Investigation of biofilm production and its association with genetic and phenotypic characteristics of OM (osteomyelitis) and non-OM orthopedic Staphylococcus aureus

Shengpeng Yu; Bei Jiang; Chao Jia; Hongri Wu; Jie Shen; Xiaomei Hu; Zhao Xie

doi:10.1186/s12941-020-00352-4

Annals of Clinical Microbiology and Antimicrobials (Mar 2020)

Investigation of biofilm production and its association with genetic and phenotypic characteristics of OM (osteomyelitis) and non-OM orthopedic Staphylococcus aureus

Shengpeng Yu,
Bei Jiang,
Chao Jia,
Hongri Wu,
Jie Shen,
Xiaomei Hu,
Zhao Xie

Affiliations

Shengpeng Yu: Department of Orthopedics, Southwest Hospital, Army Medical University
Bei Jiang: Department of Orthopedics, Southwest Hospital, Army Medical University
Chao Jia: Department of Orthopedics, Southwest Hospital, Army Medical University
Hongri Wu: Department of Orthopedics, Southwest Hospital, Army Medical University
Jie Shen: Department of Orthopedics, Southwest Hospital, Army Medical University
Xiaomei Hu: Department of Microbiology, College of Basic Medical Sciences, Army Medical University
Zhao Xie: Department of Orthopedics, Southwest Hospital, Army Medical University

DOI: https://doi.org/10.1186/s12941-020-00352-4
Journal volume & issue: Vol. 19, no. 1
pp. 1 – 9

Abstract

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Abstract Background Staphylococcus aureus is a primary pathogen of orthopedic infections. By mediating antimicrobial resistance, S. aureus biofilm plays an important role in the recalcitrance of orthopedic infections, especially for the intractable osteomyelitis (OM). This study investigated the relationship between biofilm production and various genetic or phenotypic characteristics among orthopedic S. aureus strains. Methods A total of 137 orthopedic S. aureus isolates were enrolled and divided into OM and non-OM groups. Biofilm production was evaluated using the crystal violet assay. Genetic and phenotypic characteristics including MRSA identification, MLST and spa typing, carriage of virulence genes, drug resistance, and patients’ inflammatory responses indicators were characterized. The relationship between biofilm production and above-mentioned features was respectively analyzed among all isolates and compared between OM and non-OM isolates. Results Biofilm production presented no significant difference between OM (including 9 MRSA isolates) and non-OM (including 21 MRSA isolates) strains. We found that ST88, t377 and ST630-MSSA-t377 strains produced very strong biofilms, while MLST types of ST15, ST25, ST398, ST5, ST59 and spa types of t002, t2325, t437 tended to produce weaker biofilms. Strains with the following profiles produced stronger biofilms: fib(+)-hlgv(+)-lukED(+)-sei(-)-sem(-)-seo(-) for all isolates, sei(-)-sem(-)-seo(-) for OM isolates, and cna (+)-fib (+)-hlgv (+)-lukED (+)-seb(-)-sed(-) for non-OM isolates. In addition, not any single drug resistance was found to be related to biofilm production. We also observed that, among OM patients, strains with stronger biofilms caused weaker inflammatory responses. Conclusion Some genetic or phenotypic characteristics of orthopedic strains were associated with biofilm production, and this association could be different among OM and non-OM strains. The results are of great significance for better understanding, evaluating and managing different kinds of biofilm-associated orthopedic infections, and provide potential targets for biofilm clearance.

Published in Annals of Clinical Microbiology and Antimicrobials

ISSN: 1476-0711 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Therapeutics. Pharmacology; Medicine: Internal medicine: Infectious and parasitic diseases; Science: Microbiology
Website: http://ann-clinmicrob.biomedcentral.com

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