site, and utilizes reduced nicotinamide adenine dinucleotide phosphate as its preferred reductant. The large hydrophobic cavity situated above FMN, specifically accommodates 12-oxo-phytodienoic acid and N-ethylmaleimide substrates as observed in ArOYE6-FMN-substrate ternary complex models. Site-directed mutations in the conserved catalytic (His196, His199 and Tyr201) and FMN-binding (Lys249 and Arg348) residues render the enzyme inactive. Intriguingly, the ArOYE6 structure contains a novel C-terminus (369-445 residues) made of three α-helices, which stabilizes the FMN binding pocket as its mutation/truncation lead to complete loss of FMN binding. Moreover, the loss of the extended C-terminus does not alter the monomeric nature of ArOYE6. In this study, for the first time, we provide the structural and biochemical insights for a fungi-specific class III OYE homologue and dissect the oxidoreductase mechanism. Our findings hold broad biological significance during host-fungus interactions owing to the conservation of this class among pathogenic fungi, and would have potential implications in the pharmacochemical industry.

Keywords: Ascochyta rabiei; C-terminal domain; old yellow enzyme; oxidoreductases; β/α barrel.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Crystallography, X-Ray
Ergot Alkaloids*
Ethylmaleimide
Flavin Mononucleotide / chemistry
NADP
NADPH Dehydrogenase* / chemistry
Oxidoreductases / metabolism
Reducing Agents

Substances

Ergot Alkaloids
Reducing Agents
NADP
Flavin Mononucleotide
Oxidoreductases
NADPH Dehydrogenase
Ethylmaleimide