Your browser version may not work well with NCBI's Web applications. More information here...
1: Biochem Biophys Res Commun. 1999 Oct 5;263(3):728-36.Click here to read Links

Genomic organization and structure of the 3' region of human MUC3: alternative splicing predicts membrane-bound and soluble forms of the mucin.

Crawley SC, Gum JR Jr, Hicks JW, Pratt WS, Aubert JP, Swallow DM, Kim YS.

Department of Medicine, University of California, San Francisco, California 94143, USA.

The MUC3 gene encodes a large, glycosylated mucin produced by intestinal epithelial cells to form a protective barrier against the external environment. Recently published cDNA sequences for the carboxyl-terminal region of MUC3 polypeptide indicated that rodent Muc3 possesses two epidermal growth factor (EGF)-like domains, and putative transmembrane and cytoplasmic domains, whereas the sequence of human MUC3 predicted termination after the first EGF-like domain. Here we describe the complete genomic sequence encompassing the carboxyl terminal region of human MUC3, revealing the boundaries of 11 exons. RT-PCR and cDNA library cloning experiments indicate that the gene is alternatively spliced, yielding a major membrane-bound form as well as multiple soluble forms. Thus, this work indicates that both membrane-bound and soluble MUC3 mucin proteins are produced by alternative splicing of a single gene. A potentially important polymorphism involving a Tyr residue with a proposed role in signalling is described as well. Copyright 1999 Academic Press.

PMID: 10512748 [PubMed - indexed for MEDLINE]