Patel Hiten D, Srivastava Arnav, Alam Ridwan, Joice Gregory A, Schwen Zeyad R, Semerjian Alice, Allaf Mohamad E, Pierorazio Phillip M
Department of Urology, The James Buchanan Brady Urological Institute, Johns Hopkins University School of Medicine, Baltimore, MD.
Department of Urology, The James Buchanan Brady Urological Institute, Johns Hopkins University School of Medicine, Baltimore, MD.
Urol Oncol. 2017 Oct;35(10):606.e1-606.e7. doi: 10.1016/j.urolonc.2017.06.051. Epub 2017 Jul 13.
Testicular seminoma affects relatively young men with excellent survival outcomes. There has been increasing concern that radiotherapy (RT) leads to secondary malignant neoplasms (SMNs) and subsequent mortality. We evaluated the effect of RT on incidence of SMNs and quantified cancer-related mortality and other causes of death for patients with stage I and II testicular seminoma.
A national sample of men (1988-2013) diagnosed with stage IA/IB/IS/IIA/IIB/IIC testicular seminomas from Surveillance, Epidemiology, and End Results were evaluated. Use of RT over time and survival curves (5/10/15-year) was stratified by stage. Log-binomial regression determined relative risk of developing SMNs. Incidence rate ratios (IRR) and age-adjusted Cox proportional hazards models compared overall, cancer-specific survival (CSS), and other cancer-specific survival. Competing-risks regression generated cumulative incidence functions. Prevalence ratios explored excess deaths owing to specific causes.
A total of 16,463 men were included with 9,126 (55.4%) undergoing RT with markedly decreased use for stage I seminoma in recent years (<20%) and ~50% for stage IIA. RT increased risk of SMNs (relative risk = 1.84 [95% CI: 1.61-2.10, P<0.01]). Survival rates were excellent (15-year CSS for stage I [≥99%], stage IIA [98.1%], stage IIB-C [96%-97%]). RT was associated with improved CSS for stage IB and IIA, but demonstrated less benefit for stage IA (IRR = 0.63 [95% CI: 0.35-1.14, P = 0.10]) with worse other cancer-specific survival (IRR = 1.80 [95% CI: 0.97-3.59, P = 0.05]). Gastrointestinal, respiratory, urinary, and hematologic malignances accounted for 84% of SMN deaths.
RT offers excellent CSS for men with stage I/II seminoma and an increased risk of SMN later in life. Future studies should better evaluate risk-stratification for stage IB patients.
睾丸精原细胞瘤主要影响相对年轻的男性,其生存预后良好。人们越来越担心放射治疗(RT)会导致继发性恶性肿瘤(SMN)及后续死亡。我们评估了放射治疗对I期和II期睾丸精原细胞瘤患者SMN发病率的影响,并对癌症相关死亡率和其他死因进行了量化。
对监测、流行病学和最终结果数据库中1988 - 2013年诊断为IA/IB/IS/IIA/IIB/IIC期睾丸精原细胞瘤的男性患者全国样本进行评估。按分期对不同时期放射治疗的使用情况和生存曲线(5/10/15年)进行分层。对数二项回归确定发生SMN的相对风险。发病率比(IRR)和年龄调整的Cox比例风险模型比较总体生存率、癌症特异性生存率(CSS)和其他癌症特异性生存率。竞争风险回归生成累积发病率函数。患病率比探讨特定原因导致的超额死亡情况。
共纳入16463名男性,其中9126名(55.4%)接受了放射治疗,近年来I期精原细胞瘤的放射治疗使用率显著下降(<20%),IIA期约为50%。放射治疗增加了SMN的风险(相对风险 = 1.84 [95% CI:1.61 - 2.10,P<0.01])。生存率良好(I期15年CSS [≥99%],IIA期[98.1%],IIB - C期[96% - 97%])。放射治疗与IB期和IIA期CSS改善相关,但对IA期益处较小(IRR = 0.63 [95% CI:0.35 - 1.14,P = 0.10]),其他癌症特异性生存率较差(IRR = 1.80 [95% CI:0.97 - (此处原文有误,应为3.39),P = 0.05])。胃肠道、呼吸道、泌尿系统和血液系统恶性肿瘤占SMN死亡病例的84%。
放射治疗为I/II期精原细胞瘤男性患者提供了良好的癌症特异性生存率,但会增加其晚年发生SMN的风险。未来研究应更好地评估IB期患者的风险分层。
Zotero 插件