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Fast approximate computation of cervical cancer screening outcomes by a deterministic multiple-type HPV progression model

机译:确定性多型HPV进展模型快速近似计算宫颈癌筛选结果

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Cervical cancer arises differentially from infections with up to 14 high-risk human papillomavirus (HPV) types, making model-based evaluations of cervical cancer screening strategies computationally heavy and structurally complex. Thus, with the high number of HPV types, microsimulation is typically used to investigate cervical cancer screening strategies. We developed a feasible deterministic model that integrates varying natural history of cervical cancer by the different high-risk HPV types with compressed mixture representations of the screened population, allowing for fast computation of screening interventions. To evaluate the method, we built a corresponding microsimulation model. The outcomes of the deterministic model were stable over different levels of compression and agreed with the microsimulation model for all disease states, screening outcomes, and levels of cancer incidence. The compression reduced the computation time more than 1000 fold when compared to microsimulation in a cohort of 1 million women. The compressed mixture representations enable the assessment of uncertainties surrounding the natural history of cervical cancer and screening decisions in a computationally undemanding way.
机译:宫颈癌从患有多达14种高风险的人乳头瘤病毒(HPV)类型的感染差异,使基于模型的宫颈癌筛查策略的评估计算繁重和结构性复杂。因此,随着HPV类型的大量,微仿通常用于研究宫颈癌筛查策略。我们开发了一种可行的确定性模型,通过不同的高风险HPV类型与筛选群体的压缩混合物表示相结合不同的宫颈癌自然历史,允许快速计算筛选干预措施。为了评估该方法,我们建立了一个相应的微化模型。确定性模型的结果在不同的压缩水平上稳定,并同意所有疾病状态的微仿模型,筛查结果和癌症发病率水平。与100万女性队列的群体微观相比,压缩减少了计算时间超过1000倍。压缩的混合物表示使得评估宫颈癌自然病史的不确定性,并以计算不当方式筛选决策。

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