Abstract

Human salivary mucins protect the oral tissues by providing a physical barrier to environmental agents, possessing viscoelastic properties essential for lubrication and participating in the modulation of the oral flora. These properties are dependent, in large part, on the mucin's O- linked oligosaccharides and the peptide moieties surrounding the glycopeptide linkage. Several central questions regarding the patterns of O-glycosylation remain to be understood for the prediction of the influence of O-glycosylation patterns on the mucin's biological function(s). First, a consensus sequence akin to the Asn-Xxx-Thr/Ser motif for N-glycosylation has not been identified and hence the factor(s) that determine which Ser and Thr residues are O-glycosylated are not known. Second, factors that determine the final structure of the O- linked units and their distribution along the peptide backbone are not understood. Our hypothesis is that the patterns of MG2 O-glycosylation are important determinants in biological activity. Importantly, these patterns are influenced by the conformation adopted by O-linked units and adjacent or flanking peptide sequences. For example, mucin's interaction with certain bacteria (e.g. viridans streptococci and Actinomyces viscosus) involves stereochemical recognition between mucin's O-linked oligosaccharides and bacterial adhesins. Our long range goal is to obtain a detailed understanding of human salivary mucin O- glycosylation patterns for the eventual production by design and mimicry of bioactive mucin analogs to be used as saliva substitutes. To achieve this goal, we will use MG2 as a model since its structure has been well characterized in our laboratory. Our approach to this problem is biphasic in nature. In the first phase, we will synthesize MG2 glycopeptides present in the tandem repeat with varying levels of O- linked units. The bioactivity of these glycopeptides will be compared to native MG2 to assess the role of glycosylation patterns on biological function. In the later phase, a complete understanding of the conformational dynamics of these bioactive glycopeptides will be carried out. The data obtained will then be used to design mucin peptides (e.g. glycomimetics) that mimic the conformation and biological properties of bioactive glycopeptides.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Program Projects (P01)
Project #
5P01DE007585-08
Application #
5210094
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
8
Fiscal Year
1996
Total Cost
Indirect Cost

  Publications

Satyanarayana, J; Gururaja, T L; Narasimhamurthy, S et al. (2001) Synthesis and conformational features of human salivary mucin C-terminal derived peptide epitope carrying Thomsen-Friedenreich antigen: implications for its role in self-association. Biopolymers 58:500-10
Narasimhamurthy, S; Naganagowda, G A; Janagani, S et al. (2000) Solution structure of O-glycosylated C-terminal leucine zipper domain of human salivary mucin (MUC7). J Biomol Struct Dyn 18:145-54
Tseng, C C; Tseng, C P; Levine, M J et al. (2000) Differential effect toward inhibition of papain and cathepsin C by recombinant human salivary cystatin SN and its variants produced by a baculovirus system. Arch Biochem Biophys 380:133-40
Satyanarayana, J; Situ, H; Narasimhamurthy, S et al. (2000) Divergent solid-phase synthesis and candidacidal activity of MUC7 D1, a 51-residue histidine-rich N-terminal domain of human salivary mucin MUC7. J Pept Res 56:275-82
Gururaja, T L; Levine, J H; Tran, D T et al. (1999) Candidacidal activity prompted by N-terminus histatin-like domain of human salivary mucin (MUC7)1. Biochim Biophys Acta 1431:107-19
Naganagowda, G A; Gururaja, T L; Satyanarayana, J et al. (1999) NMR analysis of human salivary mucin (MUC7) derived O-linked model glycopeptides: comparison of structural features and carbohydrate-peptide interactions. J Pept Res 54:290-310
Khan, S H; Aguirre, A; Bobek, L A (1998) In-situ hybridization localized MUC7 mucin gene expression to the mucous acinar cells of human and MUC7-transgenic mouse salivary glands. Glycoconj J 15:1125-32
Satyanarayana, J; Gururaja, T L; Naganagowda, G A et al. (1998) A concise methodology for the stereoselective synthesis of O-glycosylated amino acid building blocks: complete 1H NMR assignments and their application in solid-phase glycopeptide synthesis. J Pept Res 52:165-79
Gururaja, T L; Ramasubbu, N; Venugopalan, P et al. (1998) Structural features of the human salivary mucin, MUC7. Glycoconj J 15:457-67
Naganagowda, G A; Gururaja, T L; Levine, M J (1998) Delineation of conformational preferences in human salivary statherin by 1H, 31P NMR and CD studies: sequential assignment and structure-function correlations. J Biomol Struct Dyn 16:91-107

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