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Fully Human Immunoglobulin G From Transchromosomic Bovines Treats Nonhuman Primates Infected With Ebola Virus Makona Isolate

Transchromosomic bovines (Tc-bovines) adaptively produce fully human polyclonal immunoglobulin (Ig)G antibodies after exposure to immunogenic antigen(s). The National Interagency Confederation for Biological Research and collaborators rapidly produced and then evaluated anti-Ebola virus IgG immunogl...

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Autores principales: Luke, Thomas, Bennett, Richard S, Gerhardt, Dawn M, Burdette, Tracey, Postnikova, Elena, Mazur, Steven, Honko, Anna N, Oberlander, Nicholas, Byrum, Russell, Ragland, Dan, St. Claire, Marisa, Janosko, Krisztina B, Smith, Gale, Glenn, Gregory, Hooper, Jay, Dye, John, Pal, Subhamoy, Bishop-Lilly, Kimberly A, Hamilton, Theron, Frey, Kenneth, Bollinger, Laura, Wada, Jiro, Wu, Hua, Jiao, Jin-an, Olinger, Gene G, Gunn, Bronwyn, Alter, Galit, Khurana, Surender, Hensley, Lisa E, Sullivan, Eddie, Jahrling, Peter B
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6249570/
https://www.ncbi.nlm.nih.gov/pubmed/30010950
http://dx.doi.org/10.1093/infdis/jiy377
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author Luke, Thomas
Bennett, Richard S
Gerhardt, Dawn M
Burdette, Tracey
Postnikova, Elena
Mazur, Steven
Honko, Anna N
Oberlander, Nicholas
Byrum, Russell
Ragland, Dan
St. Claire, Marisa
Janosko, Krisztina B
Smith, Gale
Glenn, Gregory
Hooper, Jay
Dye, John
Pal, Subhamoy
Bishop-Lilly, Kimberly A
Hamilton, Theron
Frey, Kenneth
Bollinger, Laura
Wada, Jiro
Wu, Hua
Jiao, Jin-an
Olinger, Gene G
Gunn, Bronwyn
Alter, Galit
Khurana, Surender
Hensley, Lisa E
Sullivan, Eddie
Jahrling, Peter B
author_facet Luke, Thomas
Bennett, Richard S
Gerhardt, Dawn M
Burdette, Tracey
Postnikova, Elena
Mazur, Steven
Honko, Anna N
Oberlander, Nicholas
Byrum, Russell
Ragland, Dan
St. Claire, Marisa
Janosko, Krisztina B
Smith, Gale
Glenn, Gregory
Hooper, Jay
Dye, John
Pal, Subhamoy
Bishop-Lilly, Kimberly A
Hamilton, Theron
Frey, Kenneth
Bollinger, Laura
Wada, Jiro
Wu, Hua
Jiao, Jin-an
Olinger, Gene G
Gunn, Bronwyn
Alter, Galit
Khurana, Surender
Hensley, Lisa E
Sullivan, Eddie
Jahrling, Peter B
author_sort Luke, Thomas
collection PubMed
description Transchromosomic bovines (Tc-bovines) adaptively produce fully human polyclonal immunoglobulin (Ig)G antibodies after exposure to immunogenic antigen(s). The National Interagency Confederation for Biological Research and collaborators rapidly produced and then evaluated anti-Ebola virus IgG immunoglobulins (collectively termed SAB-139) purified from Tc-bovine plasma after sequential hyperimmunization with an Ebola virus Makona isolate glycoprotein nanoparticle vaccine. SAB-139 was characterized by several in vitro production, research, and clinical level assays using wild-type Makona-C05 or recombinant virus/antigens from different Ebola virus variants. SAB-139 potently activates natural killer cells, monocytes, and peripheral blood mononuclear cells and has high-binding avidity demonstrated by surface plasmon resonance. SAB-139 has similar concentrations of galactose-α-1,3-galactose carbohydrates compared with human-derived intravenous Ig, and the IgG1 subclass antibody is predominant. All rhesus macaques infected with Ebola virus/H.sapiens-tc/GIN/2014/Makona-C05 and treated with sufficient SAB-139 at 1 day (n = 6) or 3 days (n = 6) postinfection survived versus 0% of controls. This study demonstrates that Tc-bovines can produce pathogen-specific human Ig to prevent and/or treat patients when an emerging infectious disease either threatens to or becomes an epidemic.
