Structure and Dynamics of the Staphylococcal Pyridoxal 5-phosphate Synthase Complex Reveal Transient Interactions at the Enzyme Interface

Overview

Journal J Biol Chem

Specialty Biochemistry

Date 2024 May 23

PMID 38782204

Authors

Angelica Luana C Barra

Najeeb Ullah

Hevila Brognaro

Raissa F Gutierrez

Carsten Wrenger

Christian Betzel

Alessandro S Nascimento

Affiliations

Soon will be listed here.

Abstract

Infectious diseases are a significant cause of death, and recent studies estimate that common bacterial infectious diseases were responsible for 13.6% of all global deaths in 2019. Among the most significant bacterial pathogens is Staphylococcus aureus, accounting for more than 1.1 million deaths worldwide in 2019. Vitamin biosynthesis has been proposed as a promising target for antibacterial therapy. Here, we investigated the biochemical, structural, and dynamic properties of the enzyme complex responsible for vitamin B6 (pyridoxal 5-phosphate, PLP) biosynthesis in S. aureus, which comprises enzymes SaPdx1 and SaPdx2. The crystal structure of the 24-mer complex of SaPdx1-SaPdx2 enzymes indicated that the S. aureus PLP synthase complex forms a highly dynamic assembly with transient interaction between the enzymes. Solution scattering data indicated that SaPdx2 typically binds to SaPdx1 at a substoichiometric ratio. We propose a structure-based view of the PLP synthesis mechanism initiated with the assembly of SaPLP synthase complex that proceeds in a highly dynamic interaction between Pdx1 and Pdx2. This interface interaction can be further explored as a potentially druggable site for the design of new antibiotics.

Citing Articles

Structure and identification of the native PLP synthase complex from lysate.

Agnew A, Humm E, Zhou K, Gunsalus R, Zhou Z mBio. 2024; 16(1):e0309024.

PMID: 39589128 PMC: 11708016. DOI: 10.1128/mbio.03090-24.

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