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Elucidating the Signal Transduction Mechanism of the Blue-Light-Regulated Photoreceptor YtvA: From Photoactivation to Downstream Regulation

  • Yong Le He
  • , Jinnette Tolentino Collado
  • , James N. Iuliano
  • , Helena A. Woroniecka
  • , Christopher R. Hall
  • , Agnieszka A. Gil
  • , Sergey P. Laptenok
  • , Gregory M. Greetham
  • , Boris Illarionov
  • , Adelbert Bacher
  • , Markus Fischer
  • , Jarrod B. French
  • , Andras Lukacs
  • , Stephen R. Meech
  • , Peter J. Tonge
  • Stony Brook University
  • Rutherford Appleton Laboratory
  • University of East Anglia
  • University of Hamburg
  • Technical University of Munich
  • University of Minnesota
  • University of Pecs

Research output: Contribution to journalArticlepeer-review

5 Scopus citations

Abstract

The blue-light photoreceptor YtvA from Bacillus subtilis has an N-terminal flavin mononucleotide (FMN)-binding light-oxygen-voltage (LOV) domain that is fused to a C-terminal sulfate transporter and anti-σ factor antagonist (STAS) output domain. To interrogate the signal transduction pathway that leads to photoactivation, the STAS domain was replaced with a histidine kinase, so that photoexcitation of the flavin could be directly correlated with biological activity. N94, a conserved Asn that is hydrogen bonded to the FMN C2═O group, was replaced with Ala, Asp, and Ser residues to explore the role of this residue in triggering the structural dynamics that activate the output domain. Femtosecond to millisecond time-resolved multiple probe spectroscopy coupled with a fluorescence polarization assay revealed that the loss of the hydrogen bond between N94 and the C2═O group decoupled changes in the protein structure from photoexcitation. In addition, alterations in N94 also decreased the stability of the Cys-FMN adduct formed in the light-activated state by up to a factor of ∼25. Collectively, these studies shed light on the role of the hydrogen bonding network in the LOV β-scaffold in signal transduction.

Original languageEnglish
Pages (from-to)696-706
Number of pages11
JournalACS Chemical Biology
Volume19
Issue number3
DOIs
StatePublished - Mar 15 2024

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