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Multiplex determination of serological signatures in the sera of colorectal cancer patients using hydrogel biochips
Author(s) -
Butvilovskaya Veronika I.,
Popletaeva Sofya B.,
Chechetkin Vladimir R.,
Zubtsova Zhanna I.,
Tsybulskaya Marya V.,
Samokhina Larisa O.,
Vinnitskii Leonid I.,
Ragimov Aligeydar A.,
Pozharitskaya Elena I.,
Grigor´eva Galina A.,
Meshalkitalya Y.,
Golysheva Svetlana V.,
Shilova Nadezhda V.,
Bovin Nicolai V.,
Zasedatelev Aleksander S.,
Rubina Alla Y.
Publication year - 2016
Publication title -
cancer medicine
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.403
H-Index - 53
ISSN - 2045-7634
DOI - 10.1002/cam4.692
Subject(s) - carcinoembryonic antigen , multiplex , antibody , colorectal cancer , serology , malignancy , antigen , medicine , glycan , cancer , immunology , microbiology and biotechnology , biology , bioinformatics , glycoprotein
Abstract Colorectal cancer ( CRC ) is the third most common malignancy in industrialized countries. Despite the advances in diagnostics and development of new drugs, the 5‐year survival remains only 60–65%. Our approach to early diagnostics of CRC is based on the determination of serological signatures with an array of hemispherical hydrogel cells containing immobilized proteins and oligosaccharides (glycochip). The compounds immobilized on the glycochip include tumor‐associated glycans (SiaTn, Tn, TF , Le C , Le Y , SiaLe A , and Man β 1‐4Glc NA c β ) and antibodies against human immunoglobulins IgG, IgA, and IgM. The glycochip detects antibodies against tumor‐associated glycans in patients’ sera. The simultaneous measurement of the levels of immunoglobulins enhances the diagnostic impact of the signatures. In this work, we found previously unreported increase in antibodies against oligosaccharide Man β 1‐4Glc NA c β in patients with CRC . In parallel with these experiments, we determined the levels of oncomarkers carcinoembryonic antigen ( CEA ), cancer antigen ( CA ) 19–9, CA 125, CA 15–3, human chorionic gonadotropin ( HCG ), and alpha‐fetoprotein ( AFP ) using another gel‐based biochip with immobilized antibodies (oncochip) developed earlier in our laboratory. In total, 69 samples from healthy donors, 33 from patients with colorectal carcinoma, and 27 from patients with inflammatory bowel diseases were studied. The use of combined signatures of antiglycan antibodies and oncomarkers provides much better predictive value than the conventional measurement of oncomarkers CEA and CA 19–9. Positive predictive value of CRC diagnoses using together glycochip and oncochip reached 95% with the sensitivity and specificity 88% and 98%, respectively. Thus, the combination of antibody profiling with detection of conventional oncomarkers proved to be a promising tool in diagnostics of CRC .

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