Exploring the Utility of Recombinant Snake Venom Serine Protease Toxins as Immunogens for Generating Experimental Snakebite Antivenoms

Snakebite is a neglected tropical disease that causes high rates of global mortality and morbidity. Although snakebite can cause a variety of pathologies in victims, haemotoxic effects are particularly common and are typically characterised by haemorrhage and/or venom-induced consumption coagulopath...

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Autores principales: Alomran, Nessrin, Blundell, Patricia, Alsolaiss, Jaffer, Crittenden, Edouard, Ainsworth, Stuart, Dawson, Charlotte A., Edge, Rebecca J., Hall, Steven R., Harrison, Robert A., Wilkinson, Mark C., Menzies, Stefanie K., Casewell, Nicholas R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9319908/
https://www.ncbi.nlm.nih.gov/pubmed/35878181
http://dx.doi.org/10.3390/toxins14070443
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author Alomran, Nessrin
Blundell, Patricia
Alsolaiss, Jaffer
Crittenden, Edouard
Ainsworth, Stuart
Dawson, Charlotte A.
Edge, Rebecca J.
Hall, Steven R.
Harrison, Robert A.
Wilkinson, Mark C.
Menzies, Stefanie K.
Casewell, Nicholas R.
author_facet Alomran, Nessrin
Blundell, Patricia
Alsolaiss, Jaffer
Crittenden, Edouard
Ainsworth, Stuart
Dawson, Charlotte A.
Edge, Rebecca J.
Hall, Steven R.
Harrison, Robert A.
Wilkinson, Mark C.
Menzies, Stefanie K.
Casewell, Nicholas R.
author_sort Alomran, Nessrin
collection PubMed
description Snakebite is a neglected tropical disease that causes high rates of global mortality and morbidity. Although snakebite can cause a variety of pathologies in victims, haemotoxic effects are particularly common and are typically characterised by haemorrhage and/or venom-induced consumption coagulopathy. Despite polyclonal antibody-based antivenoms being the mainstay life-saving therapy for snakebite, they are associated with limited cross-snake species efficacy, as there is often extensive toxin variation between snake venoms, including those used as immunogens for antivenom production. This restricts the therapeutic utility of any antivenom to certain geographical regions. In this study, we explored the feasibility of using recombinantly expressed toxins as immunogens to stimulate focused, pathology-specific, antibodies in order to broadly counteract specific toxins associated with snakebite envenoming. Three snake venom serine proteases (SVSP) toxins, sourced from geographically diverse and medically important viper snake venoms, were successfully expressed in HEK293F mammalian cells and used for murine immunisation. Analyses of the resulting antibody responses revealed that ancrod and RVV-V stimulated the strongest immune responses, and that experimental antivenoms directed against these recombinant SVSP toxins, and a mixture of the three different immunogens, extensively recognised and exhibited immunological binding towards a variety of native snake venoms. While the experimental antivenoms showed some reduction in abnormal clotting parameters stimulated by the toxin immunogens and crude venom, specifically reducing the depletion of fibrinogen levels and prolongation of prothrombin times, fibrinogen degradation experiments revealed that they broadly protected against venom- and toxin-induced fibrinogenolytic functional activities. Overall, our findings further strengthen the case for the use of recombinant venom toxins as supplemental immunogens to stimulate focused and desirable antibody responses capable of neutralising venom-induced pathological effects, and therefore potentially circumventing some of the limitations associated with current snakebite therapies.
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spelling pubmed-93199082022-07-27 Exploring the Utility of Recombinant Snake Venom Serine Protease Toxins as Immunogens for Generating Experimental Snakebite Antivenoms Alomran, Nessrin Blundell, Patricia Alsolaiss, Jaffer Crittenden, Edouard Ainsworth, Stuart Dawson, Charlotte A. Edge, Rebecca J. Hall, Steven R. Harrison, Robert A. Wilkinson, Mark C. Menzies, Stefanie K. Casewell, Nicholas R. Toxins (Basel) Article Snakebite is a neglected tropical disease that causes high rates of global mortality and morbidity. Although snakebite can cause a variety of pathologies in victims, haemotoxic effects are particularly common and are typically characterised by haemorrhage and/or venom-induced consumption coagulopathy. Despite polyclonal antibody-based antivenoms being the mainstay life-saving therapy for snakebite, they are associated with limited cross-snake species efficacy, as there is often extensive toxin variation between snake venoms, including those used as immunogens for antivenom production. This restricts the therapeutic utility of any antivenom to certain geographical regions. In this study, we explored the feasibility of using recombinantly expressed toxins as immunogens to stimulate focused, pathology-specific, antibodies in order to broadly counteract specific toxins associated with snakebite envenoming. Three snake venom serine proteases (SVSP) toxins, sourced from geographically diverse and medically important viper snake venoms, were successfully expressed in HEK293F mammalian cells and used for murine immunisation. Analyses of the resulting antibody responses revealed that ancrod and RVV-V stimulated the strongest immune responses, and that experimental antivenoms directed against these recombinant SVSP toxins, and a mixture of the three different immunogens, extensively recognised and exhibited immunological binding towards a variety of native snake venoms. While the experimental antivenoms showed some reduction in abnormal clotting parameters stimulated by the toxin immunogens and crude venom, specifically reducing the depletion of fibrinogen levels and prolongation of prothrombin times, fibrinogen degradation experiments revealed that they broadly protected against venom- and toxin-induced fibrinogenolytic functional activities. Overall, our findings further strengthen the case for the use of recombinant venom toxins as supplemental immunogens to stimulate focused and desirable antibody responses capable of neutralising venom-induced pathological effects, and therefore potentially circumventing some of the limitations associated with current snakebite therapies. MDPI 2022-06-29 /pmc/articles/PMC9319908/ /pubmed/35878181 http://dx.doi.org/10.3390/toxins14070443 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/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 (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Alomran, Nessrin
Blundell, Patricia
Alsolaiss, Jaffer
Crittenden, Edouard
Ainsworth, Stuart
Dawson, Charlotte A.
Edge, Rebecca J.
Hall, Steven R.
Harrison, Robert A.
Wilkinson, Mark C.
Menzies, Stefanie K.
Casewell, Nicholas R.
Exploring the Utility of Recombinant Snake Venom Serine Protease Toxins as Immunogens for Generating Experimental Snakebite Antivenoms
title Exploring the Utility of Recombinant Snake Venom Serine Protease Toxins as Immunogens for Generating Experimental Snakebite Antivenoms
title_full Exploring the Utility of Recombinant Snake Venom Serine Protease Toxins as Immunogens for Generating Experimental Snakebite Antivenoms
title_fullStr Exploring the Utility of Recombinant Snake Venom Serine Protease Toxins as Immunogens for Generating Experimental Snakebite Antivenoms
title_full_unstemmed Exploring the Utility of Recombinant Snake Venom Serine Protease Toxins as Immunogens for Generating Experimental Snakebite Antivenoms
title_short Exploring the Utility of Recombinant Snake Venom Serine Protease Toxins as Immunogens for Generating Experimental Snakebite Antivenoms
title_sort exploring the utility of recombinant snake venom serine protease toxins as immunogens for generating experimental snakebite antivenoms
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9319908/
https://www.ncbi.nlm.nih.gov/pubmed/35878181
http://dx.doi.org/10.3390/toxins14070443
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