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Search for breast cancer biomarkers in fractionated serum samples by protein profiling with SELDI-TOF MS.

Annemieke W J Opstal-van Winden ,
Jos H Beijnen ,
Arnoud Loof ,
Waander L van Heerde ,
Roel Vermeulen ,
Petra H M Peeters ,
Carla H van Gils

Abstract

METHODS

We aimed to detect lower abundant discriminating proteins by performing serum fractionation by strong anion exchange chromatography preceding protein profiling with SELDI-TOF MS. In a pilot study, we tested the different fractions resulting from fractionation, on several array types. Fraction 3 on IMAC30 and Fraction 6 on Q10 yielded the most discriminative proteins and were used for serum protein profiling of 73 incident breast cancer cases and 73 matched controls.

CONCLUSION

By extensive serum fractionation, we detected many more proteins than in previous studies without fractionation. However, discriminating proteins were still high abundant. Results indicate that either lower abundant proteins are less distinctive, or more rigorous fractionation and selective protein depletion, or a more sensitive assay, are needed to detect lower abundant discriminative proteins.

RESULTS

Eight peaks showed statistically significantly different intensities between cases and controls (P⧁0.05), and had less than 10% chance to be a false-positive finding. Seven of these were tentatively identified as apolipoprotein C-II (m/z 8,909), oxidized apolipoprotein C-II (m/z 8,925), apolipoprotein C-III (m/z 8,746), fragment of coagulation factor XIIIa (m/z 3,959), heterodimer of apolipoprotein A-I and apolipoprotein A-II (m/z 45,435), hemoglobin B-chain (m/z 15,915), and post-translational modified hemoglobin (m/z 15,346).

BACKGROUND

Many high-abundant acute phase reactants have been previously detected as potential breast cancer biomar-kers. However, they are unlikely to be specific for breast cancer. Cancer-specific biomarkers are thought to be among the lower abundant proteins.

More about this publication

Journal of clinical laboratory analysis

Volume 26
Issue nr. 1
Pages 1-9
Publication date 01-01-2012

Full text links

Publisher website (DOI) 10.1002/jcla.20492
Europe PubMed Central 24833528
Pubmed 24833528

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