4wvj Citations

Peptide binding to a bacterial signal peptidase visualized by peptide tethering and carrier-driven crystallization.

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Ting YT, Harris PW, Batot G, Brimble MA, Baker EN, Young PG
OpenAccess logo IUCrJ 3 10-9 (2016)
Related entries: 4wvg, 4wvh, 4wvi

Cited: 9 times
EuropePMC logo PMID: 26870377

Abstract

Bacterial type I signal peptidases (SPases) are membrane-anchored serine proteases that process the signal peptides of proteins exported via the Sec and Tat secretion systems. Despite their crucial importance for bacterial virulence and their attractiveness as drug targets, only one such enzyme, LepB from Escherichia coli, has been structurally characterized, and the transient nature of peptide binding has stymied attempts to directly visualize SPase-substrate complexes. Here, the crystal structure of SpsB, the type I signal peptidase from the Gram-positive pathogen Staphylococcus aureus, is reported, and a peptide-tethering strategy that exploits the use of carrier-driven crystallization is described. This enabled the determination of the crystal structures of three SpsB-peptide complexes, both with cleavable substrates and with an inhibitory peptide. SpsB-peptide interactions in these complexes are almost exclusively limited to the canonical signal-peptide motif Ala-X-Ala, for which clear specificity pockets are found. Minimal contacts are made outside this core, with the variable side chains of the peptides accommodated in shallow grooves or exposed faces. These results illustrate how high fidelity is retained despite broad sequence diversity, in a process that is vital for cell survival.

Articles - 4wvj mentioned but not cited (3)

  1. Peptide binding to a bacterial signal peptidase visualized by peptide tethering and carrier-driven crystallization. Ting YT, Harris PW, Batot G, Brimble MA, Baker EN, Young PG. IUCrJ 3 10-19 (2016)
  2. Targeted Isolation of Antibiotic Brominated Alkaloids from the Marine Sponge Pseudoceratina durissima Using Virtual Screening and Molecular Networking. Lever J, Kreuder F, Henry J, Hung A, Allard PM, Brkljača R, Rix C, Taki AC, Gasser RB, Kaslin J, Wlodkowic D, Wolfender JL, Urban S. Mar Drugs 20 554 (2022)
  3. Structural basis of broad-spectrum β-lactam resistance in Staphylococcus aureus. Alexander JAN, Worrall LJ, Hu J, Vuckovic M, Satishkumar N, Poon R, Sobhanifar S, Rosell FI, Jenkins J, Chiang D, Mosimann WA, Chambers HF, Paetzel M, Chatterjee SS, Strynadka NCJ. Nature 613 375-382 (2023)


Reviews citing this publication (4)

  1. Protein export through the bacterial Sec pathway. Tsirigotaki A, De Geyter J, Šoštaric N, Economou A, Karamanou S. Nat Rev Microbiol 15 21-36 (2017)
  2. Emerging peptide antibiotics with therapeutic potential. Upert G, Luther A, Obrecht D, Ermert P. Med Drug Discov 9 100078 (2021)
  3. Bacterial Signal Peptides- Navigating the Journey of Proteins. Kaushik S, He H, Dalbey RE. Front Physiol 13 933153 (2022)
  4. Increasing the Efficiency of the Accumulation of Recombinant Proteins in Plant Cells: The Role of Transport Signal Peptides. Rozov SM, Deineko EV. Plants (Basel) 11 2561 (2022)

Articles citing this publication (2)

  1. Group A Streptococcus T Antigens Have a Highly Conserved Structure Concealed under a Heterogeneous Surface That Has Implications for Vaccine Design. Young PG, Raynes JM, Loh JM, Proft T, Baker EN, Moreland NJ. Infect Immun 87 (2019)
  2. Antimicrobial Activity of Rhenium Di- and Tricarbonyl Diimine Complexes: Insights on Membrane-Bound S. aureus Protein Binding. Schindler K, Cortat Y, Nedyalkova M, Crochet A, Lattuada M, Pavic A, Zobi F. Pharmaceuticals (Basel) 15 1107 (2022)


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