Dimeric Le(a) (Le(a)-on-Le(a)) status of beta-haptoglobin in sera of colon cancer, chronic inflammatory disease and normal subjects

The glycosyl epitope dimeric Lea (Lea-on-Lea), defined by mouse monoclonal antibody NCC-ST-421, was identified previously as tumor-associated antigen, expressed highly in various human cancer tissues and cell lines derived therefrom, but with minimal expression in various normal tissues. In the pres...

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Published inInternational journal of oncology Vol. 36; no. 5; p. 1291
Main Authors Park, Seung-Yeol, Yoon, Seon-Joo, Hakomori, Sen-Itiroh, Kim, Jin-Man, Kim, Ji-Yeon, Bernert, Bradford, Ullman, Thomas, Itzkowitz, Steven H, Kim, Jung Hoe
Format Journal Article
LanguageEnglish
Published Greece 01.05.2010
Subjects
alpha-L-Fucosidase - chemistry
Animals
Cell Line, Tumor
Chromatography, Thin Layer - methods
Colonic Neoplasms - blood
Epitopes - chemistry
Gangliosides - metabolism
Gene Expression Regulation, Neoplastic
Glycosphingolipids - metabolism
Haptoglobins - biosynthesis
Humans
Inflammation - blood
Mice
Peptide-N4-(N-acetyl-beta-glucosaminyl) Asparagine Amidase - chemistry
Polysaccharides - chemistry
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Summary:The glycosyl epitope dimeric Lea (Lea-on-Lea), defined by mouse monoclonal antibody NCC-ST-421, was identified previously as tumor-associated antigen, expressed highly in various human cancer tissues and cell lines derived therefrom, but with minimal expression in various normal tissues. In the present study, we observed clearly higher expression of this epitope, defined by ST421, in beta-haptoglobin (beta-Hap) from sera of patients with colorectal cancer, compared to normal, healthy subjects or patients with chronic inflammatory processes (Crohn's disease, ulcerative colitis). We focused, therefore, on biochemical characterization of glycosyl epitope status expressed in beta-Hap. We concluded that the dimeric Lea epitope is carried by O-linked but not by N-linked structure, based on the following observations: i) Treatment of beta-Hap with alpha-L-fucosidase reduced its reactivity with ST421, but did not affect its reactivity with anti-Hap antibody. In contrast, treatment of purified beta-Hap with PNGase F, which releases N-linked glycans, had no effect on reactivity with ST421, but changed molecular mass from 40 kDa to 30 kDa. ii) Strong reactivity of Colo205 supernatant with ST421 was reduced clearly by pre-incubation of cells with benzyl-alpha-GalNAc.
ISSN:1791-2423
DOI:10.3892/ijo_00000614