Multimeric bivalent immunogens from recombinant tetanus toxin HC fragment, synthetic hexasaccharides, and a glycopeptide adjuvant

Bongat, Aileen F. G.; Saksena, Rina; Adamo, Roberto; Fujimoto, Yukari; Shiokawa, Zenyu; Peterson, Dwight C.; Fukase, Koichi; Vann, Willie F.; Kòváč, Pavol

doi:10.1007/s10719-009-9259-4

Cited by 31 publications

(23 citation statements)

References 49 publications

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“…[13] Briefly, rTT–Hc (26.8 mg, 1 eq) was dissolved in pH 9 borate buffer (775 µ1) to form a clear solution. Ogawa hexasaccharide squarate [4] (5.5 mg, 6 eq) was added, and the clear solution was stirred at room temperature for 24 h. The mixture was dialyzed (eight times) against 10 mM ammonium carbonate using Millipore Amicon Ultra centrifugal filter device (30 kDa cut-off, 4°C).…”

Section: Methodsmentioning

confidence: 99%

“…[4,8,9] Using this method, they synthesized different carbohydrate-protein neoglycoconjugates by attachment of fragments of the O-specific polysaccharide of Vibrio cholerae O1 serotype Ogawa [9,10] and lnaba [11,12] to bovine serum albumin (BSA), and also the Ogawa hexasaccharide to the medically acceptable carrier, rTT–Hc. [13] These hapten–protein glycoconjugates are not only immunogenic but also offer protective capacity. [14–16] …”

Section: Introductionmentioning

confidence: 99%

“…[17,18] The toxoid form of this protein has also been used as a carrier protein for antigens in experimental carbohydrate-protein conjugate vaccines. [13] However, because the structure of TT is not fully characterized, the reproducibility of the synthesis of a well-defined polysaccharide–TT neoglycoconjugate vaccine was found to be poor. Consequently, the use of a fully characterized Hc fragment for the preparation of such vaccines is generally preferred.…”

Section: Introductionmentioning

confidence: 99%

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Mapping the glycation sites in the neoglycoconjugate from hexasaccharide antigen of Vibrio cholerae, serotype Ogawa and the recombinant tetanus toxin C‐fragment carrier

Jahouh

Vann³

et al. 2013

J. Mass Spectrom.

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We report herein the glycation sites in a vaccine candidate for cholera formed by conjugation of the synthetic hexasaccharide fragment of the O-specific polysaccharide of Vibrio cholerae, serotype Ogawa, to the recombinant tetanus toxin C-fragment (rTT–Hc) carrier. Matrix-assisted laser desorption/ionization time-of-flight mass spectrometry analysis of the vaccine revealed that it is composed of a mixture of neoglycoconjugates with carbohydrate:protein ratios of 1.9:1,3.0:1,4.0:1,4.9:1, 5.9:1, 6.9:1, 7.9:1 and 9.1:1. Liquid chromatography tandem mass spectrometry (LC-MS/MS) analysis of the tryptic and GluC V8 digests allowed identification of 12 glycation sites in the carbohydrate–protein neoglycoconjugate vaccine. The glycation sites are located exclusively on lysine (Lys) residues and are listed as follows: Lys 22, Lys 61, Lys 145, Lys 239, Lys 278, Lys 318, Lys 331, Lys 353, Lys 378, Lys 389, Lys 396 and Lys 437. Based on the 3-D representation of the rTT–Hc protein, all the glycation sites correspond to lysines located at the outer surface of the protein.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Mapping the glycation sites in the neoglycoconjugate from hexasaccharide antigen of Vibrio cholerae, serotype Ogawa and the recombinant tetanus toxin C‐fragment carrier

Jahouh

Vann³

et al. 2013

J. Mass Spectrom.

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“…The immunogenicity of the synthetic oligosaccharide fragment of the O-specific polysaccharide (O-PS) of Vibrio cholera O1, serotype Ogawa, conjugated to bovine serum albumin has been investigated in a mouse model [62,63]. A multimeric bivalent synthetic hexasaccharide fragment of the O-specific polysaccharide of Vibrio cholera O 1 , s e r o t y p e O g a w a , i n combination with Inaba:1 or a synthetic disaccharide tetrapeptide peptidoglycan fragment as adjuvant were prepared and conjugated to recombinant tetanus toxin H(C) fragment as protein carrier [64]. The immunogenicity of synthetic oligosaccharides mimicking the Oantigen of the Shigella flexneri 2a lipopolysaccharide (LPS) was also investigated in mice [65,66].…”

