Selection of a Novel Anti-Nicotine Vaccine: Influence of Antigen Design on Antibody Function in Mice

Anti-nicotine vaccines may aid smoking cessation via the induction of anti-nicotine antibodies (Ab) which reduce nicotine entering the brain, and hence the associated reward. Ab function depends on both the quantity (titer) and the quality (affinity) of the Ab. Anti-nicotine vaccines tested previous...

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Autores principales: Pryde, David C., Jones, Lyn H., Gervais, David P., Stead, David R., Blakemore, David C., Selby, Matthew D., Brown, Alan D., Coe, Jotham W., Badland, Matthew, Beal, David M., Glen, Rebecca, Wharton, Yvonne, Miller, Gavin J., White, Phil, Zhang, Ningli, Benoit, Michelle, Robertson, Karen, Merson, James R., Davis, Heather L., McCluskie, Michael J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3788104/
https://www.ncbi.nlm.nih.gov/pubmed/24098532
http://dx.doi.org/10.1371/journal.pone.0076557
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author Pryde, David C.
Jones, Lyn H.
Gervais, David P.
Stead, David R.
Blakemore, David C.
Selby, Matthew D.
Brown, Alan D.
Coe, Jotham W.
Badland, Matthew
Beal, David M.
Glen, Rebecca
Wharton, Yvonne
Miller, Gavin J.
White, Phil
Zhang, Ningli
Benoit, Michelle
Robertson, Karen
Merson, James R.
Davis, Heather L.
McCluskie, Michael J.
author_facet Pryde, David C.
Jones, Lyn H.
Gervais, David P.
Stead, David R.
Blakemore, David C.
Selby, Matthew D.
Brown, Alan D.
Coe, Jotham W.
Badland, Matthew
Beal, David M.
Glen, Rebecca
Wharton, Yvonne
Miller, Gavin J.
White, Phil
Zhang, Ningli
Benoit, Michelle
Robertson, Karen
Merson, James R.
Davis, Heather L.
McCluskie, Michael J.
author_sort Pryde, David C.
collection PubMed
description Anti-nicotine vaccines may aid smoking cessation via the induction of anti-nicotine antibodies (Ab) which reduce nicotine entering the brain, and hence the associated reward. Ab function depends on both the quantity (titer) and the quality (affinity) of the Ab. Anti-nicotine vaccines tested previously in clinical studies had poor efficacy despite high Ab titer, and this may be due to inadequate function if Ab of low affinity were induced. In this study, we designed and synthesized a series of novel nicotine-like haptens which were all linked to diphtheria toxoid (DT) as carrier, but which differed in the site of attachment of linker to nicotine, the nature of linker used, and the handle used to attach the hapten to DT. The resulting hapten conjugates were evaluated in a mouse model, using CpG (a TLR9 agonist) and aluminum hydroxide (Al(OH)(3)) as adjuvants, whereby Ab titers, affinity and function were evaluated using a radiolabeled nicotine challenge model. A series of additional linkers varying in length, rigidity and polarity were used with a single hapten to generate additional DT-conjugates, which were also tested in mice. Conjugates made with different haptens resulted in various titers of anti-nicotine Ab. Several haptens gave similarly high Ab titers, but among these, Ab affinity and hence function varied considerably. Linker also influenced Ab titer, affinity and function. These results demonstrate that immune responses induced in mice by nicotine-conjugate antigens are greatly influenced by hapten design including site of attachment of linker to nicotine, the nature of linker used, and the handle used to attach the hapten to DT. While both Ab titer and affinity contributed to function, affinity was more sensitive to antigen differences.
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spelling pubmed-37881042013-10-04 Selection of a Novel Anti-Nicotine Vaccine: Influence of Antigen Design on Antibody Function in Mice Pryde, David C. Jones, Lyn H. Gervais, David P. Stead, David R. Blakemore, David C. Selby, Matthew D. Brown, Alan D. Coe, Jotham W. Badland, Matthew Beal, David M. Glen, Rebecca Wharton, Yvonne Miller, Gavin J. White, Phil Zhang, Ningli Benoit, Michelle Robertson, Karen Merson, James R. Davis, Heather L. McCluskie, Michael J. PLoS One Research Article Anti-nicotine vaccines may aid smoking cessation via the induction of anti-nicotine antibodies (Ab) which reduce nicotine entering the brain, and hence the associated reward. Ab function depends on both the quantity (titer) and the quality (affinity) of the Ab. Anti-nicotine vaccines tested previously in clinical studies had poor efficacy despite high Ab titer, and this may be due to inadequate function if Ab of low affinity were induced. In this study, we designed and synthesized a series of novel nicotine-like haptens which were all linked to diphtheria toxoid (DT) as carrier, but which differed in the site of attachment of linker to nicotine, the nature of linker used, and the handle used to attach the hapten to DT. The resulting hapten conjugates were evaluated in a mouse model, using CpG (a TLR9 agonist) and aluminum hydroxide (Al(OH)(3)) as adjuvants, whereby Ab titers, affinity and function were evaluated using a radiolabeled nicotine challenge model. A series of additional linkers varying in length, rigidity and polarity were used with a single hapten to generate additional DT-conjugates, which were also tested in mice. Conjugates made with different haptens resulted in various titers of anti-nicotine Ab. Several haptens gave similarly high Ab titers, but among these, Ab affinity and hence function varied considerably. Linker also influenced Ab titer, affinity and function. These results demonstrate that immune responses induced in mice by nicotine-conjugate antigens are greatly influenced by hapten design including site of attachment of linker to nicotine, the nature of linker used, and the handle used to attach the hapten to DT. While both Ab titer and affinity contributed to function, affinity was more sensitive to antigen differences. Public Library of Science 2013-10-01 /pmc/articles/PMC3788104/ /pubmed/24098532 http://dx.doi.org/10.1371/journal.pone.0076557 Text en © 2013 Pryde 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
Pryde, David C.
Jones, Lyn H.
Gervais, David P.
Stead, David R.
Blakemore, David C.
Selby, Matthew D.
Brown, Alan D.
Coe, Jotham W.
Badland, Matthew
Beal, David M.
Glen, Rebecca
Wharton, Yvonne
Miller, Gavin J.
White, Phil
Zhang, Ningli
Benoit, Michelle
Robertson, Karen
Merson, James R.
Davis, Heather L.
McCluskie, Michael J.
Selection of a Novel Anti-Nicotine Vaccine: Influence of Antigen Design on Antibody Function in Mice
title Selection of a Novel Anti-Nicotine Vaccine: Influence of Antigen Design on Antibody Function in Mice
title_full Selection of a Novel Anti-Nicotine Vaccine: Influence of Antigen Design on Antibody Function in Mice
title_fullStr Selection of a Novel Anti-Nicotine Vaccine: Influence of Antigen Design on Antibody Function in Mice
title_full_unstemmed Selection of a Novel Anti-Nicotine Vaccine: Influence of Antigen Design on Antibody Function in Mice
title_short Selection of a Novel Anti-Nicotine Vaccine: Influence of Antigen Design on Antibody Function in Mice
title_sort selection of a novel anti-nicotine vaccine: influence of antigen design on antibody function in mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3788104/
https://www.ncbi.nlm.nih.gov/pubmed/24098532
http://dx.doi.org/10.1371/journal.pone.0076557
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