Ajaj Rand, Gershon Andrea S, Lau Cindy, Gupta Sumit, Baxter Nancy N, Sutradhar Rinku, Pole Jason D, Shaikh Furqan, Nathan Paul C
Institute of Medical Science, Temerty Faculty of Medicine, University of Toronto, Toronto, Ontario, Canada.
The Hospital for Sick Children Research Institute, Child Health Evaluative Sciences, Toronto, Ontario, Canada.
Int J Cancer. 2025 Nov 1;157(9):1841-1852. doi: 10.1002/ijc.70017. Epub 2025 Jun 24.
While testicular germ cell tumors (TGCT) are highly curable, survivors experience toxicities. Pulmonary outcomes post-TGCT are not well understood, particularly among children, adolescents, and young adults (CAYA). Using provincial cancer registries, we identified all CAYA (aged 11-21 years) diagnosed with a TGCT from 1992 to 2021 in Ontario, Canada, and matched them (1:5) to general population males (controls). We linked CAYA to health administrative databases to identify pulmonary disease and pulmonary disease healthcare visits (PDV) and classified PDV severity as low (outpatient family physician/pediatrician), medium (outpatient respirologist/internist), or high (hospitalization/emergency department). We assessed acute (<5 years from diagnosis) and late (≥5 years after diagnosis) toxicities using the cumulative incidence function and cause-specific hazard models. We identified 748 patients (404 chemotherapy-treated) and 3740 controls. Patients' median age at diagnosis was 19.0 years [interquartile range (IQR):18.0-21.0] and 29.7 years (IQR:25.0-37.6) at end of follow-up. Non-chemotherapy-treated patients had higher risk of acute toxicities (obstructive lung disease, medium severity PDV, hospitalizations) but similar risk of late toxicities to controls. Chemotherapy-treated patients had higher risk than controls of most acute pulmonary toxicities (except asthma and low severity PDV) and several late toxicities: asthma [hazard ratio (HR) = 2.0, 95%CI:1.1-3.8], pulmonary embolism/infarction (HR = 7.3, 95%CI:1.2-44.3), medium severity PDV (HR = 3.9, 95%CI:2.1-7.3), and high severity PDV (HR = 1.7, 95%CI:1.0-2.8), particularly hospitalizations (HR = 4.1, 95%CI:1.7-9.5). CAYA TGCT survivors treated with chemotherapy are at risk for late asthma, pulmonary embolism, pulmonary fibrosis, and specialist and hospital-based pulmonary care. Further follow-up is needed to characterize late pulmonary outcomes as survivors age.
虽然睾丸生殖细胞肿瘤(TGCT)的治愈率很高,但幸存者会出现毒性反应。TGCT治疗后的肺部转归情况尚不清楚,尤其是在儿童、青少年和青年(CAYA)中。利用省级癌症登记处的数据,我们确定了1992年至2021年在加拿大安大略省被诊断为TGCT的所有CAYA(年龄在11至21岁之间),并将他们与普通人群中的男性(对照)进行(1:5)匹配。我们将CAYA与卫生行政数据库相链接,以确定肺部疾病和肺部疾病医疗就诊情况(PDV),并将PDV严重程度分为低(门诊家庭医生/儿科医生)、中(门诊呼吸科医生/内科医生)或高(住院/急诊科)。我们使用累积发病率函数和特定病因风险模型评估急性(诊断后<5年)和晚期(诊断后≥5年)毒性反应。我们确定了748例患者(404例接受化疗)和3740例对照。患者诊断时的中位年龄为19.0岁[四分位间距(IQR):18.0 - 21.0],随访结束时为29.7岁(IQR:25.0 - 37.6)。未接受化疗的患者急性毒性反应(阻塞性肺病、中度严重程度的PDV、住院)风险较高,但晚期毒性反应风险与对照相似。接受化疗的患者大多数急性肺部毒性反应(哮喘和低严重程度的PDV除外)以及几种晚期毒性反应的风险高于对照:哮喘[风险比(HR)=2.0,95%置信区间(CI):1.1 - 3.8]、肺栓塞/梗死(HR = 7.3,95%CI:1.2 - 44.3)、中度严重程度的PDV(HR = 3.9,95%CI:2.1 - 7.3)和高度严重程度的PDV(HR = 1.7,95%CI:1.0 - 2.8),尤其是住院(HR = 4.1,95%CI:1.7 - 9.5)。接受化疗的CAYA TGCT幸存者有患晚期哮喘、肺栓塞、肺纤维化以及专科和住院肺部护理的风险。随着幸存者年龄增长,需要进一步随访以明确晚期肺部转归情况。
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