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瑞典前列腺癌患者亲属的前列腺癌发病风险:一项全国性队列研究。

Risk of prostate cancer in relatives of prostate cancer patients in Sweden: A nationwide cohort study.

机构信息

Division of Preventive Oncology, National Center for Tumor Diseases (NCT), German Cancer Research Center (DKFZ), Heidelberg, Germany.

Medical Faculty Heidelberg, Heidelberg University, Heidelberg, Germany.

出版信息

PLoS Med. 2021 Jun 1;18(6):e1003616. doi: 10.1371/journal.pmed.1003616. eCollection 2021 Jun.

Abstract

BACKGROUND

Evidence-based guidance for starting ages of screening for first-degree relatives (FDRs) of patients with prostate cancer (PCa) to prevent stage III/IV or fatal PCa is lacking in current PCa screening guidelines. We aimed to provide evidence for risk-adapted starting age of screening for relatives of patients with PCa.

METHODS AND FINDINGS

In this register-based nationwide cohort study, all men (aged 0 to 96 years at baseline) residing in Sweden who were born after 1931 along with their fathers were included. During the follow-up (1958 to 2015) of 6,343,727 men, 88,999 were diagnosed with stage III/IV PCa or died of PCa. The outcomes were defined as the diagnosis of stage III/IV PCa or death due to PCa, stratified by age at diagnosis. Using 10-year cumulative risk curves, we calculated risk-adapted starting ages of screening for men with different constellations of family history of PCa. The 10-year cumulative risk of stage III/IV or fatal PCa in men at age 50 in the general population (a common recommended starting age of screening) was 0.2%. Men with ≥2 FDRs diagnosed with PCa reached this screening level at age 41 (95% confidence interval (CI): 39 to 44), i.e., 9 years earlier, when the youngest one was diagnosed before age 60; at age 43 (41 to 47), i.e., 7 years earlier, when ≥2 FDRs were diagnosed after age 59, which was similar to that of men with 1 FDR diagnosed before age 60 (41 to 45); and at age 45 (44 to 46), when 1 FDR was diagnosed at age 60 to 69 and 47 (46 to 47), when 1 FDR was diagnosed after age 69. We also calculated risk-adapted starting ages for other benchmark screening ages, such as 45, 55, and 60 years, and compared our findings with those in the guidelines. Study limitations include the lack of genetic data, information on lifestyle, and external validation.

CONCLUSIONS

Our study provides practical information for risk-tailored starting ages of PCa screening based on nationwide cancer data with valid genealogical information. Our clinically relevant findings could be used for evidence-based personalized PCa screening guidance and supplement current PCa screening guidelines for relatives of patients with PCa.

摘要

背景

目前的前列腺癌(PCa)筛查指南缺乏针对 PCa 患者一级亲属(FDR)筛查起始年龄的循证指导,以预防 III/IV 期或致命性 PCa。我们旨在为基于风险的 FDR 筛查起始年龄提供证据。

方法和发现

在这项基于登记的全国性队列研究中,纳入了所有(在基线时年龄为 0 至 96 岁)出生于 1931 年以后居住在瑞典的男性及其父亲。在 6343727 名男性的随访(1958 年至 2015 年)期间,有 88999 人被诊断为 III/IV 期 PCa 或死于 PCa。结果定义为诊断为 III/IV 期 PCa 或死于 PCa,按诊断时的年龄分层。使用 10 年累积风险曲线,我们计算了不同家族史男性的风险适应筛查起始年龄。在普通人群(普遍推荐的筛查起始年龄为 50 岁)中,50 岁男性 10 年累积 III/IV 期或致命性 PCa 风险为 0.2%。至少有 2 个 FDR 被诊断为 PCa 的男性,当最小的 FDR 在 60 岁之前被诊断时,他们达到该筛查水平的年龄为 41 岁(95%置信区间:39 至 44),即早 9 年;当 2 个 FDR 在 59 岁以后被诊断时,他们达到该筛查水平的年龄为 43 岁(41 至 47),即早 7 年;当 1 个 FDR 在 60 岁至 69 岁被诊断时,他们达到该筛查水平的年龄为 45 岁(44 至 46),当 1 个 FDR 在 69 岁以后被诊断时,他们达到该筛查水平的年龄为 47 岁(46 至 47),与在 60 岁之前被诊断为 1 个 FDR 的男性相似(41 至 45)。我们还计算了其他基准筛查年龄(如 45 岁、55 岁和 60 岁)的风险适应筛查起始年龄,并将我们的发现与指南中的发现进行了比较。研究的局限性包括缺乏遗传数据、生活方式信息和外部验证。

结论

我们的研究基于具有有效家族史信息的全国癌症数据,为基于风险的 PCa 筛查起始年龄提供了实用信息。我们具有临床相关性的发现可用于基于证据的个性化 PCa 筛查指导,并补充现有的 PCa 筛查指南,为 PCa 患者的亲属提供指导。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/365a/8168897/36b1bfa16a0f/pmed.1003616.g001.jpg

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