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粪便血红蛋白浓度依赖性预测结直肠肿瘤的新见解。

A new insight into fecal hemoglobin concentration-dependent predictor for colorectal neoplasia.

机构信息

School of Oral Hygiene, College of Oral Medicine, Taipei Medical University, Taipei, Taiwan.

出版信息

Int J Cancer. 2014 Sep 1;135(5):1203-12. doi: 10.1002/ijc.28748. Epub 2014 Feb 19.

Abstract

We sought to assess how much of the variation in incidence of colorectal neoplasia is explained by baseline fecal hemoglobin concentration (FHbC) and also to assess the additional predictive value of conventional risk factors. We enrolled subjects aged 40 years and over who attended screening for colorectal cancer with the fecal immunochemical test (FIT) in Keelung community-based integrated screening program. The accelerated failure time model was used to train the clinical weights of covariates in the prediction model. Datasets from two external communities were used for external validation. The area under curve (AUC) for the model containing only FHbC was 83.0% (95% CI: 81.5-84.4%), which was considerably greater than the one containing only conventional risk factors (65.8%, 95% CI: 64.2-67.4%). Adding conventional risk factors did not make significant additional contribution (p = 0.62, AUC = 83.5%, 95% CI: 82.1-84.9%) to the predictive model with FHbC only. Males showed a stronger linear dose-response relationship than females, yielding gender-specific FHbC predictive models. External validation confirms these results. The high predictive ability supported by a dose-dependent relationship between baseline FHbC and the risk of developing colorectal neoplasia suggests that FHbC may be useful for identifying cases requiring closer postdiagnosis clinical surveillance as well as being an early indicator of colorectal neoplasia risk in the general population. Our findings may also make contribution to the development of the FHbC-guided screening policy but its pros and cons in connection with cost and effectiveness of screening should be evaluated before it can be applied to population-based screening for colorectal cancer.

摘要

我们旨在评估粪便血红蛋白浓度(FHbC)基线水平解释结直肠肿瘤发病率差异的程度,同时评估传统危险因素的额外预测价值。我们招募了参加基隆社区综合筛查计划粪便免疫化学检测(FIT)筛查的 40 岁及以上人群。采用加速失效时间模型训练预测模型中协变量的临床权重。使用来自两个外部社区的数据集进行外部验证。仅包含 FHbC 的模型的曲线下面积(AUC)为 83.0%(95%CI:81.5-84.4%),明显大于仅包含传统危险因素的模型(65.8%,95%CI:64.2-67.4%)。仅包含传统危险因素并不能对仅包含 FHbC 的预测模型做出显著的额外贡献(p=0.62,AUC=83.5%,95%CI:82.1-84.9%)。男性比女性表现出更强的线性剂量反应关系,产生了性别特异性的 FHbC 预测模型。外部验证证实了这些结果。FHbC 基线水平与结直肠肿瘤发生风险之间存在剂量依赖性关系,这一高预测能力表明,FHbC 可能有助于识别需要更密切的诊断后临床监测的病例,并且是一般人群结直肠肿瘤风险的早期指标。我们的研究结果可能对 FHbC 指导的筛查政策的制定做出贡献,但在将其应用于基于人群的结直肠癌筛查之前,应该评估其在成本和效果方面的利弊。

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