前列腺癌筛查:欧洲前列腺癌筛查随机研究鹿特丹部分的结果。
Screening for prostate cancer: results of the Rotterdam section of the European randomized study of screening for prostate cancer.
机构信息
Department of Urology, Erasmus University Medical Center, Rotterdam, The Netherlands.
出版信息
Eur Urol. 2013 Oct;64(4):530-9. doi: 10.1016/j.eururo.2013.05.030. Epub 2013 May 25.
BACKGROUND
Evidence from randomized trials on the effects of screening for prostate cancer (PCa) on disease-specific mortality accumulates slowly with increasing follow-up.
OBJECTIVE
To assess data on PCa-specific mortality in the Rotterdam section of the European Randomized Study of Screening for Prostate Cancer (ERSPC) trial.
DESIGN, SETTING, AND PARTICIPANTS: A randomized controlled trial with randomization after signed, written informed consent (efficacy trial). In the period 1993-1999, a total of 42 376 men aged 54-74 yr were randomized to a screening arm (S-arm) (n = 21 210 with screening every 4 yr, applying a total prostate-specific antigen [PSA] level cut-off ≥ 3.0 ng/ml as biopsy indication) or a control arm (C-arm) (n = 21 166; no intervention).
OUTCOME MEASUREMENTS AND STATISTICAL ANALYSIS
Number of PCas detected per arm depicted by predefined time periods and prognostic groups. PCa-specific mortality analyses using Poisson regression in age group 55-74 yr at randomization and separately in the predefined age group of 55-69 yr.
RESULTS AND LIMITATIONS
After a median follow-up of 12.8 yr, 19 765 men (94.2%) were screened at least once and 2674 PCas were detected (of which 561 [21.0%] were interval PCas). In the C-arm, 1430 PCas were detected, resulting in an excess incidence of 59 PCas per 1000 men randomized (61 PCas per 1000 in age group 55-69 yr). Thirty-two percent of all men randomized have died. PCa-specific mortality relative-risk (RR) reductions of 20.0% overall (age: 55-74 yr; p = 0.042) and 31.6% (age: 55-69 yr; p = 0.004) were found. A 14.1% increase was found in men aged 70-74 yr (not statistically significant). Absolute PCa mortality was 1.8 per 1000 men randomized (2.6 per 1000 men randomized in age group 55-69 yr). The number needed to invite and number needed to manage were 565 and 33, respectively, for age group 55-74 yr, and 392 and 24, respectively, for age group 65-69 yr. Given the slow natural history of the disease, follow-up might be too short.
CONCLUSIONS
Systematic PSA-based screening reduced PCa-specific mortality by 32% in the age range of 55-69 yr. The roughly twofold higher incidence in the S-arm underlines the importance of tools to better identify those men who would benefit from screening.
背景
有关前列腺癌(PCa)筛查对疾病特异性死亡率影响的随机试验证据随着随访时间的延长而缓慢积累。
目的
评估欧洲前列腺癌筛查随机研究(ERSPC)中 Rotterdam 部分的 PCa 特异性死亡率数据。
设计、地点和参与者:这是一项基于随机、签署书面知情同意书后的对照临床试验(有效性试验)。在 1993 年至 1999 年期间,共有 42376 名年龄在 54-74 岁的男性被随机分配至筛查组(S 组)(n=21210,每 4 年筛查一次,应用总前列腺特异性抗原[PSA]水平截断值≥3.0ng/ml 作为活检指征)或对照组(C 组)(n=21166;无干预)。
观察指标和统计分析
通过预设时间段和预后组描述每个手臂检测到的 PCa 数量。使用 Poisson 回归分析年龄组为 55-74 岁的随机分组和 55-69 岁的预设年龄组的 PCa 特异性死亡率。
结果和局限性
中位随访 12.8 年后,19765 名男性(94.2%)至少接受了一次筛查,共检出 2674 例 PCa(其中 561 例[21.0%]为间隔性 PCa)。C 组检出 1430 例 PCa,导致每 1000 名随机分配的男性中发病率增加 59 例(55-69 岁年龄组为每 1000 例增加 61 例)。32%的随机分配男性死亡。总体 PCa 特异性死亡率相对风险(RR)降低 20.0%(年龄:55-74 岁;p=0.042)和 31.6%(年龄:55-69 岁;p=0.004)。70-74 岁年龄组的 RR 增加 14.1%(无统计学意义)。每 1000 名随机分配的男性的绝对 PCa 死亡率为 1.8 例(55-69 岁年龄组为每 1000 名随机分配的男性 2.6 例)。对于年龄组 55-74 岁的男性,需要邀请的人数和需要管理的人数分别为 565 人和 33 人,对于年龄组 65-69 岁的男性,需要邀请的人数和需要管理的人数分别为 392 人和 24 人。考虑到疾病的自然病程缓慢,随访时间可能太短。
结论
基于 PSA 的系统性筛查将 55-69 岁年龄组的 PCa 特异性死亡率降低了 32%。S 组的发病率约为两倍,这突出了需要更好地识别那些将受益于筛查的男性的工具的重要性。
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