Hyperimmune Targeting Staphylococcal Toxins Effectively Protect Against USA 300 MRSA Infection in Mouse Bacteremia and Pneumonia Models

Staphylococcus aureus has been acquiring multiple drug resistance and has evolved into superbugs such as Methicillin/Vancomycin-resistant S. aureus (MRSA/VRSA) and, consequently, is a major cause of nosocomial and community infections associated with high morbidity and mortality for which no FDA-app...

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Autores principales: Han, Xiaobing, Ortines, Roger, Mukherjee, Ipsita, Kanipakala, Tulasikumari, Kort, Thomas, Sherchand, Shardulendra P., Liao, Grant, Mednikov, Mark, Chenine, Agnes L., Aman, M. Javad, Nykiforuk, Cory L., Adhikari, Rajan P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9152286/
https://www.ncbi.nlm.nih.gov/pubmed/35655774
http://dx.doi.org/10.3389/fimmu.2022.893921
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author Han, Xiaobing
Ortines, Roger
Mukherjee, Ipsita
Kanipakala, Tulasikumari
Kort, Thomas
Sherchand, Shardulendra P.
Liao, Grant
Mednikov, Mark
Chenine, Agnes L.
Aman, M. Javad
Nykiforuk, Cory L.
Adhikari, Rajan P.
author_facet Han, Xiaobing
Ortines, Roger
Mukherjee, Ipsita
Kanipakala, Tulasikumari
Kort, Thomas
Sherchand, Shardulendra P.
Liao, Grant
Mednikov, Mark
Chenine, Agnes L.
Aman, M. Javad
Nykiforuk, Cory L.
Adhikari, Rajan P.
author_sort Han, Xiaobing
collection PubMed
description Staphylococcus aureus has been acquiring multiple drug resistance and has evolved into superbugs such as Methicillin/Vancomycin-resistant S. aureus (MRSA/VRSA) and, consequently, is a major cause of nosocomial and community infections associated with high morbidity and mortality for which no FDA-approved vaccines or biotherapeutics are available. Previous efforts targeting the surface-associated antigens have failed in clinical testing. Here, we generated hyperimmune products from sera in rabbits against six major S. aureus toxins targeted by an experimental vaccine (IBT-V02) and demonstrated significant efficacy for an anti-virulence passive immunization strategy. Extensive in vitro binding and neutralizing titers were analyzed against six extracellular toxins from individual animal sera. All IBT-V02 immunized animals elicited the maximum immune response upon the first boost dose against all pore-forming vaccine components, while for superantigen (SAgs) components of the vaccine, second and third doses of a boost were needed to reach a plateau in binding and toxin neutralizing titers. Importantly, both anti-staphylococcus hyperimmune products consisting of full-length IgG (IBT-V02-IgG) purified from the pooled sera and de-speciated F(ab’)(2) (IBT-V02-F(ab’)2) retained the binding and neutralizing titers against IBT-V02 target toxins. F(ab’)(2) also exhibited cross-neutralization titers against three leukotoxins (HlgAB, HlgCB, and LukED) and four SAgs (SEC1, SED, SEK, and SEQ) which were not part of IBT-V02. F(ab’)(2) also neutralized toxins in bacterial culture supernatant from major clinical strains of S. aureus. In vivo efficacy data generated in bacteremia and pneumonia models using USA300 S. aureus strain demonstrated dose-dependent protection by F(ab’)(2). These efficacy data confirmed the staphylococcal toxins as viable targets and support the further development effort of hyperimmune products as a potential adjunctive therapy for emergency uses against life-threatening S. aureus infections.
