Journal
JOURNAL OF INNATE IMMUNITY
Volume 9, Issue 3, Pages 281-299Publisher
KARGER
DOI: 10.1159/000453594
Keywords
Mucosal immunology; MUC1; MUC3; MUC4; MUC12; MUC13; MUC16; MUC17; Post-translational modification; Extracellular domain; Ectodomain; Intracellular domain; Cytoplasmic tail; Intracellular signaling; beta-Catenin; Transcriptional modulation; Carcinogenesis; Metastasis
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Funding
- Marie Curie International Incoming Fellowship (IIF)
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Mucosal surfaces line our body cavities and provide the interaction surface between commensal and pathogenic microbiota and the host. The barrier function of the mucosal layer is largely maintained by gel-forming mucin proteins that are secreted by goblet cells. In addition, mucosal epithelial cells express cell-bound mucins that have both barrier and signaling functions. The family of transmembrane mucins consists of diverse members that share a few characteristics. The highly glycosylated extracellular mucin domains inhibit invasion by pathogenic bacteria and can form a tight mesh structure that protects cells in harmful conditions. The intracellular tails of transmembrane mucins can be phosphorylated and connect to signaling pathways that regulate inflammation, cell-cell interactions, differentiation, and apoptosis. Transmembrane mucins play important roles in preventing infection at mucosal surfaces, but are also re-nowned for their contributions to the development, progression, and metastasis of adenocarcinomas. In general, transmembrane mucins seem to have evolved to monitor and repair damaged epithelia, but these functions can be highjacked by cancer cells to yield a survival advantage. This review presents an overview of the current knowledge of the functions of transmembrane mucins in inflammatory processes and carcinogenesis in order to better understand the diverse functions of these multifunctional proteins. (C) 2017 S. Karger AG, Basel
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