4.3 Article

Mapping bacterial biofilm on explanted orthopedic hardware: An analysis of 14 consecutive cases

期刊

APMIS
卷 131, 期 4, 页码 170-179

出版社

WILEY
DOI: 10.1111/apm.13295

关键词

Mapping biofilm; periprosthetic joint infection; total joint arthroplasty; implant surface culture; Staphylococcus aureus

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This study aimed to investigate whether certain components and their surface features are more prone to biofilm formation in primary total joint arthroplasty. It was found that biofilm predominantly formed on the non-articulating surfaces between components and on ridges and edges. This has important implications for intraoperative debridement, retention choices, and implant design.
Hardware implanted during primary total joint arthroplasty carries a serious risk for periprosthetic joint infection (PJI). The formation of bacterial biofilms, which are highly tolerant of antibiotics and host immunity, is recognized as being a major barrier to treatment. It is not known whether some components and their surface features are more prone to biofilm than others. This study attempted to map biofilm on different components and features of orthopedic hardware recovered during revision. Implant surface culture (ISC) was used on 53 components from 14 hip and knee revisions. ISC achieves a thin agar coating over components, followed by incubation and observation for colony outgrowth over 9 days. Recovered organisms were identified by selective culture and 16s rRNA sequencing. Outcomes were compared with clinical culturing and PJI diagnosis based on 2013 Musculoskeletal Infection Society criteria. ISC paralleled clinical culturing with a sensitivity of 100% and a specificity of 57.1%. When compared to Musculoskeletal Infection Society criteria, sensitivity remained at 100% while specificity was 80%. Biofilm accumulation was patchy and heterogeneous throughout different prostheses, though notably the non-articulating surfaces between the tibial tray and polyethylene insert showed consistent growth. On individual components, ridges and edges consistently harbored biofilm, while growth elsewhere was case dependent. ISC successfully identified microbial growth with high sensitivity while also revealing that biofilm growth was commonly localized to particular locations. Understanding where biofilm formation occurs most often on implanted hardware will help guide debridement, retention choices, and implant design.

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