Buys Saundra S, Sandbach John F, Gammon Amanda, Patel Gayle, Kidd John, Brown Krystal L, Sharma Lavania, Saam Jennifer, Lancaster Johnathan, Daly Mary B
University of Utah School of Medicine, Department of Internal Medicine and Huntsman Cancer Institute, Salt Lake City, Utah.
Texas Oncology Austin, Austin, Texas.
Cancer. 2017 May 15;123(10):1721-1730. doi: 10.1002/cncr.30498. Epub 2017 Jan 13.
As panel testing becomes more common in clinical practice, it is important to understand the prevalence and trends associated with the pathogenic variants (PVs) identified. This is especially true for genetically heterogeneous cancers, such as breast cancer (BC), in which PVs in different genes may be associated with various risks and cancer subtypes. The authors evaluated the outcomes of genetic testing among women who had a personal history of BC.
A total of 35,409 women with a single diagnosis of BC who underwent clinical genetic testing with a 25-gene panel were included in the current analysis. Women with multiple BCs and men with BC were excluded. The frequency and distribution of PVs were assessed for the overall cohort, among women with triple-negative BC (TNBC) (n = 4797), and by age at diagnosis.
PVs were identified in 9.3% of women tested; 51.5% of PVs were identified in genes other than breast cancer 1 (BRCA1) and BRCA2, including checkpoint kinase 2 (CHEK2) (11.7%), ataxia telangiectasia mutated (ATM; ATM serine/threonine kinase) (9.7%), and partner and localizer of BRCA2 (PALB2) (9.3%). The prevalence of PVs in BRCA1, PALB2, BRCA1-associated RING domain 1 (BARD1), BRCA1-interacting protein C-terminal helicase 1 (BRIP1), and RAD51 paralog C (RAD51C) was statistically higher among women with TNBC. The PV rate was higher among women aged <40 years, lower among women aged >59 years, and relatively constant (8.5%-9.0%) among women who were diagnosed between ages 40 and 59 years.
These results demonstrate that panel testing increased the number of women identified as carrying a PV in this cohort compared with BRCA testing alone. Furthermore, the proportion of women identified who carried a PV in this cohort did not decrease between ages 40 and 59 years. Cancer 2017;123:1721-1730. © 2017 American Cancer Society.
随着基因组合检测在临床实践中变得越来越普遍,了解所鉴定的致病变异(PVs)的患病率和趋势很重要。对于基因异质性癌症,如乳腺癌(BC)而言尤其如此,其中不同基因中的PVs可能与各种风险和癌症亚型相关。作者评估了有BC个人病史的女性的基因检测结果。
本分析纳入了总共35409例仅诊断为BC且接受了25基因组合临床基因检测的女性。排除了患有多发性BC的女性和男性BC患者。评估了整个队列、三阴性乳腺癌(TNBC)女性(n = 4797)以及诊断时年龄的PVs频率和分布。
在9.3%的检测女性中鉴定出PVs;51.5%的PVs在乳腺癌1(BRCA1)和BRCA2以外的基因中鉴定出,包括细胞周期蛋白依赖性激酶2(CHEK2)(11.7%)、共济失调毛细血管扩张症突变基因(ATM;ATM丝氨酸/苏氨酸激酶)(9.7%)以及BRCA2的伴侣和定位蛋白(PALB2)(9.3%)。TNBC女性中BRCA1、PALB2、BRCA1相关的环结构域1(BARD1)、BRCA1相互作用蛋白C末端解旋酶1(BRIP1)和RAD51旁系同源物C(RAD51C)中PVs的患病率在统计学上更高。PV率在年龄<40岁的女性中较高,在年龄>59岁的女性中较低,而在40至59岁之间诊断的女性中相对恒定(8.5% - 9.0%)。
这些结果表明,与单独的BRCA检测相比,基因组合检测增加了该队列中鉴定出携带PV的女性数量。此外,该队列中鉴定出携带PV的女性比例在4
