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Safety Studies of Pneumococcal Endolysins Cpl-1 and Pal

Bacteriophage-derived endolysins have gained increasing attention as potent antimicrobial agents and numerous publications document the in vivo efficacy of these enzymes in various rodent models. However, little has been documented about their safety and toxicity profiles. Here, we present preclinic...

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Autores principales: Harhala, Marek, Nelson, Daniel C., Miernikiewicz, Paulina, Heselpoth, Ryan D., Brzezicka, Beata, Majewska, Joanna, Linden, Sara B., Shang, Xiaoran, Szymczak, Aleksander, Lecion, Dorota, Marek-Bukowiec, Karolina, Kłak, Marlena, Wojciechowicz, Bartosz, Lahutta, Karolina, Konieczny, Andrzej, Dąbrowska, Krystyna
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6266847/
https://www.ncbi.nlm.nih.gov/pubmed/30445722
http://dx.doi.org/10.3390/v10110638
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author Harhala, Marek
Nelson, Daniel C.
Miernikiewicz, Paulina
Heselpoth, Ryan D.
Brzezicka, Beata
Majewska, Joanna
Linden, Sara B.
Shang, Xiaoran
Szymczak, Aleksander
Lecion, Dorota
Marek-Bukowiec, Karolina
Kłak, Marlena
Wojciechowicz, Bartosz
Lahutta, Karolina
Konieczny, Andrzej
Dąbrowska, Krystyna
author_facet Harhala, Marek
Nelson, Daniel C.
Miernikiewicz, Paulina
Heselpoth, Ryan D.
Brzezicka, Beata
Majewska, Joanna
Linden, Sara B.
Shang, Xiaoran
Szymczak, Aleksander
Lecion, Dorota
Marek-Bukowiec, Karolina
Kłak, Marlena
Wojciechowicz, Bartosz
Lahutta, Karolina
Konieczny, Andrzej
Dąbrowska, Krystyna
author_sort Harhala, Marek
collection PubMed
description Bacteriophage-derived endolysins have gained increasing attention as potent antimicrobial agents and numerous publications document the in vivo efficacy of these enzymes in various rodent models. However, little has been documented about their safety and toxicity profiles. Here, we present preclinical safety and toxicity data for two pneumococcal endolysins, Pal and Cpl-1. Microarray, and gene profiling was performed on human macrophages and pharyngeal cells exposed to 0.5 µM of each endolysin for six hours and no change in gene expression was noted. Likewise, in mice injected with 15 mg/kg of each endolysin, no physical or behavioral changes were noted, pro-inflammatory cytokine levels remained constant, and there were no significant changes in the fecal microbiome. Neither endolysin caused complement activation via the classic pathway, the alternative pathway, or the mannose-binding lectin pathway. In cellular response assays, IgG levels in mice exposed to Pal or Cpl-1 gradually increased for the first 30 days post exposure, but IgE levels never rose above baseline, suggesting that hypersensitivity or allergic reaction is unlikely. Collectively, the safety and toxicity profiles of Pal and Cpl-1 support further preclinical studies.
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spelling pubmed-62668472018-12-07 Safety Studies of Pneumococcal Endolysins Cpl-1 and Pal Harhala, Marek Nelson, Daniel C. Miernikiewicz, Paulina Heselpoth, Ryan D. Brzezicka, Beata Majewska, Joanna Linden, Sara B. Shang, Xiaoran Szymczak, Aleksander Lecion, Dorota Marek-Bukowiec, Karolina Kłak, Marlena Wojciechowicz, Bartosz Lahutta, Karolina Konieczny, Andrzej Dąbrowska, Krystyna Viruses Article Bacteriophage-derived endolysins have gained increasing attention as potent antimicrobial agents and numerous publications document the in vivo efficacy of these enzymes in various rodent models. However, little has been documented about their safety and toxicity profiles. Here, we present preclinical safety and toxicity data for two pneumococcal endolysins, Pal and Cpl-1. Microarray, and gene profiling was performed on human macrophages and pharyngeal cells exposed to 0.5 µM of each endolysin for six hours and no change in gene expression was noted. Likewise, in mice injected with 15 mg/kg of each endolysin, no physical or behavioral changes were noted, pro-inflammatory cytokine levels remained constant, and there were no significant changes in the fecal microbiome. Neither endolysin caused complement activation via the classic pathway, the alternative pathway, or the mannose-binding lectin pathway. In cellular response assays, IgG levels in mice exposed to Pal or Cpl-1 gradually increased for the first 30 days post exposure, but IgE levels never rose above baseline, suggesting that hypersensitivity or allergic reaction is unlikely. Collectively, the safety and toxicity profiles of Pal and Cpl-1 support further preclinical studies. MDPI 2018-11-15 /pmc/articles/PMC6266847/ /pubmed/30445722 http://dx.doi.org/10.3390/v10110638 Text en © 2018 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Harhala, Marek
Nelson, Daniel C.
Miernikiewicz, Paulina
Heselpoth, Ryan D.
Brzezicka, Beata
Majewska, Joanna
Linden, Sara B.
Shang, Xiaoran
Szymczak, Aleksander
Lecion, Dorota
Marek-Bukowiec, Karolina
Kłak, Marlena
Wojciechowicz, Bartosz
Lahutta, Karolina
Konieczny, Andrzej
Dąbrowska, Krystyna
Safety Studies of Pneumococcal Endolysins Cpl-1 and Pal
title Safety Studies of Pneumococcal Endolysins Cpl-1 and Pal
title_full Safety Studies of Pneumococcal Endolysins Cpl-1 and Pal
title_fullStr Safety Studies of Pneumococcal Endolysins Cpl-1 and Pal
title_full_unstemmed Safety Studies of Pneumococcal Endolysins Cpl-1 and Pal
title_short Safety Studies of Pneumococcal Endolysins Cpl-1 and Pal
title_sort safety studies of pneumococcal endolysins cpl-1 and pal
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6266847/
https://www.ncbi.nlm.nih.gov/pubmed/30445722
http://dx.doi.org/10.3390/v10110638
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