Snapshots of PLP-substrate and PLP-product external aldimines as intermediates in two types of cysteine desulfurase enzymes

Ryosuke Nakamura; Masahide Hikita; Shoko Ogawa; Yasuhiro Takahashi; Takashi Fujishiro

doi:10.1111/febs.15081

Snapshots of PLP-substrate and PLP-product external aldimines as intermediates in two types of cysteine desulfurase enzymes

FEBS J. 2020 Mar;287(6):1138-1154. doi: 10.1111/febs.15081. Epub 2019 Oct 19.

Authors

Ryosuke Nakamura¹, Masahide Hikita², Shoko Ogawa¹, Yasuhiro Takahashi¹, Takashi Fujishiro¹

Affiliations

¹ Department of Biochemistry and Molecular Biology, Graduate School of Science and Engineering, Saitama University, Saitama, Japan.
² Structural Biology Research Center, Photon Factory, Institute of Materials Structure Science, High Energy Accelerator Research Organization, Tsukuba, Japan.

PMID: 31587510
DOI: 10.1111/febs.15081

Abstract

Cysteine desulfurase enzymes catalyze sulfur mobilization from l-cysteine to sulfur-containing biomolecules such as iron-sulfur (Fe-S) clusters and thio-tRNAs. The enzymes utilize the cofactor pyridoxal-5'-phosphate (PLP), which forms the external substrate- and product-aldimines and ketimines during catalysis and are grouped into two types (I and II) based on their different catalytic loops. To clarify the structure-based catalytic mechanisms for each group, we determined the structures of the external substrate- and product-aldimines as catalytic intermediates of NifS (type I) and SufS (type II) that are involved in Fe-S cluster biosynthesis using X-ray crystallographic snapshot analysis. As a common intermediate structure, the thiol group of the PLP-l-cysteine external aldimine is stabilized by the conserved histidine adjacent to PLP through a polar interaction. This interaction makes the thiol group orientated for subsequent nucleophilic attack by a conserved cysteine residue on the catalytic loop in the state of PLP-l-cysteine ketimine, which is formed from the PLP-l-cysteine aldimine. Unlike the intermediates, structural changes of the loops were different between the type I and II enzymes. In the type I enzyme, conformational and topological change of the loop is necessary for nucleophilic attack by the cysteine. In contrast, the loop in type II cysteine desulfurase enzymes showed no large conformational change; rather, it might possibly orient the thiol group of the catalytic cysteine for nucleophilic attack toward PLP-l-cysteine. The present structures allow a revision of the catalytic mechanism and may provide a clue for consideration of enzyme function, structural diversity, and evolution of cysteine desulfurase enzymes. DATABASE: Structural data are available in PDB database under the accession numbers 5WT2, 5WT4, 5ZSP, 5ZST, 5ZS9, 5ZSK, 5ZSO, 6KFZ, 6KG0, and 6KG1.

Keywords: X-ray crystallography; biosynthesis; cysteine desulfurase; enzyme catalysis; reaction intermediates.

Publication types

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

MeSH terms

Bacillus subtilis / enzymology
Biocatalysis
Carbon-Sulfur Lyases / chemistry
Carbon-Sulfur Lyases / metabolism*
Crystallography, X-Ray
Helicobacter pylori / enzymology
Imines / chemistry
Imines / metabolism*
Models, Molecular
Pyridoxal Phosphate / chemistry
Pyridoxal Phosphate / metabolism*

Substances

Imines
Pyridoxal Phosphate
Carbon-Sulfur Lyases
cysteine desulfurase