Abstract
Bacteriophage endolysins and their derivatives have strong potential as antibacterial agents considering the increasing prevalence of antibiotic resistance in common bacterial pathogens. The peptidoglycan degrading peptidase CHAPk, a truncated derivate of staphylococcal phage K endolysin (LysK), has proven efficacy in preventing and disrupting staphylococcal biofilms. Nevertheless, the concentration of CHAPk required to eliminate populations of stationary-phase cells was previously found to be four-fold higher than that for log-phase cells. Moreover, CHAPk-mediated lysis of stationary-phase cells was observed to be slower than for log-phase cultures. In the present study, we report the fusion of a 165 amino acid fragment containing CHAPk with a 136 amino acid fragment containing the cell-binding domain of the bacteriocin lysostaphin to create a chimeric enzyme designated CHAPk-SH3blys in the vector pET28a. The chimeric protein was employed in concentrations as low as 5 μg/mL, producing a reduction in turbidity in 7-day-old cultures, whereas the original CHAPk required at least 20 μg/mL to achieve this. Where 7-day old liquid cultures were used, the chimeric enzyme exhibited a 16-fold lower MIC than CHAPk. In terms of biofilm prevention, a concentration of 1 μg/mL of the chimeric enzyme was sufficient, whereas for CHAPk, 125 μg/mL was needed. Moreover, the chimeric enzyme exhibited total biofilm disruption when 5 μg/mL was employed in 4-h assays, whereas CHAPk could only partially disrupt the biofilms at this concentration. This study demonstrates that the cell-binding domain from lysostaphin can make the phage endolysin CHAPk more effective against sessile staphylococcal cells.
Highlights
Staphylococcus aureus is a common member of the human skin flora, being an opportunistic pathogen in clinical and healthcare settings [1]
Apart from demonstrating again how the cell-binding domain of lysostaphin can improve the lytic activity of an endolysin, we proved that the unique mechanism of this cell-binding domain [35,36] could make a phage endolysin more efficient against nondividing cultures and biofilms
Lysostaphin was found to be as active on 7-day old cultures as on log-phase cells, while CHAPk was not
Summary
Staphylococcus aureus is a common member of the human skin flora, being an opportunistic pathogen in clinical and healthcare settings [1]. These bacteria can cause a wide variety of diseases commonly involving the skin and soft tissue It can be associated with other clinical infectious syndromes, in which bacteria can be dividing very slowly or not dividing at all, including bacteremia, endocarditis, intravascular infections, pneumonia, osteomyelitis, septic arthritis, pyomyositis, necrotizing fasciitis, orbital infections, endophthalmitis, parotitis, staphylococcal toxinoses, urogenital infections, and central nervous system infections [2]. Many of these syndromes involve biofilm-associated infections, in which cells are in the stationary phase, presenting a higher tolerance to different antibiotics [4]. Cell surface-associated proteins are expected to play a role when cells switch into a persister state, as they form the first line of molecular interaction with substances in the environment [9]
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