Molecular forms and microheterogeneity of the oligosaccharide chains of pregnancy-associated CA125 antigen

doi:10.1093/humrep/dei095

Hum. Reprod. Advance Access originally published online on May 19, 2005
Human Reproduction 2005 20(9):2632-2638; doi:10.1093/humrep/dei095

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© The Author 2005. Published by Oxford University Press on behalf of the European Society of Human Reproduction and Embryology. All rights reserved. For Permissions, please email: journals.permissions{at}oupjournals.org

Molecular forms and microheterogeneity of the oligosaccharide chains of pregnancy-associated CA125 antigen

Miroslava M. Jankovic¹ and Bojana S. Tapuskovic

Institute for the Application of Nuclear Energy – INEP, Belgrade, Banatska 31b, 11080 Zemun-Belgrade, Serbia and Montenegro

¹ To whom correspondence should be addressed. Email: miraj{at}inep.co.yu

BACKGROUND: The cancer antigen CA125 has a very complex moleculararchitecture in terms of both protein backbone and oligosaccharidechains. In this study, we examined the molecular forms and microheterogeneityof oligosaccharide chains of pregnancy-associated CA125, asa first step towards gaining an insight into its possible involvementas a ligand in carbohydrate-dependent interactions. The glycobiochemicalproperties of CA125 may be of diagnostic and biomedical importanceas specific markers of physiological and pathological conditionsof early pregnancy, as well as targets in different therapeuticprocedures. METHODS: Pregnancy-associated CA125 was characterizedby gel filtration and ion-exchange chromatography, followedby lectin-affinity chromatography with a panel of plant lectinsas ligands. RESULTS: CA125 antigen isolated from first trimesterplacental extract was found to be heterogeneous in respect tomolecular mass and the existence of different glyco-isoforms.Thus, elution profiles from the lectin-affinity columns demonstratedmolecular subpopulations bound with low, intermediate and highaffinity. Under the applied experimental conditions, CA125 boundmost strongly to Triticum vulgaris agglutinin (WGA) and Ricinuscommunis agglutinin (RCA), but low affinity interactions occurredwith the other lectins tested. CONCLUSIONS: The assessment ofthe carbohydrate composition of N- and O-glycans of pregnancy-associatedCA125 was in general agreement with available data on CA125of cancer origin. The main difference was observed in reactivityto Canavalia ensiformis agglutinin (ConA) and Phaseolus vulgariserythroagglutinin (PHA-E) binding.

Key words: CA125 antigen/glycosylation/lectin-binding pattern/placenta/pregnancy

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