Section: Pneumococcal Synthetic Oligosaccharide-based Vaccinesmentioning

confidence: 99%

The Future of Synthetic Carbohydrate Vaccines: Immunological Studies on Streptococcus pneumoniae Type 14

Safari¹,

Rijkers²,

Snippe³

2012

The Complex World of Polysaccharides

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Additional information is available at the end of the chapter http://dx.doi.org/10.5772/48326 IntroductionStudies on synthetic carbohydrates to be used as potential vaccine candidates for polysaccharide encapsulated bacteria were started in the mid-1970s. They were the logical follow-up to studies being performed at that time on the immunogenicity of antigens composed of carrier proteins and synthetic hapten groups. Hapten-carrier complexes were first introduced in immunology by Karl Landsteiner in the early 1900s [1]. He discovered that (i) small organic molecules with a simple structure, such as phenyl arsonates and nitrophenyls, do not provoke antibodies by themselves, but (ii) if those molecules are attached covalently, by simple chemical reactions, to a protein carrier, then antibodies against those small organic molecules are evoked. Since their introduction, these haptencarrier complexes have become excellent tools to elucidate the role of different antigenreactive cells in the immune response [2]. The key players in this immunological process are thymus-derived T cells and bone marrow-derived B cells. The former group of lymphoid cells is responsible for various phenomena of cell-mediated immunity, e.g. delayed hypersensitivity, allograft-, and graft-versus-host reactions, and reacts with specific determinants on the carrier protein (T cell epitopes). The latter group of lymphoid cells (B cells) give rise to the precursors of antibody-secreting cells, and reacts with both the carrier protein and the synthetic haptenic determinants. This results in antibody formation to both the carrier and the hapten.The reason to apply the above concepts and techniques to carbohydrate antigens was to address an immunological problem: polysaccharide molecules are classified as so-called thymus-independent (TI) antigens, because they do not require T cells to induce an immune response of B cells. As a result, the antibodies formed are mainly of the IgM class and have aThe Complex World of Polysaccharides 618 low avidity. Moreover, no immunological memory is generated and the antigens are poorly immunogenic in infants. Latter characteristic has major implications for development of vaccines against polysaccharide encapsulated bacteria. It was hypothesized that by linking small carbohydrates (oligosaccharides) to a carrier protein, the immunogenic behavior would change to that of a thymus-dependent (TD) antigen. Therefore, the studies of both Goebel [3,4] and Campbell and Pappenheimer [5], who first isolated the antigenic determinant of Streptococcus pneumoniae type 3, were combined and extended. The hapteninhibition studies by Mage and Kabat [6] demonstrated that the antibody-combining site of type 3 pneumococcal polysaccharide consists of two to three cellobiuronic acid units. In the dextran-anti-dextran system extensively studied by Kabat and colleagues [7] the upper size limit of the antibody-combining site appeared to be a hexa-or heptasaccharide and the lower limit was estimated to be somewhat larger than a monosac...

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“…6,14,19,20 Especially, the Hc-C subdomains of BoNTs might be used as a carrier or component of a chimeric vaccine as fragments of TeNT. [21][22][23] Therefore, recombinant AHc-C as antigen or vectors for chimeric vaccines has been also explored in our laboratory. In the current study, the AHc-C was co-expressed in E. coli with Trx and its binding activity and immunogenic characterization were explored and compared with the AHc.…”

Section: Introductionmentioning

confidence: 99%

Binding activity and immunogenic characterization of recombinant C-terminal quarter and half of the heavy chain of botulinum neurotoxin serotype A

Yu¹,

Ma²,

Chen³

et al. 2011

Human Vaccines

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Multimeric bivalent immunogens from recombinant tetanus toxin HC fragment, synthetic hexasaccharides, and a glycopeptide adjuvant

Cited by 31 publications

References 49 publications

Mapping the glycation sites in the neoglycoconjugate from hexasaccharide antigen of Vibrio cholerae, serotype Ogawa and the recombinant tetanus toxin C‐fragment carrier

Mapping the glycation sites in the neoglycoconjugate from hexasaccharide antigen of Vibrio cholerae, serotype Ogawa and the recombinant tetanus toxin C‐fragment carrier

The Future of Synthetic Carbohydrate Vaccines: Immunological Studies on Streptococcus pneumoniae Type 14

Binding activity and immunogenic characterization of recombinant C-terminal quarter and half of the heavy chain of botulinum neurotoxin serotype A

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