AI Article Synopsis

  • Cysteine dioxygenase (CDO) is an enzyme that converts cysteine into cysteine sulfinic acid, with a unique crosslink enhancing its catalytic efficiency.
  • The study focused on creating a variant of bacterial CDO (G82C) to test if a single DNA mutation could allow crosslink formation, showing that it indeed can form the crosslink but with lower efficiency than the wild-type enzyme.
  • Bioinformatics revealed many potential crosslinked CDOs in Gram-negative pathogenic bacteria, indicating a broader biological significance for this crosslink formation.

Article Abstract

Cysteine dioxygenase (CDO) is a non-heme iron-containing enzyme that catalyzes the oxidation of cysteine (Cys) to cysteine sulfinic acid (CSA). Crystal structures of eukaryotic CDOs revealed the presence of an unusual crosslink between the sulfur of a cysteine residue (C93 in CDO, CDO) and a carbon atom adjacent to the phenyl group of a tyrosine residue (Y157). Formation of this crosslink occurs over time as a byproduct of catalysis and increases the catalytic efficiency of CDO by at least 10-fold. Interestingly, in bacterial CDOs, the residue corresponding to C93 is replaced by a highly conserved glycine (G82 in CDO, CDO), which precludes the formation of a C-Y crosslink in these enzymes; yet bacterial CDOs achieve turnover rates paralleling those of fully crosslinked eukaryotic CDOs. In the present study, we prepared the G82C variant of CDO to determine if a single DNA point mutation could lead to C-Y crosslink formation in this enzyme. We used gel electrophoresis, peptide mass spectrometry, electron paramagnetic resonance spectroscopy, and kinetic assays to characterize this variant alongside the natively crosslinked wild-type (WT) CDO and the natively non-crosslinked WT CDO. Collectively, our results provide compelling evidence that the G82C CDO variant is indeed capable of C-Y crosslink formation. Our kinetic studies indicate that G82C CDO has a reduced catalytic efficiency compared to WT CDO and that activity increases as the ratio of crosslinked to non-crosslinked enzyme increases. Finally, by carrying out a bioinformatic analysis of the CDO family, we were able to identify a large number of putatively crosslinked bacterial CDOs, the majority of which are from Gram-negative pathogenic bacteria.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10697556PMC
http://dx.doi.org/10.1021/acs.biochem.3c00083DOI Listing

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