Literature DB >> 25671348

Intact reducing glycan promotes the specific immune response to lacto-N-neotetraose-BSA neoglycoconjugates.

Nina S Prasanphanich1, Xuezheng Song1, Jamie Heimburg-Molinaro1, Anthony E Luyai1, Yi Lasanajak1, Christopher E Cutler1, David F Smith1, Richard D Cummings1.   

Abstract

The mammalian immune system responds to eukaryotic glycan antigens during infections, cancer, and autoimmune disorders, but the immunological bases for such responses are unclear. Conjugate vaccines containing bacterial polysaccharides linked to carrier proteins (neoglycoconjugates) have proven successful, but these often contain repeating epitopes and the reducing end of the glycan is less important, unlike typical glycan determinants in eukaryotes, which are shorter in length and may include the reducing end. Here, we have compared the effects of two linkage methods, one that opens the ring at the reducing end of the glycan, and one that leaves the reducing end closed, on the glycan specificity of the vaccine response in rabbits and mice. We immunized rabbits and mice with bovine serum albumin (BSA) conjugates of synthetic open- and closed-ring forms (OR versus CR) of a simple tetrasaccharide lacto-N-neotetraose (LNnT, Galβ1-4GlcNAcβ1-3Galβ1-4Glc), and tested reactivity to the immunogens and several related glycans in both OR and CR versions on glycan microarrays. We found that in rabbits the immune response to the CR conjugate was directed toward the glycan, whereas the OR conjugate elicited antibodies to the reducing end of the glycan and linker region but not specifically to the glycan itself. Unexpectedly, mice did not generate a glycan-specific response to the CR conjugate. Our findings indicate that the reducing end of the sugar is crucial for generation of a glycan-specific response to some eukaryotic vaccine epitopes, and that there are species-specific differences in the ability to make a glycan-specific response to some glycoconjugates. These findings warrant further investigation with regard to rational design of glycoconjugate vaccines.

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Year:  2015        PMID: 25671348      PMCID: PMC4517824          DOI: 10.1021/acs.bioconjchem.5b00036

Source DB:  PubMed          Journal:  Bioconjug Chem        ISSN: 1043-1802            Impact factor:   4.774


  38 in total

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4.  Preparation and analysis of glycan microarrays.

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6.  Immunogenicity of synthetic conjugates of Lewis(y) oligosaccharide with proteins in mice: towards the design of anticancer vaccines.

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10.  A mechanism for glycoconjugate vaccine activation of the adaptive immune system and its implications for vaccine design.

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  8 in total

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2.  Efficient Synthesis of Heparinoid Bioconjugates for Tailoring FGF2 Activity at the Stem Cell-Matrix Interface.

Authors:  Greg W Trieger; Stephen Verespy; Philip L S M Gordts; Kamil Godula
Journal:  Bioconjug Chem       Date:  2019-02-08       Impact factor: 4.774

3.  Anthranilic Acid as a Versatile Fluorescent Tag and Linker for Functional Glycomics.

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Review 4.  Preparation of Complex Glycans From Natural Sources for Functional Study.

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Journal:  Front Chem       Date:  2020-07-03       Impact factor: 5.221

Review 5.  Glycan Microarrays as Chemical Tools for Identifying Glycan Recognition by Immune Proteins.

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6.  A Clickable Bioorthogonal Sydnone-Aglycone for the Facile Preparation of a Core 1 O-Glycan-Array.

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7.  Galectin Binding to Neo-Glycoproteins: LacDiNAc Conjugated BSA as Ligand for Human Galectin-3.

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8.  Immunogenicity and Induction of Functional Antibodies in Rabbits Immunized with a Trivalent Typhoid-Invasive Nontyphoidal Salmonella Glycoconjugate Formulation.

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Journal:  Molecules       Date:  2018-07-17       Impact factor: 4.411

  8 in total

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