Wan Qiting, Hu Li, Ouyang Tao, Li Jinfeng, Wang Tianfeng, Fan Zhaoqing, Fan Tie, Lin Benyao, Xu Ye, Xie Yuntao
Breast Center, Key Laboratory of Carcinogenesis and Translational Research (Ministry of Education/Beijing), Peking University Cancer Hospital & Institute, 52 Fucheng Road, Haidian District, Beijing, 100142, People's Republic of China.
Fam Cancer. 2021 Apr;20(2):85-95. doi: 10.1007/s10689-020-00202-4. Epub 2020 Aug 17.
Characterizing the pathogenicity of BRCA1 variants of uncertain significance (VUSs) is a major bottleneck in clinical management of BRCA1-associated breast cancer. Saturation genome editing (SGE) was recently reported as an innovative laboratory-based approach to assess the pathogenicity of BRCA1 variants. We combined clinical phenotypes and SGE score to identify the pathogenicity of BRCA1 VUSs detected in a cohort of 8,085 breast cancer patients. According to SGE function score, 33 out of 144 BRCA1 VUSs detected were classified into "loss of function" (n = 13), "intermediate" (n = 2), and "functional" (n = 18) groups. Compared with non-carriers, "loss of function" VUS carriers (n = 19) presented significantly worse clinicopathological characteristics. These included younger age at breast cancer diagnosis (44.4 years vs. 51.2 years, P = 0.01), stronger family history of any cancer (57.9% vs. 32.3%, P = 0.017) especially breast or ovarian cancer (47.4% vs. 9.3%, P < 0.001), more bilateral breast cancer (31.6% vs. 3.4%, P < 0.001), and triple-negative breast cancer (47.4% vs. 12.8%, P < 0.001), which were comparable to those of pathogenic variant carriers. In contrast, the clinical phenotypes of "functional" VUS carriers were similar to those of non-carriers. These results indicated that SGE was a reliable method in BRCA1 variant classification. Combining SGE function score and the available evidence, twelve out of 33 BRCA1 VUSs were reclassified as pathogenic or likely pathogenic variants and one was benign.
确定意义不明确的BRCA1变异(VUS)的致病性是BRCA1相关乳腺癌临床管理中的一个主要瓶颈。最近有报道称,饱和基因组编辑(SGE)是一种基于实验室的创新方法,用于评估BRCA1变异的致病性。我们结合临床表型和SGE评分,以确定在8085例乳腺癌患者队列中检测到的BRCA1 VUS的致病性。根据SGE功能评分,在检测到的144个BRCA1 VUS中,有33个被分为“功能丧失”(n = 13)、“中间型”(n = 2)和“功能型”(n = 18)组。与非携带者相比,“功能丧失”VUS携带者(n = 19)的临床病理特征明显更差。这些特征包括乳腺癌诊断时年龄更小(44.4岁对51.2岁,P = 0.01)、任何癌症的家族史更强(57.9%对32.3%,P = 0.017),尤其是乳腺癌或卵巢癌(47.4%对9.3%,P < 0.001)、更多双侧乳腺癌(31.6%对3.4%,P < 0.001)和三阴性乳腺癌(47.4%对12.8%,P < 0.001),这些与致病性变异携带者的特征相当。相比之下,“功能型”VUS携带者的临床表型与非携带者相似。这些结果表明,SGE是BRCA1变异分类中的一种可靠方法。结合SGE功能评分和现有证据,33个BRCA1 VUS中有12个被重新分类为致病性或可能致病性变异,1个为良性变异。
