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1 Emma Children's Hospital,
To help us investigate the role of mucin in the
protection of the colonic epithelium in the mouse, we aimed to identify
the murine colonic mucin (MCM) and its encoding gene. We isolated MCM,
raised an anti-MCM antiserum, and studied the biosynthesis of MCM in
the gastrointestinal tract. Isolated MCM resembled other mucins in
physicochemical properties. Anti-MCM recognized MCM as well as rat and
human MUC2 on Western blots, interacting primarily with
peptide epitopes, indicating that MCM was identical to murine Muc2.
Using anti-MCM and previously characterized anti-human and anti-rat
MUC2 antibodies, we identified a murine Muc2 precursor in the colon of
~600 kDa, which appeared similar in size to rat and human MUC2
precursors. Western blotting, immunoprecipitation of metabolically
labeled mucins, and immunohistochemistry showed that murine Muc2 was
expressed in the colon and the small intestine but was absent in the
stomach. To independently identify murine Muc2, we cloned a cDNA
fragment from murine colonic mRNA, encoding the 302 NH2-terminal amino acids of murine
Muc2. The NH2 terminus of murine
Muc2 showed 86 and 75% identity to the corresponding rat and human
MUC2 peptide sequences, respectively. Northern blotting with a murine
Muc2 cDNA probe showed hybridization to a very large mRNA, which was
expressed highly in the colon and to some extend in the small intestine
but was absent in the stomach. In situ hybridization showed that the
murine Muc2 mRNA was confined to intestinal goblet cells. In
conclusion, by two independent sets of experiments we identified murine
Muc2, which appears homologous to rat and human MUC2. Because Muc2 is
prominently expressed in the colon, it is most likely to be the
predominant mucin in the colonic mucus layer.
mucin; gastrointestinal tract; colon; intestine
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