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Intravenous Vipera berus Venom-Specific Fab Fragments and Intramuscular Vipera ammodytes Venom-Specific F(ab’)(2) Fragments in Vipera ammodytes-Envenomed Patients

Vipera ammodytes (V. ammodytes) is the most venomous European viper. The aim of this study was to compare the clinical efficacy and pharmacokinetic values of intravenous Vipera berus venom-specific (paraspecific) Fab fragments (ViperaTAb) and intramuscular V. ammodytes venom-specific F(ab’)(2) fragm...

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Autores principales: Kurtović, Tihana, Karabuva, Svjetlana, Grenc, Damjan, Dobaja Borak, Mojca, Križaj, Igor, Lukšić, Boris, Halassy, Beata, Brvar, Miran
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8070888/
https://www.ncbi.nlm.nih.gov/pubmed/33919927
http://dx.doi.org/10.3390/toxins13040279
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author Kurtović, Tihana
Karabuva, Svjetlana
Grenc, Damjan
Dobaja Borak, Mojca
Križaj, Igor
Lukšić, Boris
Halassy, Beata
Brvar, Miran
author_facet Kurtović, Tihana
Karabuva, Svjetlana
Grenc, Damjan
Dobaja Borak, Mojca
Križaj, Igor
Lukšić, Boris
Halassy, Beata
Brvar, Miran
author_sort Kurtović, Tihana
collection PubMed
description Vipera ammodytes (V. ammodytes) is the most venomous European viper. The aim of this study was to compare the clinical efficacy and pharmacokinetic values of intravenous Vipera berus venom-specific (paraspecific) Fab fragments (ViperaTAb) and intramuscular V. ammodytes venom-specific F(ab’)(2) fragments (European viper venom antiserum, also called “Zagreb” antivenom) in V. ammodytes-envenomed patients. This was a prospective study of V. ammodytes-envenomed patients that were treated intravenously with ViperaTAb or intramuscularly with European viper venom antiserum that was feasible only due to the unique situation of an antivenom shortage. The highest venom concentration, survival, length of hospital stay and adverse reactions did not differ between the groups. Patients treated with intravenous Fab fragments were sicker, with significantly more rhabdomyolysis and neurotoxicity. The kinetics of Fab fragments after one or more intravenous applications matched better with the venom concentration in the early phase of envenomation compared to F(ab’)(2) fragments that were given intramuscularly only on admission. F(ab’)(2) fragments given intramuscularly had 25-fold longer apparent total body clearance and 14-fold longer elimination half-time compared to Fab fragments given intravenously (2 weeks vs. 24 h, respectively). In V. ammodytes-envenomed patients, the intramuscular use of specific F(ab’)(2) fragments resulted in a slow rise of antivenom serum concentration that demanded their early administration but without the need for additional doses for complete resolution of all clinical signs of envenomation. Intravenous use of paraspecific Fab fragments resulted in the immediate rise of antivenom serum concentration that enabled their use according to the clinical progress, but multiple doses might be needed for efficient therapy of thrombocytopenia due to venom recurrence, while the progression of rhabdomyolysis and neurotoxic effects of the venom could not be prevented.
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spelling pubmed-80708882021-04-26 Intravenous Vipera berus Venom-Specific Fab Fragments and Intramuscular Vipera ammodytes Venom-Specific F(ab’)(2) Fragments in Vipera ammodytes-Envenomed Patients Kurtović, Tihana Karabuva, Svjetlana Grenc, Damjan Dobaja Borak, Mojca Križaj, Igor Lukšić, Boris Halassy, Beata Brvar, Miran Toxins (Basel) Article Vipera ammodytes (V. ammodytes) is the most venomous European viper. The aim of this study was to compare the clinical efficacy and pharmacokinetic values of intravenous Vipera berus venom-specific (paraspecific) Fab fragments (ViperaTAb) and intramuscular V. ammodytes venom-specific F(ab’)(2) fragments (European viper venom antiserum, also called “Zagreb” antivenom) in V. ammodytes-envenomed patients. This was a prospective study of V. ammodytes-envenomed patients that were treated intravenously with ViperaTAb or intramuscularly with European viper venom antiserum that was feasible only due to the unique situation of an antivenom shortage. The highest venom concentration, survival, length of hospital stay and adverse reactions did not differ between the groups. Patients treated with intravenous Fab fragments were sicker, with significantly more rhabdomyolysis and neurotoxicity. The kinetics of Fab fragments after one or more intravenous applications matched better with the venom concentration in the early phase of envenomation compared to F(ab’)(2) fragments that were given intramuscularly only on admission. F(ab’)(2) fragments given intramuscularly had 25-fold longer apparent total body clearance and 14-fold longer elimination half-time compared to Fab fragments given intravenously (2 weeks vs. 24 h, respectively). In V. ammodytes-envenomed patients, the intramuscular use of specific F(ab’)(2) fragments resulted in a slow rise of antivenom serum concentration that demanded their early administration but without the need for additional doses for complete resolution of all clinical signs of envenomation. Intravenous use of paraspecific Fab fragments resulted in the immediate rise of antivenom serum concentration that enabled their use according to the clinical progress, but multiple doses might be needed for efficient therapy of thrombocytopenia due to venom recurrence, while the progression of rhabdomyolysis and neurotoxic effects of the venom could not be prevented. MDPI 2021-04-14 /pmc/articles/PMC8070888/ /pubmed/33919927 http://dx.doi.org/10.3390/toxins13040279 Text en © 2021 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
Kurtović, Tihana
Karabuva, Svjetlana
Grenc, Damjan
Dobaja Borak, Mojca
Križaj, Igor
Lukšić, Boris
Halassy, Beata
Brvar, Miran
Intravenous Vipera berus Venom-Specific Fab Fragments and Intramuscular Vipera ammodytes Venom-Specific F(ab’)(2) Fragments in Vipera ammodytes-Envenomed Patients
title Intravenous Vipera berus Venom-Specific Fab Fragments and Intramuscular Vipera ammodytes Venom-Specific F(ab’)(2) Fragments in Vipera ammodytes-Envenomed Patients
title_full Intravenous Vipera berus Venom-Specific Fab Fragments and Intramuscular Vipera ammodytes Venom-Specific F(ab’)(2) Fragments in Vipera ammodytes-Envenomed Patients
title_fullStr Intravenous Vipera berus Venom-Specific Fab Fragments and Intramuscular Vipera ammodytes Venom-Specific F(ab’)(2) Fragments in Vipera ammodytes-Envenomed Patients
title_full_unstemmed Intravenous Vipera berus Venom-Specific Fab Fragments and Intramuscular Vipera ammodytes Venom-Specific F(ab’)(2) Fragments in Vipera ammodytes-Envenomed Patients
title_short Intravenous Vipera berus Venom-Specific Fab Fragments and Intramuscular Vipera ammodytes Venom-Specific F(ab’)(2) Fragments in Vipera ammodytes-Envenomed Patients
title_sort intravenous vipera berus venom-specific fab fragments and intramuscular vipera ammodytes venom-specific f(ab’)(2) fragments in vipera ammodytes-envenomed patients
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8070888/
https://www.ncbi.nlm.nih.gov/pubmed/33919927
http://dx.doi.org/10.3390/toxins13040279
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