A Polygenic Risk Score for Late Bladder Toxicity Following Radiotherapy for Non-Metastatic Prostate Cancer.

IF 3.7 3区医学 Q2 ONCOLOGY

Cancer Epidemiology Biomarkers & Prevention Pub Date : 2025-05-02 DOI:10.1158/1055-9965.EPI-24-1228

Manzur Farazi, Xin Yang, Carson J Gehl, Gillian C Barnett, Neil G Burnet, Jenny Chang-Claude, Christopher C Parker, Alison M Dunning, David Azria, Ananya Choudhury, Tiziana Rancati, Dirk De Ruysscher, Petra Seibold, Elena Sperk, Christopher J Talbot, Liv Veldeman, Adam J Webb, Rebecca Elliott, Miguel E Aguado-Barrera, Ana M Carballo, Olivia Fuentes-Ríos, Antonio Gómez-Caamaño, Paula Peleteiro, Ana Vega, Harry Ostrer, Barry S Rosenstein, Shiro Saito, Matthew Parliament, Nawaid Usmani, Brian Marples, Yuhchyau Chen, Gary Morrow, Edward Messing, Michelle C Janelsins, William Hall, Catharine M L West, Paul L Auer, Sarah L Kerns

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引用次数: 0

Abstract

Background: Late bladder toxicity is a concern for patients receiving prostate cancer radiotherapy and negatively affects survivors. Few risk factors are known beyond the radiation dose and volume of bladder exposed. A polygenic risk score (PRS) could identify susceptible patients.

Methods: A PRS was built using genome-wide association results from the Radiogenomics Consortium (N = 3,988) and then tested in the prospective REQUITE and URWCI studies (N = 2,034). The primary outcome was time to patient-reported gross [grade ≥2, (≥G2)] hematuria, analyzed using Cox proportional hazards regression. Secondary outcomes were ≥G2 urinary retention and frequency. The PRS was externally validated for clinically diagnosed irradiation cystitis in the UK Biobank (N = 8,430). A gene-burden test evaluated rare coding variants.

Results: A 115-variant PRS was associated with a significantly increased risk of ≥G2 hematuria [hazard ratio (HR) per SD = 1.22; P = 0.009] as well as urinary retention (HR per SD = 1.18; P = 0.016) and frequency (HR per SD = 1.14; P = 0.036). When binarized, men in the upper decile (PRShigh) had a >2-fold increased risk of hematuria after adjusting for clinical risk factors [HR = 2.12; P = 0.002; Harrel's concordance index = 0.71 (95% confidence interval, 0.65-0.76)]. A similar effect size was seen in the UK Biobank for clinically diagnosed irradiation cystitis [odds ratio (OR) = 2.15; P = 0.026]. The burden test identified BOD1L1 as a putative novel radiosensitivity gene.

Conclusions: This PRS identifies susceptible patients and could guide the selection of those needing reoptimized treatment plans that spare the bladder beyond currently recommended constraints.

Impact: PRS-guided treatment planning in radiation oncology could lower the incidence of clinically relevant bladder toxicity and reduce the impact of this outcome on prostate cancer survivors.

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非转移性前列腺癌放疗后晚期膀胱毒性的多基因风险评分。

背景：晚期膀胱毒性是前列腺癌放疗患者关注的问题，对幸存者有负面影响。除了辐射剂量和膀胱暴露量之外，几乎没有其他已知的危险因素。多基因风险评分（PRS）可以识别易感患者。方法：利用放射基因组学联盟（Radiogenomics Consortium）的全基因组关联结果（N= 3988）建立PRS，然后在REQUITE和URWCI前瞻性研究（N= 2034）中进行测试。主要终点是患者报告总血尿时间（≥2级，G2），使用Cox比例风险回归分析。次要结局为≥G2尿潴留和尿频。PRS在英国生物银行（UK Biobank）进行了临床诊断的放射性膀胱炎的外部验证（N=8,430）。基因负荷测试评估罕见的编码变异。结果：115个变异的PRS与≥G2血尿（每标准差[SD]的风险比[HR] =1.22, p=0.009）、尿潴留（HR-per-SD=1.18, p=0.016）和尿频（HR-per-SD=1.14, p=0.036）的风险显著增加相关。当二值化时，在调整临床危险因素后，上十分位数（prhigh）的男性血尿风险增加了2倍(HR=2.12, p=0.002；Harrel’s c指数0.71 [95%CI=0.65 ~ 0.76])。在UK Biobank中，临床诊断的放射性膀胱炎也出现了类似的效应值（OR=2.15, p=0.026）。负荷试验确定BOD1L1为推测的新型放射敏感基因。结论：该PRS识别了易感患者，并可以指导选择那些需要重新优化治疗方案的患者，以避免膀胱超出目前推荐的限制。影响：prs指导的放射肿瘤学治疗方案可以降低临床相关膀胱毒性的发生率，并减少该结果对前列腺癌幸存者的影响。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Cancer Epidemiology Biomarkers & Prevention 医学-公共卫生、环境卫生与职业卫生

CiteScore

6.50

自引率

2.60%

发文量

538

审稿时长

1.6 months

期刊介绍： Cancer Epidemiology, Biomarkers & Prevention publishes original peer-reviewed, population-based research on cancer etiology, prevention, surveillance, and survivorship. The following topics are of special interest: descriptive, analytical, and molecular epidemiology; biomarkers including assay development, validation, and application; chemoprevention and other types of prevention research in the context of descriptive and observational studies; the role of behavioral factors in cancer etiology and prevention; survivorship studies; risk factors; implementation science and cancer care delivery; and the science of cancer health disparities. Besides welcoming manuscripts that address individual subjects in any of the relevant disciplines, CEBP editors encourage the submission of manuscripts with a transdisciplinary approach.