SLPW: A Virulent Bacteriophage Targeting Methicillin-Resistant Staphylococcus aureus In vitro and In vivo

Wang, Zhaofei; Zheng, Panpan; Ji, Wenhui; Fu, Qiang; Wang, Hengan; Yan, Yaxian; Sun, Jianhe

doi:10.3389/fmicb.2016.00934

Cited by 66 publications

(82 citation statements)

References 39 publications

(38 reference statements)

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“…Results from this study show that the isolated phages were thermally active even at 40°C, 50°C, and 60°C and phages remaining viable up to 60°C after 90 min of incubation. The maximum infectivity was observed at 37°C, and the least infectivity was found at 60°C (Kęsik-Szeloch et al, 2013; Piracha et al, 2014; Wang et al, 2016).…”

Section: Discussionmentioning

confidence: 99%

Bacteriophages inhibit biofilms formed by multi-drug resistant bacteria isolated from septic wounds

Rani

Lakshmi

Praasad

2019

Preprint

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Section: Discussionmentioning

confidence: 99%

Bacteriophages inhibit biofilms formed by multi-drug resistant bacteria isolated from septic wounds

Rani

Lakshmi

Praasad

2019

Preprint

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“…Moreover, the release of filamentous Pf Pseudomonas phage was also associated with reduced lung injury and lower cytokine levels [39]. Wang et al demonstrated that phage therapy of uninfected mice does not alter the cytokine levels and significantly lowers those levels during therapy in infected mice, attenuating inflammation caused by S. aureus [40]. Similar findings were reported by Pabary et al, whose data indicate that phage administration reduced inflammation in a murine model of lung infection, lowering inflammatory cytokine and neutrophils levels in bronchoalveolar lavage fluid [41].…”

Section: • Phages and Inflammationmentioning

confidence: 99%

Phages and Immunomodulation

et al. 2017

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In the past years, the microbiome and its role in the pathophysiology of diseases have gained great interest. The progress of our knowledge in this field opens completely novel prospects for treating disorders, including those which are most challenging to medicine today. Of special interest are studies on the interactions of the microbiome with the immune system. Only recently has the presence of bacteriophages in the microbiome been highlighted, and their potential role in maintaining normal immunity has gained increasing attention. We summarize the available data pointing to the potential impact of phages in maintaining immunological homeostasis.

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“…As a potential alternative or complement to current antimicrobial agents (i.e., antibiotics), phage therapy has been drawing more and more attention as a strategy to treat MRSA infections (12,13). The potent bactericidal effect of phages is mainly attributed to their genome-encoded cell wall hydrolase, also called lysin, which exhibits a lethal effect by forming holes in the cell wall through peptidoglycan digestion (14).…”

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confidence: 99%

A Phage Lysin Fused to a Cell-Penetrating Peptide Kills Intracellular Methicillin-Resistant Staphylococcus aureus in Keratinocytes and Has Potential as a Treatment for Skin Infections in Mice

Wang

Kong

Liu

et al. 2018

Appl Environ Microbiol

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is the main pathogen that causes skin and skin structure infections and is able to survive and persist in keratinocytes of the epidermis. Since the evolution of multidrug-resistant bacteria, the use of phages and their lysins has presented a promising alternative approach to treatment. In this study, a cell wall hydrolase (also called lysin) derived from phage JD007 (JDlys) was identified. JDlys showed strong lytic activity against methicillin-resistant (MRSA) strains from different sources and of different multilocus sequence typing (MLST) types. Furthermore, a fusion protein consisting of a cell-penetrating peptide derived from the -activating transcription (Tat) factor fused to JDlys (CPP-JDlys) was used to kill MRSA bacteria causing intracellular infections. CPP-JDlys, in which the fusion of CPP to JDlys had almost no effect on the bacteriolytic activity of JDlys, was able to effectively eliminate intracellular MRSA bacteria and alleviate the inflammatory response and cell damage caused by MRSA. Specifically, CPP-JDlys was able to combat MRSA-induced murine skin infections and, consequently, expedite the healing of cutaneous abscesses. These data suggest that the novel antimicrobial CPP-JDlys may be a worthwhile candidate as a treatment for skin and skin structure infections caused by MRSA. is the main cause of skin and skin structure infections due to its ability to invade and survive in the epithelial barrier. Due to the overuse of antibiotics in humans and animals, has shown a high capacity for acquiring and accumulating mechanisms of resistance to antibiotics. Moreover, most antibiotics are usually limited in their ability to overcome the intracellular persistence of bacteria causing skin and skin structure infections. So, it is critical to seek a novel antimicrobial agent to eradicate intracellular In this study, a cell-penetrating peptide fused to lysin (CPP-JDlys) was engineered. Our results show that CPP-JDlys can enter keratinocytes and effectively eliminate intracellular MRSA. Meanwhile, experiments with mice revealed that CPP-JDlys efficiently inhibits the proliferation of MRSA in murine skin and thus shortens the course of wound healing. Our results indicate that the CPP-fused lysin has potential for use for the treatment of skin infections caused by MRSA.

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SLPW: A Virulent Bacteriophage Targeting Methicillin-Resistant Staphylococcus aureus In vitro and In vivo

Cited by 66 publications

References 39 publications

Bacteriophages inhibit biofilms formed by multi-drug resistant bacteria isolated from septic wounds

Bacteriophages inhibit biofilms formed by multi-drug resistant bacteria isolated from septic wounds

Phages and Immunomodulation

A Phage Lysin Fused to a Cell-Penetrating Peptide Kills Intracellular Methicillin-Resistant Staphylococcus aureus in Keratinocytes and Has Potential as a Treatment for Skin Infections in Mice

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