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Risk stratification in cervical cancer screening by complete screening history: Applying bioinformatics to a general screening population. | LitMetric

AI Article Synopsis

  • A study in Sweden evaluated the effectiveness of a cervical cancer screening program, suggesting it could be improved by using women's complete screening histories to identify risk patterns.
  • Analysis of data from over 125,000 women revealed moderate accuracy in predicting cancer risk, with some screening history patterns showing significantly higher odds ratios for developing cervical cancer.
  • The findings indicate that targeted screening could be beneficial, allowing for increased frequency in high-risk subgroups and potentially reduced frequency in low-risk subgroups without elevating risk.

Article Abstract

Women screened for cervical cancer in Sweden are currently treated under a one-size-fits-all programme, which has been successful in reducing the incidence of cervical cancer but does not use all of the participants' available medical information. This study aimed to use women's complete cervical screening histories to identify diagnostic patterns that may indicate an increased risk of developing cervical cancer. A nationwide case-control study was performed where cervical cancer screening data from 125,476 women with a maximum follow-up of 10 years were evaluated for patterns of SNOMED diagnoses. The cancer development risk was estimated for a number of different screening history patterns and expressed as Odds Ratios (OR), with a history of 4 benign cervical tests as reference, using logistic regression. The overall performance of the model was moderate (64% accuracy, 71% area under curve) with 61-62% of the study population showing no specific patterns associated with risk. However, predictions for high-risk groups as defined by screening history patterns were highly discriminatory with ORs ranging from 8 to 36. The model for computing risk performed consistently across different screening history lengths, and several patterns predicted cancer outcomes. The results show the presence of risk-increasing and risk-decreasing factors in the screening history. Thus it is feasible to identify subgroups based on their complete screening histories. Several high-risk subgroups identified might benefit from an increased screening density. Some low-risk subgroups identified could likely have a moderately reduced screening density without additional risk.

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Source
http://dx.doi.org/10.1002/ijc.30725DOI Listing

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