Literature DB >> 16488517

Filamentous phage as an immunogenic carrier to elicit focused antibody responses against a synthetic peptide.

N E van Houten1, M B Zwick, A Menendez, J K Scott.   

Abstract

Filamentous bacteriophage are widely used as immunogenic carriers for "phage-displayed" recombinant peptides. Here we report that they are an effective immunogenic carrier for synthetic peptides. The f1.K phage was engineered to have an additional Lys residue near the N-terminus of the major coat protein, pVIII, so as to enhance access to chemical cross-linking agents. The dimeric synthetic peptide, B2.1, was conjugated to f1.K (f1.K/B2.1) in high copy number and compared as an immunogen to B2.1 conjugated to ovalbumin (OVA/B2.1) and to phage-displayed, recombinant B2.1 peptide. All immunogens were administered without adjuvant. The serum antibody titers were measured against: the peptide, the carrier, and, if appropriate, the cross-linker. All immunogens elicited anti-peptide antibody titers, with those elicited by OVA/B2.1 exceeding those by f1.K/B2.1; both titers were greater than that elicited by recombinant B2.1 phage. Comparison of the anti-peptide and anti-carrier antibody responses showed that f1.K/B2.1 elicited a more focused anti-peptide antibody response than OVA/B2.1. The anti-peptide antibody response against f1.K/B2.1 was optimized for the injection route, dose and adjuvant. Dose and adjuvant did not have a significant effect on anti-peptide antibody titers, but a change in injection route from intraperitoneal (IP) to subcutaneous (SC) enhanced anti-peptide antibody titers after seven immunizations. The optimized anti-peptide antibody response exceeded the anti-carrier one by 21-fold, compared to 0.07-fold elicited by OVA/B2.1. This indicates that phage as a carrier can focus the antibody response against the peptide. The results are discussed with respect to the advantages of phage as an alternative to traditional carrier proteins for synthetic peptides, carbohydrates and haptens, and to further improvements in phage as immunogenic carriers.

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Year:  2006        PMID: 16488517      PMCID: PMC1974903          DOI: 10.1016/j.vaccine.2006.01.001

Source DB:  PubMed          Journal:  Vaccine        ISSN: 0264-410X            Impact factor:   3.641


  54 in total

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3.  Phage-displayed T-cell epitope grafted into immunoglobulin heavy-chain complementarity-determining regions: an effective vaccine design tested in murine cysticercosis.

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4.  Identification of epitope regions recognized by tumor inhibitory and stimulatory anti-ErbB-2 monoclonal antibodies: implications for vaccine design.

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5.  Recognition of HIV-derived B and T cell epitopes displayed on filamentous phages.

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Journal:  Vaccine       Date:  1999-03-17       Impact factor: 3.641

6.  Molecular analysis of the autoantibody response in peptide-induced autoimmunity.

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10.  Conformational mimicry of a chlamydial neutralization epitope on filamentous phage.

Authors:  G Zhong; G P Smith; J Berry; R C Brunham
Journal:  J Biol Chem       Date:  1994-09-30       Impact factor: 5.157

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  31 in total

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2.  Exploring peptide mimics for the production of antibodies against discontinuous protein epitopes.

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Journal:  Cell Mol Life Sci       Date:  2010-03       Impact factor: 9.261

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6.  Cancer-associated CD43 glycoforms as target of immunotherapy.

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7.  A high throughput combinatorial library technique for identifying formalin-sensitive epitopes.

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8.  Phage display of functional, full-length human and viral membrane proteins.

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9.  Engineering filamentous phage carriers to improve focusing of antibody responses against peptides.

Authors:  Nienke E van Houten; Kevin A Henry; George P Smith; Jamie K Scott
Journal:  Vaccine       Date:  2010-01-05       Impact factor: 3.641

Review 10.  The ABC of clinical and experimental adjuvants--a brief overview.

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Journal:  Immunol Lett       Date:  2009-11-04       Impact factor: 3.685

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