Human anti-anthrax protective antigen neutralizing monoclonal antibodies derived from donors vaccinated with anthrax vaccine adsorbed

BACKGROUND: Potent anthrax toxin neutralizing human monoclonal antibodies were generated from peripheral blood lymphocytes obtained from Anthrax Vaccine Adsorbed (AVA) immune donors. The anti-anthrax toxin human monoclonal antibodies were evaluated for neutralization of anthrax lethal toxin in vivo...

Descripción completa

Detalles Bibliográficos
Autores principales: Sawada-Hirai, Ritsuko, Jiang, Ivy, Wang, Fei, Sun, Shu Man, Nedellec, Rebecca, Ruther, Paul, Alvarez, Alejandro, Millis, Diane, Morrow, Phillip R, Kang, Angray S
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2004
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC420254/
https://www.ncbi.nlm.nih.gov/pubmed/15140257
http://dx.doi.org/10.1186/1476-8518-2-5
_version_ 1782121472483917824
author Sawada-Hirai, Ritsuko
Jiang, Ivy
Wang, Fei
Sun, Shu Man
Nedellec, Rebecca
Ruther, Paul
Alvarez, Alejandro
Millis, Diane
Morrow, Phillip R
Kang, Angray S
author_facet Sawada-Hirai, Ritsuko
Jiang, Ivy
Wang, Fei
Sun, Shu Man
Nedellec, Rebecca
Ruther, Paul
Alvarez, Alejandro
Millis, Diane
Morrow, Phillip R
Kang, Angray S
author_sort Sawada-Hirai, Ritsuko
collection PubMed
description BACKGROUND: Potent anthrax toxin neutralizing human monoclonal antibodies were generated from peripheral blood lymphocytes obtained from Anthrax Vaccine Adsorbed (AVA) immune donors. The anti-anthrax toxin human monoclonal antibodies were evaluated for neutralization of anthrax lethal toxin in vivo in the Fisher 344 rat bolus toxin challenge model. METHODS: Human peripheral blood lymphocytes from AVA immunized donors were engrafted into severe combined immunodeficient (SCID) mice. Vaccination with anthrax protective antigen and lethal factor produced a significant increase in antigen specific human IgG in the mouse serum. The antibody producing lymphocytes were immortalized by hybridoma formation. The genes encoding the protective antibodies were rescued and stable cell lines expressing full-length human immunoglobulin were established. The antibodies were characterized by; (1) surface plasmon resonance; (2) inhibition of toxin in an in vitro mouse macrophage cell line protection assay and (3) in vivo in a Fischer 344 bolus lethal toxin challenge model. RESULTS: The range of antibodies generated were diverse with evidence of extensive hyper mutation, and all were of very high affinity for PA83~1 × 10(-10-11)M. Moreover all the antibodies were potent inhibitors of anthrax lethal toxin in vitro. A single IV dose of AVP-21D9 or AVP-22G12 was found to confer full protection with as little as 0.5× (AVP-21D9) and 1× (AVP-22G12) molar equivalence relative to the anthrax toxin in the rat challenge prophylaxis model. CONCLUSION: Here we describe a powerful technology to capture the recall antibody response to AVA vaccination and provide detailed molecular characterization of the protective human monoclonal antibodies. AVP-21D9, AVP-22G12 and AVP-1C6 protect rats from anthrax lethal toxin at low dose. Aglycosylated versions of the most potent antibodies are also protective in vivo, suggesting that lethal toxin neutralization is not Fc effector mediated. The protective effect of AVP-21D9 persists for at least one week in rats. These potent fully human anti-PA toxin-neutralizing antibodies are attractive candidates for prophylaxis and/or treatment against Anthrax Class A bioterrorism toxins.
format Text
id pubmed-420254
institution National Center for Biotechnology Information
language English
publishDate 2004
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-4202542004-06-06 Human anti-anthrax protective antigen neutralizing monoclonal antibodies derived from donors vaccinated with anthrax vaccine adsorbed Sawada-Hirai, Ritsuko Jiang, Ivy Wang, Fei Sun, Shu Man Nedellec, Rebecca Ruther, Paul Alvarez, Alejandro Millis, Diane Morrow, Phillip R Kang, Angray S J Immune Based Ther Vaccines Original Research BACKGROUND: Potent anthrax toxin neutralizing human monoclonal antibodies were generated from peripheral blood lymphocytes obtained from Anthrax Vaccine Adsorbed (AVA) immune donors. The anti-anthrax toxin human monoclonal antibodies were evaluated for neutralization of anthrax lethal toxin in vivo in the Fisher 344 rat bolus toxin challenge model. METHODS: Human peripheral blood lymphocytes from AVA immunized donors were engrafted into severe combined immunodeficient (SCID) mice. Vaccination with anthrax protective antigen and lethal factor produced a significant increase in antigen specific human IgG in the mouse serum. The antibody producing