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spelling pubmed-91522862022-06-01 Hyperimmune Targeting Staphylococcal Toxins Effectively Protect Against USA 300 MRSA Infection in Mouse Bacteremia and Pneumonia Models Han, Xiaobing Ortines, Roger Mukherjee, Ipsita Kanipakala, Tulasikumari Kort, Thomas Sherchand, Shardulendra P. Liao, Grant Mednikov, Mark Chenine, Agnes L. Aman, M. Javad Nykiforuk, Cory L. Adhikari, Rajan P. Front Immunol Immunology Staphylococcus aureus has been acquiring multiple drug resistance and has evolved into superbugs such as Methicillin/Vancomycin-resistant S. aureus (MRSA/VRSA) and, consequently, is a major cause of nosocomial and community infections associated with high morbidity and mortality for which no FDA-approved vaccines or biotherapeutics are available. Previous efforts targeting the surface-associated antigens have failed in clinical testing. Here, we generated hyperimmune products from sera in rabbits against six major S. aureus toxins targeted by an experimental vaccine (IBT-V02) and demonstrated significant efficacy for an anti-virulence passive immunization strategy. Extensive in vitro binding and neutralizing titers were analyzed against six extracellular toxins from individual animal sera. All IBT-V02 immunized animals elicited the maximum immune response upon the first boost dose against all pore-forming vaccine components, while for superantigen (SAgs) components of the vaccine, second and third doses of a boost were needed to reach a plateau in binding and toxin neutralizing titers. Importantly, both anti-staphylococcus hyperimmune products consisting of full-length IgG (IBT-V02-IgG) purified from the pooled sera and de-speciated F(ab’)(2) (IBT-V02-F(ab’)2) retained the binding and neutralizing titers against IBT-V02 target toxins. F(ab’)(2) also exhibited cross-neutralization titers against three leukotoxins (HlgAB, HlgCB, and LukED) and four SAgs (SEC1, SED, SEK, and SEQ) which were not part of IBT-V02. F(ab’)(2) also neutralized toxins in bacterial culture supernatant from major clinical strains of S. aureus. In vivo efficacy data generated in bacteremia and pneumonia models using USA300 S. aureus strain demonstrated dose-dependent protection by F(ab’)(2). These efficacy data confirmed the staphylococcal toxins as viable targets and support the further development effort of hyperimmune products as a potential adjunctive therapy for emergency uses against life-threatening S. aureus infections. Frontiers Media S.A. 2022-05-17 /pmc/articles/PMC9152286/ /pubmed/35655774 http://dx.doi.org/10.3389/fimmu.2022.893921 Text en Copyright © 2022 Han, Ortines, Mukherjee, Kanipakala, Kort, Sherchand, Liao, Mednikov, Chenine, Aman, Nykiforuk and Adhikari https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Han, Xiaobing
Ortines, Roger
Mukherjee, Ipsita
Kanipakala, Tulasikumari
Kort, Thomas
Sherchand, Shardulendra P.
Liao, Grant
Mednikov, Mark
Chenine, Agnes L.
Aman, M. Javad
Nykiforuk, Cory L.
Adhikari, Rajan P.
Hyperimmune Targeting Staphylococcal Toxins Effectively Protect Against USA 300 MRSA Infection in Mouse Bacteremia and Pneumonia Models
title Hyperimmune Targeting Staphylococcal Toxins Effectively Protect Against USA 300 MRSA Infection in Mouse Bacteremia and Pneumonia Models
title_full Hyperimmune Targeting Staphylococcal Toxins Effectively Protect Against USA 300 MRSA Infection in Mouse Bacteremia and Pneumonia Models
title_fullStr Hyperimmune Targeting Staphylococcal Toxins Effectively Protect Against USA 300 MRSA Infection in Mouse Bacteremia and Pneumonia Models
title_full_unstemmed Hyperimmune Targeting Staphylococcal Toxins Effectively Protect Against USA 300 MRSA Infection in Mouse Bacteremia and Pneumonia Models
title_short Hyperimmune Targeting Staphylococcal Toxins Effectively Protect Against USA 300 MRSA Infection in Mouse Bacteremia and Pneumonia Models
title_sort hyperimmune targeting staphylococcal toxins effectively protect against usa 300 mrsa infection in mouse bacteremia and pneumonia models
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9152286/
https://www.ncbi.nlm.nih.gov/pubmed/35655774
http://dx.doi.org/10.3389/fimmu.2022.893921
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