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spelling pubmed-62495702018-11-27 Fully Human Immunoglobulin G From Transchromosomic Bovines Treats Nonhuman Primates Infected With Ebola Virus Makona Isolate Luke, Thomas Bennett, Richard S Gerhardt, Dawn M Burdette, Tracey Postnikova, Elena Mazur, Steven Honko, Anna N Oberlander, Nicholas Byrum, Russell Ragland, Dan St. Claire, Marisa Janosko, Krisztina B Smith, Gale Glenn, Gregory Hooper, Jay Dye, John Pal, Subhamoy Bishop-Lilly, Kimberly A Hamilton, Theron Frey, Kenneth Bollinger, Laura Wada, Jiro Wu, Hua Jiao, Jin-an Olinger, Gene G Gunn, Bronwyn Alter, Galit Khurana, Surender Hensley, Lisa E Sullivan, Eddie Jahrling, Peter B J Infect Dis Supplement Articles Transchromosomic bovines (Tc-bovines) adaptively produce fully human polyclonal immunoglobulin (Ig)G antibodies after exposure to immunogenic antigen(s). The National Interagency Confederation for Biological Research and collaborators rapidly produced and then evaluated anti-Ebola virus IgG immunoglobulins (collectively termed SAB-139) purified from Tc-bovine plasma after sequential hyperimmunization with an Ebola virus Makona isolate glycoprotein nanoparticle vaccine. SAB-139 was characterized by several in vitro production, research, and clinical level assays using wild-type Makona-C05 or recombinant virus/antigens from different Ebola virus variants. SAB-139 potently activates natural killer cells, monocytes, and peripheral blood mononuclear cells and has high-binding avidity demonstrated by surface plasmon resonance. SAB-139 has similar concentrations of galactose-α-1,3-galactose carbohydrates compared with human-derived intravenous Ig, and the IgG1 subclass antibody is predominant. All rhesus macaques infected with Ebola virus/H.sapiens-tc/GIN/2014/Makona-C05 and treated with sufficient SAB-139 at 1 day (n = 6) or 3 days (n = 6) postinfection survived versus 0% of controls. This study demonstrates that Tc-bovines can produce pathogen-specific human Ig to prevent and/or treat patients when an emerging infectious disease either threatens to or becomes an epidemic. Oxford University Press 2018-12-15 2018-07-16 /pmc/articles/PMC6249570/ /pubmed/30010950 http://dx.doi.org/10.1093/infdis/jiy377 Text en © The Author(s) 2018. Published by Oxford University Press for the Infectious Diseases Society of America. http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs licence (http://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial reproduction and distribution of the work, in any medium, provided the original work is not altered or transformed in any way, and that the work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Supplement Articles
Luke, Thomas
Bennett, Richard S
Gerhardt, Dawn M
Burdette, Tracey
Postnikova, Elena
Mazur, Steven
Honko, Anna N
Oberlander, Nicholas
Byrum, Russell
Ragland, Dan
St. Claire, Marisa
Janosko, Krisztina B
Smith, Gale
Glenn, Gregory
Hooper, Jay
Dye, John
Pal, Subhamoy
Bishop-Lilly, Kimberly A
Hamilton, Theron
Frey, Kenneth
Bollinger, Laura
Wada, Jiro
Wu, Hua
Jiao, Jin-an
Olinger, Gene G
Gunn, Bronwyn
Alter, Galit
Khurana, Surender
Hensley, Lisa E
Sullivan, Eddie
Jahrling, Peter B
Fully Human Immunoglobulin G From Transchromosomic Bovines Treats Nonhuman Primates Infected With Ebola Virus Makona Isolate
title Fully Human Immunoglobulin G From Transchromosomic Bovines Treats Nonhuman Primates Infected With Ebola Virus Makona Isolate
title_full Fully Human Immunoglobulin G From Transchromosomic Bovines Treats Nonhuman Primates Infected With Ebola Virus Makona Isolate
title_fullStr Fully Human Immunoglobulin G From Transchromosomic Bovines Treats Nonhuman Primates Infected With Ebola Virus Makona Isolate
title_full_unstemmed Fully Human Immunoglobulin G From Transchromosomic Bovines Treats Nonhuman Primates Infected With Ebola Virus Makona Isolate
title_short Fully Human Immunoglobulin G From Transchromosomic Bovines Treats Nonhuman Primates Infected With Ebola Virus Makona Isolate
title_sort fully human immunoglobulin g from transchromosomic bovines treats nonhuman primates infected with ebola virus makona isolate
topic Supplement Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6249570/
https://www.ncbi.nlm.nih.gov/pubmed/30010950
http://dx.doi.org/10.1093/infdis/jiy377
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