Staphylococcus aureushas been involved in transfusion-transmitted fatalities associated with platelet concentrates (PCs) due to its heightened pathogenicity enhanced by genome-encoded virulence and antibiotic resistance genes. This may be facilitated by mobile genetic elements (MGEs) that can cause rearrangements. Several factors contribute toS. aureusvirulence, including the type VII secretion system (T7SS), composed of six core genes conserved acrossS. aureusstrains. In this study, we conducted comparative genome analyses of fiveS. aureusisolates from PCs (CI/BAC/25/13 /W, PS/BAC/169/17 /W and PS/BAC/317/16 /W were detected during PCs screening with the BACT/ALERT automated culture system, and ATR-20003 and CBS2016-05 were missed during screening and caused septic transfusion reactions). Multiple alignments of the genomes revealed evidence of rearrangements involving phage Sa3int in PS/BAC/169/17 /W and PS/BAC/317/16 /W. While the former had undergone translocation of its immune evasion cluster (IEC), the latter had lost part of the phage, leaving behind the IEC. This observation highlightsS. aureusgenome plasticity. Unexpectedly, strain CBS2016-05 was found to encode a pseudo-type VII secretion system (T7SS) that had lost five of the conserved core genes (esxA,esaA, essA, esaBandessB) and contained a 5′ truncatedessC. Since these genes are essential for the function of the T7SS protein transport machinery, which plays a key role inS. aureusvirulence, CBS2016-05 probably compensates by recruiting other export mechanisms and/or alternative virulence factors, such as neu-tralizing immunity proteins. This study unravels genome rearrangements inS. aureusisolated from PCs and reports the firstS. aureusisolate lacking conserved T7SS core genes.
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