Biosynthetic Oligoclonal Antivenom (BOA) for Snakebite and Next-Generation Treatments for Snakebite Victims

Snakebite envenoming is a neglected tropical disease that each year claims the lives of 80,000⁻140,000 victims worldwide. The only effective treatment against envenoming involves intravenous administration of antivenoms that comprise antibodies that have been isolated from the plasma of im...

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Main Authors: R. Manjunatha Kini, Sachdev S. Sidhu, Andreas Hougaard Laustsen
Format: Article
Language:English
Published: MDPI AG 2018-12-01
Series:Toxins
Subjects:
Online Access:https://www.mdpi.com/2072-6651/10/12/534
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spelling doaj-b5d129fc4dc847ab8455ed15ed395da72020-11-24T21:23:13ZengMDPI AGToxins2072-66512018-12-01101253410.3390/toxins10120534toxins10120534Biosynthetic Oligoclonal Antivenom (BOA) for Snakebite and Next-Generation Treatments for Snakebite VictimsR. Manjunatha Kini0Sachdev S. Sidhu1Andreas Hougaard Laustsen2Department of Biological Sciences, National University of Singapore, 14 Science Drive 4, Singapore 117543, SingaporeDepartment of Molecular Genetics, The Donnelly Centre, University of Toronto, 160 College Street, Toronto, ON M5S 3E1, CanadaDepartment of Biotechnology and Biomedicine, Technical University of Denmark, DK-2800 Kongens Lyngby, DenmarkSnakebite envenoming is a neglected tropical disease that each year claims the lives of 80,000⁻140,000 victims worldwide. The only effective treatment against envenoming involves intravenous administration of antivenoms that comprise antibodies that have been isolated from the plasma of immunized animals, typically horses. The drawbacks of such conventional horse-derived antivenoms include their propensity for causing allergenic adverse reactions due to their heterologous and foreign nature, an inability to effectively neutralize toxins in distal tissue, a low content of toxin-neutralizing antibodies, and a complex manufacturing process that is dependent on husbandry and procurement of snake venoms. In recent years, an opportunity to develop a fundamentally novel type of antivenom has presented itself. By using modern antibody discovery strategies, such as phage display selection, and repurposing small molecule enzyme inhibitors, next-generation antivenoms that obviate the drawbacks of existing plasma-derived antivenoms could be developed. This article describes the conceptualization of a novel therapeutic development strategy for biosynthetic oligoclonal antivenom (BOA) for snakebites based on recombinantly expressed oligoclonal mixtures of human monoclonal antibodies, possibly combined with repurposed small molecule enzyme inhibitors.https://www.mdpi.com/2072-6651/10/12/534snakebite envenomingneglected tropical diseasesantivenomnext-generation antivenomrecombinant antivenomsmall molecule inhibitors
collection DOAJ
language English
format Article
sources DOAJ
author R. Manjunatha Kini
Sachdev S. Sidhu
Andreas Hougaard Laustsen
spellingShingle R. Manjunatha Kini
Sachdev S. Sidhu
Andreas Hougaard Laustsen
Biosynthetic Oligoclonal Antivenom (BOA) for Snakebite and Next-Generation Treatments for Snakebite Victims
Toxins
snakebite envenoming
neglected tropical diseases
antivenom
next-generation antivenom
recombinant antivenom
small molecule inhibitors
author_facet R. Manjunatha Kini
Sachdev S. Sidhu
Andreas Hougaard Laustsen
author_sort R. Manjunatha Kini
title Biosynthetic Oligoclonal Antivenom (BOA) for Snakebite and Next-Generation Treatments for Snakebite Victims
title_short Biosynthetic Oligoclonal Antivenom (BOA) for Snakebite and Next-Generation Treatments for Snakebite Victims
title_full Biosynthetic Oligoclonal Antivenom (BOA) for Snakebite and Next-Generation Treatments for Snakebite Victims
title_fullStr Biosynthetic Oligoclonal Antivenom (BOA) for Snakebite and Next-Generation Treatments for Snakebite Victims
title_full_unstemmed Biosynthetic Oligoclonal Antivenom (BOA) for Snakebite and Next-Generation Treatments for Snakebite Victims
title_sort biosynthetic oligoclonal antivenom (boa) for snakebite and next-generation treatments for snakebite victims
publisher MDPI AG
series Toxins
issn 2072-6651
publishDate 2018-12-01
description Snakebite envenoming is a neglected tropical disease that each year claims the lives of 80,000⁻140,000 victims worldwide. The only effective treatment against envenoming involves intravenous administration of antivenoms that comprise antibodies that have been isolated from the plasma of immunized animals, typically horses. The drawbacks of such conventional horse-derived antivenoms include their propensity for causing allergenic adverse reactions due to their heterologous and foreign nature, an inability to effectively neutralize toxins in distal tissue, a low content of toxin-neutralizing antibodies, and a complex manufacturing process that is dependent on husbandry and procurement of snake venoms. In recent years, an opportunity to develop a fundamentally novel type of antivenom has presented itself. By using modern antibody discovery strategies, such as phage display selection, and repurposing small molecule enzyme inhibitors, next-generation antivenoms that obviate the drawbacks of existing plasma-derived antivenoms could be developed. This article describes the conceptualization of a novel therapeutic development strategy for biosynthetic oligoclonal antivenom (BOA) for snakebites based on recombinantly expressed oligoclonal mixtures of human monoclonal antibodies, possibly combined with repurposed small molecule enzyme inhibitors.
topic snakebite envenoming
neglected tropical diseases
antivenom
next-generation antivenom
recombinant antivenom
small molecule inhibitors
url https://www.mdpi.com/2072-6651/10/12/534
work_keys_str_mv AT rmanjunathakini biosyntheticoligoclonalantivenomboaforsnakebiteandnextgenerationtreatmentsforsnakebitevictims
AT sachdevssidhu biosyntheticoligoclonalantivenomboaforsnakebiteandnextgenerationtreatmentsforsnakebitevictims
AT andreashougaardlaustsen biosyntheticoligoclonalantivenomboaforsnakebiteandnextgenerationtreatmentsforsnakebitevictims
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