AI Article Synopsis

  • An early detection tool for early ovarian cancer (EOC) was developed using serum biomarker data from a long-term study (UKCTOCS) involving 49 EOC cases and 31 controls over seven years.
  • The tool utilizes a logit model analyzing four key biomarkers (CA125, phosphatidylcholine-sterol acyltransferase, vitamin K-dependent protein Z, and C-reactive protein) to improve diagnostic specificity before clinical diagnosis.
  • The model shows promise in diagnosing EOC 1-2 years earlier than current methods, with over 30% positive predictive value (PPV) for early detection, although limitations exist due to the number of samples analyzed.

Article Abstract

Background: An early detection tool for EOC was constructed from analysis of biomarker expression data from serum collected during the UKCTOCS.

Methods: This study included 49 EOC cases (19 Type I and 30 Type II) and 31 controls, representing 482 serial samples spanning seven years pre-diagnosis. A logit model was trained by analysis of dysregulation of expression data of four putative biomarkers, (CA125, phosphatidylcholine-sterol acyltransferase, vitamin K-dependent protein Z and C-reactive protein); by scoring the specificity associated with dysregulation from the baseline expression for each individual.

Results: The model is discriminatory, passes k-fold and leave-one-out cross-validations and was further validated in a Type I EOC set. Samples were analysed as a simulated annual screening programme, the algorithm diagnosed cases with >30% PPV 1-2 years pre-diagnosis. For Type II cases (~80% were HGS) the algorithm classified 64% at 1 year and 28% at 2 years tDx as severe.

Conclusions: The panel has the potential to diagnose EOC one-two years earlier than current diagnosis. This analysis provides a tangible worked example demonstrating the potential for development as a screening tool and scrutiny of its properties. Limits on interpretation imposed by the number of samples available are discussed.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6738042PMC
http://dx.doi.org/10.1038/s41416-019-0544-0DOI Listing

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