lymphocytes were immortalized by hybridoma formation. The genes encoding the protective antibodies were rescued and stable cell lines expressing full-length human immunoglobulin were established. The antibodies were characterized by; (1) surface plasmon resonance; (2) inhibition of toxin in an in vitro mouse macrophage cell line protection assay and (3) in vivo in a Fischer 344 bolus lethal toxin challenge model. RESULTS: The range of antibodies generated were diverse with evidence of extensive hyper mutation, and all were of very high affinity for PA83~1 × 10(-10-11)M. Moreover all the antibodies were potent inhibitors of anthrax lethal toxin in vitro. A single IV dose of AVP-21D9 or AVP-22G12 was found to confer full protection with as little as 0.5× (AVP-21D9) and 1× (AVP-22G12) molar equivalence relative to the anthrax toxin in the rat challenge prophylaxis model. CONCLUSION: Here we describe a powerful technology to capture the recall antibody response to AVA vaccination and provide detailed molecular characterization of the protective human monoclonal antibodies. AVP-21D9, AVP-22G12 and AVP-1C6 protect rats from anthrax lethal toxin at low dose. Aglycosylated versions of the most potent antibodies are also protective in vivo, suggesting that lethal toxin neutralization is not Fc effector mediated. The protective effect of AVP-21D9 persists for at least one week in rats. These potent fully human anti-PA toxin-neutralizing antibodies are attractive candidates for prophylaxis and/or treatment against Anthrax Class A bioterrorism toxins. BioMed Central 2004-05-12 /pmc/articles/PMC420254/ /pubmed/15140257 http://dx.doi.org/10.1186/1476-8518-2-5 Text en Copyright © 2004 Sawada-Hirai et al; licensee BioMed Central Ltd. This is an Open Access article: verbatim copying and redistribution of this article are permitted in all media for any purpose, provided this notice is preserved along with the article's original URL.
spellingShingle Original Research
Sawada-Hirai, Ritsuko
Jiang, Ivy
Wang, Fei
Sun, Shu Man
Nedellec, Rebecca
Ruther, Paul
Alvarez, Alejandro
Millis, Diane
Morrow, Phillip R
Kang, Angray S
Human anti-anthrax protective antigen neutralizing monoclonal antibodies derived from donors vaccinated with anthrax vaccine adsorbed
title Human anti-anthrax protective antigen neutralizing monoclonal antibodies derived from donors vaccinated with anthrax vaccine adsorbed
title_full Human anti-anthrax protective antigen neutralizing monoclonal antibodies derived from donors vaccinated with anthrax vaccine adsorbed
title_fullStr Human anti-anthrax protective antigen neutralizing monoclonal antibodies derived from donors vaccinated with anthrax vaccine adsorbed
title_full_unstemmed Human anti-anthrax protective antigen neutralizing monoclonal antibodies derived from donors vaccinated with anthrax vaccine adsorbed
title_short Human anti-anthrax protective antigen neutralizing monoclonal antibodies derived from donors vaccinated with anthrax vaccine adsorbed
title_sort human anti-anthrax protective antigen neutralizing monoclonal antibodies derived from donors vaccinated with anthrax vaccine adsorbed
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC420254/
https://www.ncbi.nlm.nih.gov/pubmed/15140257
http://dx.doi.org/10.1186/1476-8518-2-5
work_keys_str_mv AT sawadahirairitsuko humanantianthraxprotectiveantigenneutralizingmonoclonalantibodiesderivedfromdonorsvaccinatedwithanthraxvaccineadsorbed
AT jiangivy humanantianthraxprotectiveantigenneutralizingmonoclonalantibodiesderivedfromdonorsvaccinatedwithanthraxvaccineadsorbed
AT wangfei humanantianthraxprotectiveantigenneutralizingmonoclonalantibodiesderivedfromdonorsvaccinatedwithanthraxvaccineadsorbed
AT sunshuman humanantianthraxprotectiveantigenneutralizingmonoclonalantibodiesderivedfromdonorsvaccinatedwithanthraxvaccineadsorbed
AT nedellecrebecca humanantianthraxprotectiveantigenneutralizingmonoclonalantibodiesderivedfromdonorsvaccinatedwithanthraxvaccineadsorbed
AT rutherpaul humanantianthraxprotectiveantigenneutralizingmonoclonalantibodiesderivedfromdonorsvaccinatedwithanthraxvaccineadsorbed
AT alvarezalejandro humanantianthraxprotectiveantigenneutralizingmonoclonalantibodiesderivedfromdonorsvaccinatedwithanthraxvaccineadsorbed
AT millisdiane humanantianthraxprotectiveantigenneutralizingmonoclonalantibodiesderivedfromdonorsvaccinatedwithanthraxvaccineadsorbed
AT morrowphillipr humanantianthraxprotectiveantigenneutralizingmonoclonalantibodiesderivedfromdonorsvaccinatedwithanthraxvaccineadsorbed
AT kangangrays humanantianthraxprotectiveantigenneutralizingmonoclonalantibodiesderivedfromdonorsvaccinatedwithanthraxvaccineadsorbed

Ejemplares similares