Characterization of pig colonic mucins

Author:

FOGG Fiona J. J.1,HUTTON David A.1,JUMEL Kornelia2,PEARSON Jeffrey P.1,HARDING Stephen E.2,ALLEN Adrian1

Affiliation:

1. Department of Physiological Sciences, Medical School, Framlington Place, The University, Newcastle upon Tyne NE2 4HH, U.K.

2. Department of Analytical Biochemistry and Food Science, Sutton Bonnington Campus, University of Nottingham, LE12 5RD, U.K.

Abstract

Pig colonic mucins isolated from the adherent mucus gel in the presence of proteinase inhibitors were solubilized by homogenization and the component mucins fractionated by CsCl density-gradient centrifugation. Polymeric and reduced pig colonic mucin were both largely excluded on Sepharose CL-2B, papain-digested colonic mucin was included. The Mr values of polymeric, reduced and digested mucins were 5.5×106, 2.1×106 and 0.6×106 respectively. This suggests that pig colonic mucin is comprised of 2–3 subunits, each subunit containing 3–4 glycosylated regions. The intrinsic viscosities of polymeric, reduced and digested mucin were 240 ml·g-1, 100 ml·g-1 and 20 ml·g-1 respectively. Polymeric pig colonic mucin comprised 16% protein per mg of glycoprotein and was rich in serine, threonine and proline (43% of total amino acids). There were approx. 150 disulphide bridges and 53 free thiol groups per mucin polymer. A seventh of the protein content was lost on reduction. This protein was particularly rich in proline and the hydrophobic amino acids. Papain-digested pig colonic mucin contained 11% protein per mg of glycoprotein and was rich in serine, threonine, glutamate and aspartate. All types of amino acids with the exception of aspartate were lost on digestion. The amino acid analysis of the proteolytically digested regions of pig colonic mucin are markedly different to the tandem repeat regions of the human mucin genes shown to be expressed in the colon.

Publisher

Portland Press Ltd.

Subject

Cell Biology,Molecular Biology,Biochemistry

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