Protective Effect of Different Anti-Rabies Virus VHH Constructs against Rabies Disease in Mice

Rabies virus causes lethal brain infection in about 61000 people per year. Each year, tens of thousands of people receive anti-rabies prophylaxis with plasma-derived immunoglobulins and vaccine soon after exposure. Anti-rabies immunoglobulins are however expensive and have limited availability. VHH...

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Autores principales: Terryn, Sanne, Francart, Aurélie, Lamoral, Sophie, Hultberg, Anna, Rommelaere, Heidi, Wittelsberger, Angela, Callewaert, Filip, Stohr, Thomas, Meerschaert, Kris, Ottevaere, Ingrid, Stortelers, Catelijne, Vanlandschoot, Peter, Kalai, Michael, Van Gucht, Steven
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4210127/
https://www.ncbi.nlm.nih.gov/pubmed/25347556
http://dx.doi.org/10.1371/journal.pone.0109367
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author Terryn, Sanne
Francart, Aurélie
Lamoral, Sophie
Hultberg, Anna
Rommelaere, Heidi
Wittelsberger, Angela
Callewaert, Filip
Stohr, Thomas
Meerschaert, Kris
Ottevaere, Ingrid
Stortelers, Catelijne
Vanlandschoot, Peter
Kalai, Michael
Van Gucht, Steven
author_facet Terryn, Sanne
Francart, Aurélie
Lamoral, Sophie
Hultberg, Anna
Rommelaere, Heidi
Wittelsberger, Angela
Callewaert, Filip
Stohr, Thomas
Meerschaert, Kris
Ottevaere, Ingrid
Stortelers, Catelijne
Vanlandschoot, Peter
Kalai, Michael
Van Gucht, Steven
author_sort Terryn, Sanne
collection PubMed
description Rabies virus causes lethal brain infection in about 61000 people per year. Each year, tens of thousands of people receive anti-rabies prophylaxis with plasma-derived immunoglobulins and vaccine soon after exposure. Anti-rabies immunoglobulins are however expensive and have limited availability. VHH are the smallest antigen-binding functional fragments of camelid heavy chain antibodies, also called Nanobodies. The therapeutic potential of anti-rabies VHH was examined in a mouse model using intranasal challenge with a lethal dose of rabies virus. Anti-rabies VHH were administered directly into the brain or systemically, by intraperitoneal injection, 24 hours after virus challenge. Anti-rabies VHH were able to significantly prolong survival or even completely rescue mice from disease. The therapeutic effect depended on the dose, affinity and brain and plasma half-life of the VHH construct. Increasing the affinity by combining two VHH with a glycine-serine linker into bivalent or biparatopic constructs, increased the neutralizing potency to the picomolar range. Upon direct intracerebral administration, a dose as low as 33 µg of the biparatopic Rab-E8/H7 was still able to establish an anti-rabies effect. The effect of systemic treatment was significantly improved by increasing the half-life of Rab-E8/H7 through linkage with a third VHH targeted against albumin. Intraperitoneal treatment with 1.5 mg (2505 IU, 1 ml) of anti-albumin Rab-E8/H7 prolonged the median survival time from 9 to 15 days and completely rescued 43% of mice. For comparison, intraperitoneal treatment with the highest available dose of human anti-rabies immunoglobulins (65 mg, 111 IU, 1 ml) only prolonged survival by 2 days, without rescue. Overall, the therapeutic benefit seemed well correlated with the time of brain exposure and the plasma half-life of the used VHH construct. These results, together with the ease-of-production and superior thermal stability, render anti-rabies VHH into valuable candidates for development of alternative post exposure treatment drugs against rabies.
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spelling pubmed-42101272014-10-30 Protective Effect of Different Anti-Rabies Virus VHH Constructs against Rabies Disease in Mice Terryn, Sanne Francart, Aurélie Lamoral, Sophie Hultberg, Anna Rommelaere, Heidi Wittelsberger, Angela Callewaert, Filip Stohr, Thomas Meerschaert, Kris Ottevaere, Ingrid Stortelers, Catelijne Vanlandschoot, Peter Kalai, Michael Van Gucht, Steven PLoS One Research Article Rabies virus causes lethal brain infection in about 61000 people per year. Each year, tens of thousands of people receive anti-rabies prophylaxis with plasma-derived immunoglobulins and vaccine soon after exposure. Anti-rabies immunoglobulins are however expensive and have limited availability. VHH are the smallest antigen-binding functional fragments of camelid heavy chain antibodies, also called Nanobodies. The therapeutic potential of anti-rabies VHH was examined in a mouse model using intranasal challenge with a lethal dose of rabies virus. Anti-rabies VHH were administered directly into the brain or systemically, by intraperitoneal injection, 24 hours after virus challenge. Anti-rabies VHH were able to significantly prolong survival or even completely rescue mice from disease. The therapeutic effect depended on the dose, affinity and brain and plasma half-life of the VHH construct. Increasing the affinity by combining two VHH with a glycine-serine linker into bivalent or biparatopic constructs, increased the neutralizing potency to the picomolar range. Upon direct intracerebral administration, a dose as low as 33 µg of the biparatopic Rab-E8/H7 was still able to establish an anti-rabies effect. The effect of systemic treatment was significantly improved by increasing the half-life of Rab-E8/H7 through linkage with a third VHH targeted against albumin. Intraperitoneal treatment with 1.5 mg (2505 IU, 1 ml) of anti-albumin Rab-E8/H7 prolonged the median survival time from 9 to 15 days and completely rescued 43% of mice. For comparison, intraperitoneal treatment with the highest available dose of human anti-rabies immunoglobulins (65 mg, 111 IU, 1 ml) only prolonged survival by 2 days, without rescue. Overall, the therapeutic benefit seemed well correlated with the time of brain exposure and the plasma half-life of the used VHH construct. These results, together with the ease-of-production and superior thermal stability, render anti-rabies VHH into valuable candidates for development of alternative post exposure treatment drugs against rabies. Public Library of Science 2014-10-27 /pmc/articles/PMC4210127/ /pubmed/25347556 http://dx.doi.org/10.1371/journal.pone.0109367 Text en © 2014 Terryn et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Terryn, Sanne
Francart, Aurélie
Lamoral, Sophie
Hultberg, Anna
Rommelaere, Heidi
Wittelsberger, Angela
Callewaert, Filip
Stohr, Thomas
Meerschaert, Kris
Ottevaere, Ingrid
Stortelers, Catelijne
Vanlandschoot, Peter
Kalai, Michael
Van Gucht, Steven
Protective Effect of Different Anti-Rabies Virus VHH Constructs against Rabies Disease in Mice
title Protective Effect of Different Anti-Rabies Virus VHH Constructs against Rabies Disease in Mice
title_full Protective Effect of Different Anti-Rabies Virus VHH Constructs against Rabies Disease in Mice
title_fullStr Protective Effect of Different Anti-Rabies Virus VHH Constructs against Rabies Disease in Mice
title_full_unstemmed Protective Effect of Different Anti-Rabies Virus VHH Constructs against Rabies Disease in Mice
title_short Protective Effect of Different Anti-Rabies Virus VHH Constructs against Rabies Disease in Mice
title_sort protective effect of different anti-rabies virus vhh constructs against rabies disease in mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4210127/
https://www.ncbi.nlm.nih.gov/pubmed/25347556
http://dx.doi.org/10.1371/journal.pone.0109367
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