Abstract
Mucins are large O-glycoproteins with high carbohydrate content and marked diversity in both the apoprotein and the oligosaccharide moieties. All three mucin types, trans-membrane (e.g., MUC1, MUC4, MUC16), secreted (gel-forming) (e.g., MUC2, MUC5AC, MUC6) and soluble (non-gel-forming) (e.g., MUC7, MUC8, MUC9, MUC20), are critical in maintaining cellular functions, particularly those of epithelial surfaces. Their aberrant expression and/or altered subcellular localization is a factor of tumour growth and apoptosis induced by oxidative stress and several anti-cancer agents. Abnormal expression of mucins was observed in human carcinomas that arise in various gastrointestinal organs. It was widely believed that hepatocellular carcinoma (HCC) does not produce mucins, whereas cholangiocarcinoma (CC) or combined HCC-CC may produce these glycoproteins. However, a growing number of reports shows that mucins can be produced by HCC cells that do not exhibit or are yet to undergo, morphological differentiation to biliary phenotypes. Evaluation of mucin expression levels in precursors and early lesions of CC, as well as other types of primary liver cancer (PLC), conducted in in vitro and in vivo models, allowed to discover the mechanisms of their action, as well as their participation in the most important signalling pathways of liver cystogenesis and carcinogenesis. Analysis of mucin expression in PLC has both basic research and clinical value. Mucins may act as oncogenes and tumour-promoting (e.g., MUC1, MUC13), and/or tumour-suppressing factors (e.g., MUC15). Given their role in promoting PLC progression, both classic (MUC1, MUC2, MUC4, MUC5AC, MUC6) and currently tested mucins (e.g., MUC13, MUC15, MUC16) have been proposed to be important diagnostic and prognostic markers. The purpose of this review was to summarize and update the role of classic and currently tested mucins in pathogenesis of PLC, with explaining the mechanisms of their action in HCC carcinogenesis. It also focuses on determination of the diagnostic and prognostic role of these glycoproteins in PLC, especially focusing on HCC, CC and other hepatic tumours with- and without biliary differentiation.
Highlights
Mucins (MUC) are a major constituent of any mucous secretion, providing the mucus with its biophysiochemical properties due to their nature and extent of glycosylation [1,2]
MUC7 and MUC19 are main components of the saliva [11,58], MUC5AC and MUC6 are characteristic for the stomach mucus, with MUC2 being proprietary to intestinal mucus [7,8,11,57]
Mucins of this group are coded by the mucin gene family, including: MUC2, MUC5AC, MUC5B, MUC6 and MUC19 (12q12) as oligomerizing mucins and MUC7 (4q13.3) as the only non-oligomerizing mucin [14,22]
Summary
Mucins (MUC) are a major constituent of any mucous secretion, providing the mucus with its biophysiochemical properties due to their nature and extent of glycosylation [1,2]. Human mucin genes exhibit a specific domain, called the Variable Number Tandem Repeat Region (VNTR) It encodes a Tandem Repeat Peptide (TRP) with high percentage of such amino acids (aa) as serine (Ser) and threonine (Thr). Function and cellular localization, the mucins are divided into two classes: membrane (cell surface associated) and secreted [11,16,23,24]. The purpose of this review was to summarize and update the role of classic (MUC1, MUC2, MUC4, MUC5AC, MUC6) and currently tested (e.g., MUC13, MUC15, MUC16) mucins in pathogenesis of PLC, with explaining the mechanisms of their action in HCC carcinogenesis It focuses on determination of the diagnostic and prognostic role of these glycoproteins in PLC, especially focusing on HCC, CC and other hepatic tumours with- and without biliary differentiation. MUC7 and MUC19 are main components of the saliva [11,58], MUC5AC and MUC6 are characteristic for the stomach mucus, with MUC2 being proprietary to intestinal mucus [7,8,11,57]
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