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

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          Abstract

          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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          Shape of the relapse curve and long-term abstinence among untreated smokers.

          G. Hughes, Patricia J. Keely, Shelly Naud (2003)
          To describe the relapse curve and rate of long-term prolonged abstinence among smokers who try to quit without treatment. Systematic literature review. Cochrane Reviews, Dissertation Abstracts, Excerpt Medica, Medline, Psych Abstracts and US Center for Disease Control databases plus bibliographies of articles and requests of scientists. Prospective studies of self-quitters or studies that included a no-treatment control group. Two reviewers independently extracted data in a non-blind manner. The number of studies was too small and the data too heterogeneous for meta-analysis or other statistical techniques. There is a paucity of studies reporting relapse curves of self-quitters. The existing eight relapse curves from two studies of self-quitters and five no-treatment control groups indicate most relapse occurs in the first 8 days. These relapse curves were heterogeneous even when the final outcome was made similar. In terms of prolonged abstinence rates, a prior summary of 10 self-quitting studies, two other studies of self-quitters and three no-treatment control groups indicate 3-5% of self-quitters achieve prolonged abstinence for 6-12 month after a given quit attempt. More reports of relapse curves of self-quitters are needed. Smoking cessation interventions should focus on the first week of abstinence. Interventions that produce abstinence rates of 5-10% may be effective. Cessation studies should report relapse curves.
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            Squaramides: physical properties, synthesis and applications.

            Morgan H. Jones, R. Ian Storer, Caroline Aciro (2011)
            Squaramides are remarkable four-membered ring systems derived from squaric acid that are able to form up to four hydrogen bonds. A high affinity for hydrogen bonding is driven through a concomitant increase in aromaticity of the ring. This hydrogen bonding and aromatic switching, in combination with structural rigidity, have been exploited in many of the applications of squaramides. Substituted squaramides can be accessed via modular synthesis under relatively mild or aqueous conditions, making them ideal units for bioconjugation and supramolecular chemistry. In this tutorial review the fundamental electronic and structural properties of squaramides are explored to rationalise the geometry, conformation, reactivity and biological activity.
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              A Vaccine against Nicotine for Smoking Cessation: A Randomized Controlled Trial

              Jacques Cornuz, Susanne Zwahlen, Walter Felix Jungi (2008)
              Background Tobacco dependence is the leading cause of preventable death and disabilities worldwide and nicotine is the main substance responsible for the addiction to tobacco. A vaccine against nicotine was tested in a 6-month randomized, double blind phase II smoking cessation study in 341 smokers with a subsequent 6-month follow-up period. Methodology/Principal Findings 229 subjects were randomized to receive five intramuscular injections of the nicotine vaccine and 112 to receive placebo at monthly intervals. All subjects received individual behavioral smoking cessation counseling. The vaccine was safe, generally well tolerated and highly immunogenic, inducing a 100% antibody responder rate after the first injection. Point prevalence of abstinence at month 2 showed a statistically significant difference between subjects treated with Nicotine-Qβ (47.2%) and placebo (35.1%) (P = 0.036), but continuous abstinence between months 2 and 6 was not significantly different. However, in subgroup analysis of the per-protocol population, the third of subjects with highest antibody levels showed higher continuous abstinence from month 2 until month 6 (56.6%) than placebo treated participants (31.3%) (OR 2.9; P = 0.004) while medium and low antibody levels did not increase abstinence rates. After 12 month, the difference in continuous abstinence rate between subjects on placebo and those with high antibody response was maintained (difference 20.2%, P = 0.012). Conclusions Whereas Nicotine-Qβ did not significantly increase continuous abstinence rates in the intention-to-treat population, subgroup analyses of the per-protocol population suggest that such a vaccination against nicotine can significantly increase continuous abstinence rates in smokers when sufficiently high antibody levels are achieved. Immunotherapy might open a new avenue to the treatment of nicotine addiction. Trial Registration Swiss Medical Registry 2003DR2327; ClinicalTrials.gov NCT00369616
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                Author and article information

