Alteration of N ‐glycan profiles in patients with chronic hepatitis and hepatocellular carcinoma

Aim Most of the modification of N ‐glycosylation reported in cancers including hepatocellular carcinoma ( HCC ) were based on the examinations of a small number of patients or particular proteins. The aim of this study is to reveal changes in whole serum N ‐glycan profiles systematically during the process of hepatocarcinogenesis and to elucidate their clinical application. Methods We analyzed sera from 105 patients with chronic hepatitis/liver cirrhosis ( CH / LC ) and age‐/sex‐matched healthy volunteers ( HLT ), as well as from 114 patients with HCC . Serum N ‐glycan profiles were measured comprehensively by a new, quantitative, high‐throughput method and compared with clinical parameters. Results The total amount of N ‐glycan expression was significantly higher in patients with CH / LC than in HLT ; however, no differences were observed between CH / LC and HCC patients. In HCC patients, multi‐antennary glycans with fucose residues, particularly m/z 3195, were increased compared with CH / LC patients. The expression of m/z 3195 was high, especially in patients with a high number of intrahepatic lesions (>3), large tumor size (>3 cm), macroscopic vascular invasion or metastasis. The ratio of pairs of glycans on the same path of the biosynthesis pathway ( m/z 3195/1914) showed a higher area under the receiver–operator curve of 0.810 than any other single glycan to distinguish HCC from CH / LC . Conclusion We demonstrate the full spectrum of the alterations of serum N ‐glycans comprehensively in patients with liver disease, and elucidate the possible use of glycans as novel biomarkers of liver disease progression.