多基因风险评分在前列腺癌筛查中的评估
Assessment of a Polygenic Risk Score in Screening for Prostate Cancer.
作者信息
McHugh Jana K, Bancroft Elizabeth K, Saunders Edward, Brook Mark N, McGrowder Eva, Wakerell Sarah, James Denzil, Rageevakumar Reshma, Benton Barbara, Taylor Natalie, Myhill Kathryn, Hogben Matthew, Kinsella Netty, Sohaib Aslam A, Cahill Declan, Hazell Stephen, Withey Samuel J, Mcaddy Naami, Page Elizabeth C, Osborne Andrea, Benafif Sarah, Jones Ann-Britt, Patel Dhruv, Huang Dean Y, Kaur Kaljit, Russell Bradley, Nicholson Ray, Croft Fionnuala, Sobczak Justyna, McNally Claire, Mutch Fiona, Bennett Samantha, Kingston Lenita, Karlsson Questa, Dadaev Tokhir, Saya Sibel, Merson Susan, Wood Angela, Dennis Nening, Hussain Nafisa, Thwaites Alison, Hussain Syed, Rafi Imran, Ferris Michelle, Kumar Pardeep, James Nicholas D, Pashayan Nora, Kote-Jarai Zsofia, Eeles Rosalind A
机构信息
Institute of Cancer Research, London.
Royal Marsden NHS Foundation Trust, London.
出版信息
N Engl J Med. 2025 Apr 10;392(14):1406-1417. doi: 10.1056/NEJMoa2407934.
BACKGROUND
The incidence of prostate cancer is increasing. Screening with an assay of prostate-specific antigen (PSA) has a high rate for false positive results. Genomewide association studies have identified common germline variants in persons with prostate cancer, which can be used to calculate a polygenic risk score associated with risk of prostate cancer.
METHODS
We recruited persons 55 to 69 years of age from primary care centers in the United Kingdom. Using germline DNA extracted from saliva, we derived polygenic risk scores from 130 variants known to be associated with an increased risk of prostate cancer. Participants with a polygenic risk score in the 90th percentile or higher were invited to undergo prostate cancer screening with multiparametric magnetic resonance imaging (MRI) and transperineal biopsy, irrespective of PSA level.
RESULTS
Among 40,292 persons invited to participate, 8953 (22.2%) expressed interest in participating and 6393 had their polygenic risk score calculated; 745 (11.7%) had a polygenic risk score in the 90th percentile or higher and were invited to undergo screening. Of these 745 participants, 468 (62.8%) underwent MRI and prostate biopsy; prostate cancer was detected in 187 participants (40.0%). The median age at diagnosis was 64 years (range, 57 to 73). Of the 187 participants with cancer, 103 (55.1%) had prostate cancer classified as intermediate or higher risk according to the 2024 National Comprehensive Cancer Network (NCCN) criteria, so treatment was indicated; cancer would not have been detected in 74 (71.8%) of these participants according to the prostate cancer diagnostic pathway currently used in the United Kingdom (high PSA level and positive MRI results). In addition, 40 of the participants with cancer (21.4%) had disease classified as unfavorable intermediate risk or as high or very high risk according to NCCN criteria.
CONCLUSIONS
In a prostate cancer screening program involving participants in the top decile of risk as determined by a polygenic risk score, the percentage found to have clinically significant disease was higher than the percentage that would have been identified with the use of PSA or MRI. (Funded by the European Research Council Seventh Framework Program and others; BARCODE1 ClinicalTrials.gov number, NCT03857477.).
背景
前列腺癌的发病率正在上升。采用前列腺特异性抗原(PSA)检测进行筛查的假阳性率很高。全基因组关联研究已经在前列腺癌患者中确定了常见的种系变异,这些变异可用于计算与前列腺癌风险相关的多基因风险评分。
方法
我们从英国的基层医疗中心招募了55至69岁的人群。使用从唾液中提取的种系DNA,我们从130个已知与前列腺癌风险增加相关的变异中得出多基因风险评分。多基因风险评分处于第90百分位或更高的参与者被邀请接受多参数磁共振成像(MRI)和经会阴活检进行前列腺癌筛查,无论其PSA水平如何。
结果
在受邀参与的40292人中,8953人(22.2%)表示有兴趣参与,6393人的多基因风险评分被计算出来;745人(11.7%)的多基因风险评分处于第90百分位或更高,并被邀请进行筛查。在这745名参与者中,468人(62.8%)接受了MRI和前列腺活检;187名参与者(40.0%)检测出前列腺癌。诊断时的中位年龄为64岁(范围57至73岁)。在这187名癌症患者中,根据2024年美国国立综合癌症网络(NCCN)标准,103人(55.1%)的前列腺癌被分类为中度或更高风险,因此需要进行治疗;根据英国目前使用的前列腺癌诊断途径(高PSA水平和MRI结果阳性),这些参与者中有74人(71.8%)不会被检测出患有癌症。此外,40名癌症患者(21.4%)的疾病根据NCCN标准被分类为不良中度风险或高风险或非常高风险。
结论
在一项前列腺癌筛查计划中,对于多基因风险评分处于最高十分位的参与者,发现患有具有临床意义疾病的百分比高于使用PSA或MRI所能识别的百分比。(由欧洲研究理事会第七框架计划及其他机构资助;BARCODE1临床试验注册号,NCT03857477。)
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