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. 2014 Apr 18;9(4):e94928.
doi: 10.1371/journal.pone.0094928. eCollection 2014.

Prediagnostic serum biomarkers as early detection tools for pancreatic cancer in a large prospective cohort study

Brian M Nolen  1 Randall E Brand  2 Denise Prosser  1 Liudmila Velikokhatnaya  1 Peter J Allen  3 Herbert J Zeh  4 William E Grizzle  5 Ying Huang  6 Aleksey Lomakin  7 Anna E Lokshin  8
Affiliations

Prediagnostic serum biomarkers as early detection tools for pancreatic cancer in a large prospective cohort study

Brian M Nolen et al. PLoS One. .

Erratum in

Abstract

Background: The clinical management of pancreatic cancer is severely hampered by the absence of effective screening tools.

Methods: Sixty-seven biomarkers were evaluated in prediagnostic sera obtained from cases of pancreatic cancer enrolled in the Prostate, Lung, Colorectal, and Ovarian Cancer Screening Trial (PLCO).

Results: The panel of CA 19-9, OPN, and OPG, identified in a prior retrospective study, was not effective. CA 19-9, CEA, NSE, bHCG, CEACAM1 and PRL were significantly altered in sera obtained from cases greater than 1 year prior to diagnosis. Levels of CA 19-9, CA 125, CEA, PRL, and IL-8 were negatively associated with time to diagnosis. A training/validation study using alternate halves of the PLCO set failed to identify a biomarker panel with significantly improved performance over CA 19-9 alone. When the entire PLCO set was used for training at a specificity (SP) of 95%, a panel of CA 19-9, CEA, and Cyfra 21-1 provided significantly elevated sensitivity (SN) levels of 32.4% and 29.7% in samples collected <1 and >1 year prior to diagnosis, respectively, compared to SN levels of 25.7% and 17.2% for CA 19-9 alone.

Conclusions: Most biomarkers identified in previously conducted case/control studies are ineffective in prediagnostic samples, however several biomarkers were identified as significantly altered up to 35 months prior to diagnosis. Two newly derived biomarker combinations offered advantage over CA 19-9 alone in terms of SN, particularly in samples collected >1 year prior to diagnosis. However, the efficacy of biomarker-based tools remains limited at present. Several biomarkers demonstrated significant velocity related to time to diagnosis, an observation which may offer considerable potential for enhancements in early detection.

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Conflict of interest statement

Competing Interests: The authors have declared that no competing interests exist.

Figures

Figure 1
Figure 1. Biomarker panel performance in the complete PLCO cohort.
A Metropolis algorithm with Monte-Carlo simulation was utilized to identify the top performing biomarker combinations in the discrimination of PDAC cases from matched controls within the PLCO cancer screening trial. ROC curves reflecting the performance of CA 19-9, the top two biomarker panel (CA 19-9/CEA), and the top three biomarker panel (CA 19-9/CEA/Cyfra 21-1) are shown. AUCs for the three models did not differ significantly according to the method of Hanley and McNeil .
Figure 2
Figure 2. Prediagnostic distributions of serum biomarker levels.
Levels of 67 biomarkers were evaluated in sera obtained from 135 subjects enrolled in the PLCO cancer screening trial who were subsequently diagnosed with pancreatic cancer and 540 matched controls. Circulating levels of biomarkers demonstrating significant differences between cases and healthy controls are presented. Level of significance: * - p<0.03, ** - p<0.01, *** - p<0.001, **** - p<0.0001.
Figure 3
Figure 3. Biomarker levels in relation to time to diagnosis.
Biomarker levels were plotted against the elapsed time interval between blood draw and cancer diagnosis and plots were evaluated by linear regression. Biomarkers demonstrating slopes differing significantly from zero are presented.
See this image and copyright information in PMC

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