Detection and expression of SapS, a class C nonspecific acid phosphatase with O-phospho-L- tyrosine-phosphatase activity, in Staphylococcus aureus isolates from patients with chronic osteomyelitis

Martínez-Canseco, Carlos; Franco-Bourland, Rebecca E.; González-Huerta, Norma; Paredes-Espinosa, Marco Antonio; Giono-Cerezo, Silvia; Sánchez-Chapul, Laura; Paniagua-Pérez, Rogelio; Valdez-Mijares, René; Hernández-Flores, Cecilia

doi:10.7705/biomedica.6604

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Biomédica

versión impresa ISSN 0120-4157versión On-line ISSN 2590-7379

Resumen

MARTINEZ-CANSECO, Carlos et al. Detection and expression of SapS, a class C nonspecific acid phosphatase with O-phospho-L- tyrosine-phosphatase activity, in Staphylococcus aureus isolates from patients with chronic osteomyelitis. Biomed. [online]. 2023, vol.43, n.2, pp.200-212. Epub 30-Jun-2023. ISSN 0120-4157. https://doi.org/10.7705/biomedica.6604.

Introduction.

The identity of Staphylococcus aureus virulence factors involved in chronic osteomyelitis remains unresolved. SapS is a class C non-specific acid phosphatase and a well-known virulence factor that has been identified in S. aureus strain 154 but in protein extracts from rotting vegetables.

Objective.

To identify the SapS gene and characterize the activity of SapS from S. aureus strains: 12 isolates from bone infected samples of patients treated for chronic osteomyelitis and 49 from a database with in silico analysis of complete bacterial genomes.

Materials and methods.

The SapS gene was isolated and sequenced from 12 S. aureus clinical isolates and two reference strains; 49 S. aureus strains and 11 coagulase-negative staphylococci were tested using in silico PCR. Culture media semi-purified protein extracts from the clinical strains were assayed for phosphatase activity with p-nitro-phenyl- phosphate, O-phospho-L-tyrosine, O-phospho-L-serine, and OphosphoL-threonine in conjunction with various phosphatase inhibitors.

Results.

SapS was detected in the clinical and in-silico S. aureus strains, but not in the in silico coagulase-negative staphylococci strains. Sec-type I lipoprotein-type N-terminal signal peptide sequences; secreted proteins, and aspartate bipartite catalytic domains coding sequences were found in the SapS nucleotide and amino acid sequence analysis. SapS dephosphorylated with p-nitro-phenyl-phosphate and ophosphoLtyrosine were selectively resistant to tartrate and fluoride, but sensitive to vanadate and molybdate.

Conclusion.

SapS gene was found in the genome of the clinical isolates and the in silico S. aureus strains. SapS shares biochemical similarities with known virulent bacterial, such as protein tyrosine phosphatases, suggesting it may be a virulence factor in chronic osteomyelitis.

Palabras clave : Staphylococcus aureus; virulence factors; osteomyelitis.

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