Laboratory for Genotyping Development, RIKEN Center for Integrative Medical Sciences, Yokohama City, Kanagawa, Japan.
Department of Genetic Medicine and Services, National Cancer Centre Hospital, Chuo-ku, Tokyo, Japan.
J Natl Cancer Inst. 2020 Apr 1;112(4):369-376. doi: 10.1093/jnci/djz124.
Genetic testing has been conducted in patients with prostate cancer (PCa) using multigene panels, but no centralized guidelines for genetic testing exist. To overcome this limitation, we investigated the demographic and clinical characteristics of patients with pathogenic variants.
We sequenced eight genes associated with hereditary PCa in 7636 unselected Japanese patients with PCa and 12 366 male, cancer-free control individuals. We assigned clinical significance for all 1456 variants using the American College of Medical Genetics and Genomics guidelines and ClinVar. We compared the frequency of carriers bearing pathogenic variants between cases and control participants with calculated PCa risk in each gene and documented the demographic and clinical characteristics of patients bearing pathogenic variants. All statistical tests were two-sided.
We identified 136 pathogenic variants, and 2.9% of patients and 0.8% of control individuals had a pathogenic variant. Association with PCa risk was statistically significant for variants in BRCA2 (P < .001, odds ratio [OR] = 5.65, 95% confidence interval [CI] = 3.55 to 9.32), HOXB13 (P < .001, OR = 4.73, 95% CI = 2.84 to 8.19), and ATM (P < .001, OR = 2.86, 95% CI = 1.63 to 5.15). We detected recurrent new pathogenic variants such as p.Gly132Glu of HOXB13. Patients with pathogenic variants were 2.0 years younger at diagnosis and more often had smoking and alcohol drinking histories as well as family histories of breast, pancreatic, lung, and liver cancers.
This largest sequencing study of PCa heredity provides additional evidence supporting the latest consensus among clinicians for developing genetic testing guidelines for PCa.
已经使用多基因panel 对前列腺癌 (PCa) 患者进行了基因检测,但尚无针对基因检测的集中指南。为了克服这一局限性,我们调查了具有致病性变异的患者的人口统计学和临床特征。
我们对 7636 名未选择的日本 PCa 患者和 12366 名男性无癌对照个体进行了与遗传性 PCa 相关的 8 个基因的测序。我们使用美国医学遗传学与基因组学学院和 ClinVar 指南对所有 1456 个变体进行了临床意义分配。我们比较了每个基因中携带致病性变异的病例和对照参与者的 PCa 风险频率,并记录了携带致病性变异的患者的人口统计学和临床特征。所有统计检验均为双侧。
我们鉴定出 136 种致病性变异,2.9%的患者和 0.8%的对照个体存在致病性变异。BRCA2 中的变异与 PCa 风险相关(P<0.001,优势比 [OR] = 5.65,95%置信区间 [CI] = 3.55 至 9.32),HOXB13(P<0.001,OR = 4.73,95% CI = 2.84 至 8.19)和 ATM(P<0.001,OR = 2.86,95% CI = 1.63 至 5.15)。我们检测到了HOXB13 中 p.Gly132Glu 等新的复发性致病性变异。携带致病性变异的患者在诊断时年轻 2.0 岁,并且更常具有吸烟和饮酒史以及乳腺癌、胰腺癌、肺癌和肝癌家族史。
这是最大规模的 PCa 遗传测序研究,为制定 PCa 遗传检测指南提供了更多证据,支持了临床医生的最新共识。
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