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open access
Published: 3 April 2013
The complete article is available as a provisional PDF. The fully formatted PDF and HTML versions are in production.
Background
The immune system is a key player in fighting cancer. Thus, we sought to identify
a molecular 'immune response signature' indicating the presence of epithelial ovarian
cancer (EOC) and to combine this with a serum protein biomarker panel to increase
the specificity and sensitivity for earlier detection of EOC.
Methods
Comparing the expression of 32,000 genes in a leukocytes fraction from 44 EOC patients
and 19 controls, three uncorrelated shrunken centroid models were selected, comprised
of 7, 14, and 6 genes. A second selection step using RT-qPCR data and significance
analysis of microarrays yielded 13 genes (AP2A1, B4GALT1, C1orf63, CCR2, CFP, DIS3,
NEAT1, NOXA1, OSM, PAPOLG, PRIC285, ZNF419, and BC037918) which were finally used
in 343 samples (90 healthy, six cystadenoma, eight low malignant potential tumor,
19 FIGO I/II, and 220 FIGO III/IV EOC patients). Using new 65 controls and 224 EOC
patients (thereof 14 FIGO I/II) the abundances of six plasma proteins (MIF, prolactin,
CA125, leptin, osteopondin, and IGF2) was determined and used in combination with
the expression values from the 13 genes for diagnosis of EOC.
Results
Combined diagnostic models using either each five gene expression and plasma protein
abundance values or 13 gene expression and six plasma protein abundance values can
discriminate controls from patients with EOC with Receiver Operator Characteristics
Area Under the Curve values of 0.998 and bootstrap .632+ validated classification
errors of 3.1% and 2.8%, respectively. The sensitivities were 97.8% and 95.6%, respectively,
at a set specificity of 99.6%.
Conclusions
The combination of gene expression and plasma protein based blood derived biomarkers
in one diagnostic model increases the sensitivity and the specificity significantly.
Such a diagnostic test may allow earlier diagnosis of epithelial ovarian cancer.
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