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The role of modelling in the policy decision making process for cancer screening: example of prostate specific antigen screening

机译:建模在癌症筛查政策决策过程中的作用:前列腺特异性抗原筛查的例子

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Although randomised controlled trials are the preferred basis for policy decisions on cancer screening, it remains difficult to assess all downstream effects of screening, particularly when screening options other than those in the specific trial design are being considered. Simulation models of the natural history of disease can play a role in quantifying harms and benefits of cancer screening scenarios. Recently, the US Preventive Services Task Force issued a C-recommendation on screening for prostate cancer for men aged 55–69?years, implying at least moderate certainty that the benefit is small. However, modelling based on data from the European Randomized study of Screening for Prostate Cancer, which included quality-of-life estimates, showed that the ratio between benefits and harms is better, and likely to be reasonable, for men screened between the ages of 55 and 63?years (i.e.?by using an earlier stopping age than applied in the trial setting). This commentary article considers the importance of simulation modelling in the decision-making process for (prostate) cancer screening. The paper also explores whether the recently published Cluster Randomized Trial of PSA Testing for Prostate Cancer, a trial of a single prostate specific antigen (PSA) testing intervention in the UK, changes the evidence for regular PSA testing for men aged 55–63?years by replicating the trial using a simulation model.
机译:尽管随机对照试验是癌症筛查政策决策的首选依据,但仍然难以评估筛查的所有下游影响,尤其是在考虑采用特定试验设计以外的筛查方案时。疾病自然史的模拟模型可以在量化癌症筛查方案的危害和益处方面发挥作用。最近,美国预防服务工作队发布了一项针对55岁至69岁男性筛查前列腺癌的C建议,这至少可以肯定地确定这种益处很小。但是,根据来自欧洲前列腺癌筛查随机研究的数据进行建模,其中包括生活质量评估,结果表明,对于年龄介于15岁至60岁之间的男性,利弊之间的比例更好,而且可能是合理的。 55岁和63岁(即,使用比试验环境中使用的年龄更早的停止年龄)。这篇评论文章认为模拟模型在(前列腺)癌症筛查的决策过程中的重要性。本文还探讨了最近发表的针对前列腺癌的PSA检测的群集随机试验是否是一项针对英国单一前列腺特异性抗原(PSA)检测干预措施的试验,是否改变了55-63岁男性定期进行PSA检测的证据?通过使用模拟模型复制试验。

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