Department of Epidemiology and Cancer Control, St. Jude Children's Research Hospital, Memphis, Tennessee.
School of Public Health, University of Alberta, Edmonton, Alberta, Canada.
Cancer Res. 2020 Sep 1;80(17):3755-3764. doi: 10.1158/0008-5472.CAN-20-0093. Epub 2020 Jun 17.
Exposure to high doses of alkylating agents is associated with increased risk of impaired spermatogenesis among nonirradiated male survivors of childhood cancer, but there is substantial variation in this risk. Here we conducted a genetic study for impaired spermatogenesis utilizing whole-genome sequencing data from 167 nonirradiated male childhood cancer survivors of European ancestry from the St. Jude Lifetime Cohort treated with cyclophosphamide equivalent dose (CED) ≥4,000 mg/m. Sperm concentration from semen analysis was assessed as the primary outcome. Common variants (MAF > 0.05) were adjusted for age at cancer diagnosis, CED, and top principal components. Rare/low-frequency variants (MAF ≤ 0.05) were evaluated jointly by various functional annotations and 4-kb sliding windows. A novel locus at 7q21.3 containing / was associated with decreased sperm concentration (rs7784118: = 3.5 × 10). This association was replicated in two independent samples of SJLIFE survivors of European ancestry, including 34 nonirradiated male survivors treated with 0 < CED < 4,000 mg/m ( = 3.1 × 10) and 24 male survivors treated with CED ≥4,000 mg/m and radiotherapy <40 Gray ( = 0.012). No association was observed among survivors not exposed to alkylating agents included in the CED ( > 0.29). rs7784118 conferred 3.48- and 9.73-fold increases in risk for clinically defined oligospermia and azoospermia and improved prediction of normospermic, oligospermic, and azoospermic states by 13.7%, 5.3%, and 21.7%. rs7784118 was associated with decreased testosterone level, increased levels of follicle stimulating and luteinizing hormones, and 8.52-fold increased risk of Leydig cell failure. Additional research is warranted to determine how this SNP influences spermatogenesis and to assess its clinical utility in characterizing high-risk survivors and guiding intervention strategies. SIGNIFICANCE: The identified genetic markers harbor potential clinical utility in characterizing high-risk survivors and guiding intervention strategies including pretreatment patient counseling and use of fertility preservation services.
暴露于高剂量的烷化剂会增加非放射性儿童癌症幸存者的生殖细胞受损的风险,但这种风险存在很大差异。在这里,我们利用来自欧洲血统的 167 名接受环磷酰胺等效剂量(CED)≥4000mg/m 的非放射性儿童癌症幸存者的全基因组测序数据进行了一项生殖细胞受损的遗传研究。精液分析中的精子浓度被评估为主要结局。常见变体(MAF>0.05)根据癌症诊断时的年龄、CED 和主要成分进行调整。罕见/低频变体(MAF≤0.05)通过各种功能注释和 4-kb 滑动窗口进行联合评估。一个包含 / 的新型 7q21.3 基因座与精子浓度降低相关(rs7784118: = 3.5×10)。这一关联在两个独立的 SJLIFE 欧洲血统幸存者样本中得到了复制,包括 34 名接受 0 <CED <4000mg/m 的非放射性男性幸存者( = 3.1×10)和 24 名接受 CED≥4000mg/m 和放疗 <40 Gray 的男性幸存者( = 0.012)。在未暴露于 CED 中包含的烷化剂的幸存者中未观察到关联(>0.29)。rs7784118 使临床上定义的少精子症和无精子症的风险分别增加了 3.48 倍和 9.73 倍,并将正常精子症、少精子症和无精子症状态的预测提高了 13.7%、5.3%和 21.7%。rs7784118 与睾酮水平降低、卵泡刺激素和黄体生成素水平升高以及 Leydig 细胞衰竭的风险增加 8.52 倍相关。需要进一步研究以确定该 SNP 如何影响生殖细胞,并评估其在描述高危幸存者和指导干预策略方面的临床实用性。意义:所确定的遗传标记具有潜在的临床实用性,可用于描述高危幸存者并指导干预策略,包括治疗前患者咨询和使用生育保护服务。
