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Quantifying the potential benefits of early detection for pancreatic cancer through a counterfactual simulation modeling analysis. | LitMetric

AI Article Synopsis

  • Early detection of cancer, including pancreatic ductal adenocarcinoma (PDAC), can have significant benefits, but these depend on factors like cancer type and screening effectiveness.
  • Research in this study used a population model to simulate PDAC progression and aimed to understand the optimal timing for early detection to maximize mortality benefits.
  • The findings suggest that detecting PDAC 4-6 years before clinical diagnosis yields the greatest life-years gained, but benefits decrease if detection happens too early or too late based on the speed of cancer progression.

Article Abstract

The benefits of cancer early detection depend on various factors, including cancer type, screening method performance, stage at diagnosis, and subsequent treatment. Although numerous studies have evaluated the effectiveness of screening interventions for identifying cancer at earlier stages, there is no quantitative analysis that studies the optimal early detection time interval that results in the greatest mortality benefit; such data could serve as a target and benchmark for cancer early detection strategies. In this study, we focus on pancreatic ductal adenocarcinoma (PDAC), a cancer known for its lack of early symptoms. Consequently, it is most often detected at late stages when the 5-year survival rate is only 3%. We developed a PDAC population model that simulates an individual patient's age and stage at diagnosis, while replicating overall US cancer incidence and mortality rates. The model includes "cancer sojourn time," serving as a proxy for the speed of cancer progression, with shorter times indicating rapid progression and longer times indicating slower progression. In our PDAC model, our hypothesis was that earlier cancer detection, potentially through a hypothetical screening intervention in the counterfactual analysis, would yield reduced mortality as compared to a no-screening group. We found that the benefits of early detection, such as increased life-years gained, are greater when the sojourn time is shorter, reaching their maximum when identification is made 4-6 years prior to clinical diagnosis (e.g., when a symptomatic diagnosis is made). However, when early detection occurs even earlier, for example 6-10 years prior to clinical diagnosis, the benefits significantly diminish for shorter sojourn time cancers, and level off for longer sojourn time cancers. Our study clarifies the potential benefits of PDAC early detection that explicitly incorporates individual patient heterogeneity in cancer progression and identifies quantitative benchmarks for future interventions.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10654404PMC
http://dx.doi.org/10.1038/s41598-023-46751-3DOI Listing

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