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前列腺特异性抗原筛查导致的过度诊断:来自美国前列腺癌发病率趋势的经验教训。

Overdiagnosis due to prostate-specific antigen screening: lessons from U.S. prostate cancer incidence trends.

作者信息

Etzioni Ruth, Penson David F, Legler Julie M, di Tommaso Dante, Boer Rob, Gann Peter H, Feuer Eric J

机构信息

Program in Biostatistics, Fred Hutchinson Cancer Research Center, Seattle, WA 98109-1024, USA.

出版信息

J Natl Cancer Inst. 2002 Jul 3;94(13):981-90. doi: 10.1093/jnci/94.13.981.

Abstract

BACKGROUND

Overdiagnosis of clinically insignificant prostate cancer is considered a major potential drawback of prostate-specific antigen (PSA) screening. Quantitative estimates of the magnitude of this problem are, however, lacking. We estimated rates of prostate cancer overdiagnosis due to PSA testing that are consistent with the observed incidence of prostate cancer in the United States from 1988 through 1998. Overdiagnosis was defined as the detection of prostate cancer through PSA testing that otherwise would not have been diagnosed within the patient's lifetime.

METHODS

We developed a computer simulation model of PSA testing and subsequent prostate cancer diagnosis and death from prostate cancer among a hypothetical cohort of two million men who were 60-84 years old in 1988. Given values for the expected lead time--that is, the time by which the test advanced diagnosis--and the expected incidence of prostate cancer in the absence of PSA testing, the model projected the increase in population incidence of prostate cancer associated with PSA testing. By comparing the model-projected incidence with the observed incidence derived from the National Cancer Institute's Surveillance, Epidemiology, and End Results (SEER) registry data, we determined the lead times and corresponding overdiagnosis rates that were consistent with the observed data.

RESULTS

SEER data on prostate cancer incidence from 1988 through 1998 were consistent with overdiagnosis rates of approximately 29% for whites and 44% for blacks among men with prostate cancers detected by PSA screening.

CONCLUSIONS

Among men with prostate cancer that would be detected only at autopsy, these rates correspond to overdiagnosis rates of, at most, 15% in whites and 37% in blacks. The observed trends in prostate cancer incidence are consistent with considerable overdiagnosis among PSA-detected cases. However, the results suggest that the majority of screen-detected cancers diagnosed between 1988 and 1998 would have presented clinically and that only a minority of cases found at autopsy would have been detected by PSA testing.

摘要

背景

临床意义不显著的前列腺癌的过度诊断被认为是前列腺特异性抗原(PSA)筛查的一个主要潜在缺陷。然而,目前缺乏对这一问题严重程度的定量估计。我们估算了1988年至1998年期间,因PSA检测导致的前列腺癌过度诊断率,这些比率与美国观察到的前列腺癌发病率相符。过度诊断被定义为通过PSA检测发现的前列腺癌,而这些癌症在患者一生中原本不会被诊断出来。

方法

我们建立了一个计算机模拟模型,用于模拟1988年年龄在60 - 84岁之间的两百万男性假想队列中PSA检测以及随后的前列腺癌诊断和前列腺癌死亡情况。给定预期提前期(即检测使诊断提前的时间)以及在无PSA检测情况下前列腺癌的预期发病率的值,该模型预测了与PSA检测相关的前列腺癌人群发病率的增加。通过将模型预测的发病率与从美国国家癌症研究所的监测、流行病学和最终结果(SEER)登记数据得出的观察发病率进行比较,我们确定了与观察数据相符的提前期和相应的过度诊断率。

结果

1988年至1998年SEER关于前列腺癌发病率的数据表明,在通过PSA筛查检测出的前列腺癌男性中,白人的过度诊断率约为29%,黑人约为44%。

结论

在那些仅在尸检时才会被发现患有前列腺癌的男性中,这些比率对应的白人过度诊断率最高为15%,黑人最高为37%。观察到的前列腺癌发病率趋势与PSA检测出的病例中存在相当程度的过度诊断相符。然而,结果表明,1988年至1998年期间通过筛查发现并诊断的大多数癌症在临床上都会出现,并且只有少数尸检时发现的病例会通过PSA检测被发现。

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