Literature DB >> 9109822

Human salivary mucin MG1 selectively forms heterotypic complexes with amylase, proline-rich proteins, statherin, and histatins.

I Iontcheva1, F G Oppenheim, R F Troxler.   

Abstract

Heterotypic complexes between the high-molecular-weight mucin MG1 and other salivary proteins in human submandibular/sublingual secretion (HSMSL) could have a significant impact on the biological properties of these proteins in oral fluids in both health and disease. We describe a mild procedure for isolation and purification of native MG1 by gel filtration chromatography on Sepharose CL-2B which does not involve dialysis, lyophilization, use of denaturing agents, or covalent modification. Western blots of native MG1 probed with antibodies against 8 different salivary proteins showed that complexing occurs between MG1 and salivary amylase, proline-rich proteins (PRPs), statherins, and histatins but not MG1, sIgA, secretory component, or cystatins. When native MG1 was placed in 4 M guanidine hydrochloride and chromatographed on Sepharose CL-4B, ELISA measurement of column fractions showed that amylase, PRPs, statherins, and histatins were released. Interestingly, gel filtration resolved the material which eluted into 4 or 5 distinct peaks, suggesting that the released entities were heterotypic complexes. From these studies, the occurrence of at least three different types of complexes between MG1 and other salivary proteins has been identified. Type 1 complexes are dissociated by SDS-PAGE and in 4 M guanidine hydrochloride. Type II complexes are not dissociated under these conditions. Type III complexes are dissociated during SDS-PAGE and by 4 M guanidine hydrochloride, but the released proteins appear to be complexes containing amylase, PRPs, statherins, and histatins. The possible functional role of heterotypic complexes between MG1 and other salivary proteins as a physiologic delivery system, a mechanism for protection against proteolysis, a repository for precursors of the acquired enamel pellicle, and a vehicle for modulation of the viscoelastic and rheological properties of saliva is discussed.

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Year:  1997        PMID: 9109822     DOI: 10.1177/00220345970760030501

Source DB:  PubMed          Journal:  J Dent Res        ISSN: 0022-0345            Impact factor:   6.116


  35 in total

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7.  Potential biomarkers of human salivary function: a modified proteomic approach.

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8.  Salivary mucins protect surfaces from colonization by cariogenic bacteria.

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9.  IL-13 and epidermal growth factor receptor have critical but distinct roles in epithelial cell mucin production.

Authors:  Guohua Zhen; Sung Woo Park; Louis T Nguyenvu; Madeleine W Rodriguez; Rebecca Barbeau; Agnes C Paquet; David J Erle
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10.  Individual differences in AMY1 gene copy number, salivary α-amylase levels, and the perception of oral starch.

Authors:  Abigail L Mandel; Catherine Peyrot des Gachons; Kimberly L Plank; Suzanne Alarcon; Paul A S Breslin
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