                Contributors
                Kim D. Janda: Role: Editor
                Journal
                Journal ID (nlm-ta): PLoS One
                Journal ID (iso-abbrev): PLoS ONE
                Journal ID (publisher-id): plos
                Journal ID (pmc): plosone
                Title: PLoS ONE
                Publisher: Public Library of Science (San Francisco, USA )
                ISSN (Electronic): 1932-6203
                Publication date Collection: 2013
                Publication date (Electronic): 1 October 2013
                Volume: 8
                Issue: 10
                Electronic Location Identifier: e76557
                Affiliations
                [1 ]Pfizer Worldwide Medicinal Chemistry, Cambridge, United Kingdom
                [2 ]Pfizer Worldwide Medicinal Chemistry, BioTherapeutics Chemistry, Cambridge, Massachusetts, United States of America
                [3 ]Pfizer Vaccine Research, La Jolla, California, United States of America
                [4 ]Pfizer Worldwide Medicinal Chemistry, Groton, Connecticut, United States of America
                [5 ]Pfizer Vaccine Research, Ottawa, Ontario, Canada
                [6 ]Peakdale Molecular Ltd, Chapel-en-le-Frith, United Kingdom
                [7 ]Pfizer Chemical Research and Development, Sandwich, United Kingdom
                The Scripps Research Institute, United States of America
                Author notes

                Competing Interests: All authors were either under paid employment or consultancy agreement with Pfizer at the time of these studies. Co-authors YW, GM, and RG were employed by Peakdale Molecular Ltd at the time of these studies. Pfizer is pursuing patents and product development on compounds that are mentioned in this paper. There are no marketed products to declare. DP, LJ, DG, DS, D. Blakemore, MS, AB, JC, M. Badland, D. Beal, PW, NZ, M. Benoit, KR, JM, HD and MM all hold shares or share options of Pfizer. This does not alter the authors' adherence to all the PLOS ONE policies on sharing data and materials.

                Conceived and designed the experiments: DP LJ DG DS D. Blakemore MS AB JC M. Badland D. Beal RG YW GM PW NZ M. Benoit KR JM HD MM. Performed the experiments: DP LJ DG DS D. Blakemore MS M. Badland D. Beal RG YW GM NZ M. Benoit KR. Analyzed the data: DP LJ DG DS D. Blakemore MS M. Badland D. Beal PW NZ M. Benoit KR JM HD MM. Contributed reagents/materials/analysis tools: DP LJ DG DS D. Blakemore MS M. Badland D. Beal RG YW GM NZ M. Benoit KR. Wrote the manuscript: DP LJ DG DS D. Blakemore MS AB JC M. Badland D. Beal RG YW GM PW NZ M. Benoit KR JM HD MM.

                [¤a]

                Current address: Health Protection Agency, Process and Analytical Development Group, Porton Down, Salisbury, United Kingdom

                [¤b]

                Current address: UCB Celltech, Slough, Berkshire, United Kingdom

                [¤c]

                Current address: School of Biosciences, University of Kent, Canterbury, Kent, United Kingdom

                [¤d]

                Current address: C-Tech Innovation Ltd, Chester, United Kingdom

                [¤e]

                Current address: School of Chemistry, the University of Manchester, Manchester, United Kingdom

                Article
                Publisher ID: PONE-D-13-16465
                DOI: 10.1371/journal.pone.0076557
                PMC ID: 3788104
                SO-VID: 996a750c-dead-4d49-a91c-8d902d8dcf56
                Copyright statement: Copyright @ 2013
                License:

                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 credited.

                History
                Date received : 24 April 2013
                Date accepted : 25 August 2013
                Funding
                No current external funding sources for this study.
                Categories
                Subject: Research Article

                ScienceOpen disciplines: Uncategorized
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