无证据表明BRIP1基因中的蛋白质截短变异与乳腺癌风险相关:对基因检测板检测的启示
No evidence that protein truncating variants in BRIP1 are associated with breast cancer risk: implications for gene panel testing.
作者信息
Easton Douglas F, Lesueur Fabienne, Decker Brennan, Michailidou Kyriaki, Li Jun, Allen Jamie, Luccarini Craig, Pooley Karen A, Shah Mitul, Bolla Manjeet K, Wang Qin, Dennis Joe, Ahmad Jamil, Thompson Ella R, Damiola Francesca, Pertesi Maroulio, Voegele Catherine, Mebirouk Noura, Robinot Nivonirina, Durand Geoffroy, Forey Nathalie, Luben Robert N, Ahmed Shahana, Aittomäki Kristiina, Anton-Culver Hoda, Arndt Volker, Baynes Caroline, Beckman Matthias W, Benitez Javier, Van Den Berg David, Blot William J, Bogdanova Natalia V, Bojesen Stig E, Brenner Hermann, Chang-Claude Jenny, Chia Kee Seng, Choi Ji-Yeob, Conroy Don M, Cox Angela, Cross Simon S, Czene Kamila, Darabi Hatef, Devilee Peter, Eriksson Mikael, Fasching Peter A, Figueroa Jonine, Flyger Henrik, Fostira Florentia, García-Closas Montserrat, Giles Graham G, Glendon Gord, González-Neira Anna, Guénel Pascal, Haiman Christopher A, Hall Per, Hart Steven N, Hartman Mikael, Hooning Maartje J, Hsiung Chia-Ni, Ito Hidemi, Jakubowska Anna, James Paul A, John Esther M, Johnson Nichola, Jones Michael, Kabisch Maria, Kang Daehee, Kosma Veli-Matti, Kristensen Vessela, Lambrechts Diether, Li Na, Lindblom Annika, Long Jirong, Lophatananon Artitaya, Lubinski Jan, Mannermaa Arto, Manoukian Siranoush, Margolin Sara, Matsuo Keitaro, Meindl Alfons, Mitchell Gillian, Muir Kenneth, Nevelsteen Ines, van den Ouweland Ans, Peterlongo Paolo, Phuah Sze Yee, Pylkäs Katri, Rowley Simone M, Sangrajrang Suleeporn, Schmutzler Rita K, Shen Chen-Yang, Shu Xiao-Ou, Southey Melissa C, Surowy Harald, Swerdlow Anthony, Teo Soo H, Tollenaar Rob A E M, Tomlinson Ian, Torres Diana, Truong Thérèse, Vachon Celine, Verhoef Senno, Wong-Brown Michelle, Zheng Wei, Zheng Ying, Nevanlinna Heli, Scott Rodney J, Andrulis Irene L, Wu Anna H, Hopper John L, Couch Fergus J, Winqvist Robert, Burwinkel Barbara, Sawyer Elinor J, Schmidt Marjanka K, Rudolph Anja, Dörk Thilo, Brauch Hiltrud, Hamann Ute, Neuhausen Susan L, Milne Roger L, Fletcher Olivia, Pharoah Paul D P, Campbell Ian G, Dunning Alison M, Le Calvez-Kelm Florence, Goldgar David E, Tavtigian Sean V, Chenevix-Trench Georgia
机构信息
Department of Oncology, Centre for Cancer Genetic Epidemiology, University of Cambridge, Cambridge, UK Department of Public Health and Primary Care, Centre for Cancer Genetic Epidemiology, University of Cambridge, Cambridge, UK.
Genetic Epidemiology of Cancer team, Inserm, U900, Institut Curie, Mines ParisTech, Paris, France.
出版信息
J Med Genet. 2016 May;53(5):298-309. doi: 10.1136/jmedgenet-2015-103529. Epub 2016 Feb 26.
BACKGROUND
BRCA1 interacting protein C-terminal helicase 1 (BRIP1) is one of the Fanconi Anaemia Complementation (FANC) group family of DNA repair proteins. Biallelic mutations in BRIP1 are responsible for FANC group J, and previous studies have also suggested that rare protein truncating variants in BRIP1 are associated with an increased risk of breast cancer. These studies have led to inclusion of BRIP1 on targeted sequencing panels for breast cancer risk prediction.
METHODS
We evaluated a truncating variant, p.Arg798Ter (rs137852986), and 10 missense variants of BRIP1, in 48 144 cases and 43 607 controls of European origin, drawn from 41 studies participating in the Breast Cancer Association Consortium (BCAC). Additionally, we sequenced the coding regions of BRIP1 in 13 213 cases and 5242 controls from the UK, 1313 cases and 1123 controls from three population-based studies as part of the Breast Cancer Family Registry, and 1853 familial cases and 2001 controls from Australia.
RESULTS
The rare truncating allele of rs137852986 was observed in 23 cases and 18 controls in Europeans in BCAC (OR 1.09, 95% CI 0.58 to 2.03, p=0.79). Truncating variants were found in the sequencing studies in 34 cases (0.21%) and 19 controls (0.23%) (combined OR 0.90, 95% CI 0.48 to 1.70, p=0.75).
CONCLUSIONS
These results suggest that truncating variants in BRIP1, and in particular p.Arg798Ter, are not associated with a substantial increase in breast cancer risk. Such observations have important implications for the reporting of results from breast cancer screening panels.
背景
BRCA1相互作用蛋白C末端解旋酶1(BRIP1)是范可尼贫血互补(FANC)组DNA修复蛋白家族成员之一。BRIP1的双等位基因突变导致FANC J组疾病,先前的研究还表明,BRIP1中罕见的蛋白质截短变异与乳腺癌风险增加有关。这些研究促使BRIP1被纳入用于乳腺癌风险预测的靶向测序panel。
方法
我们在来自参与乳腺癌协会联盟(BCAC)的41项研究的48144例欧洲血统病例和43607例对照中,评估了一个截短变异p.Arg798Ter(rs137852986)和BRIP1的10个错义变异。此外,我们对来自英国的13213例病例和5242例对照、作为乳腺癌家族登记处一部分的三项基于人群研究中的1313例病例和1123例对照,以及来自澳大利亚的1853例家族性病例和2001例对照的BRIP1编码区进行了测序。
结果
在BCAC的欧洲人中,23例病例和18例对照中观察到rs137852986的罕见截短等位基因(比值比1.09,95%置信区间0.58至2.03,p = 0.79)。在测序研究中,34例病例(0.21%)和19例对照(0.23%)中发现了截短变异(合并比值比0.90,95%置信区间0.48至1.70,p = 0.75)。
结论
这些结果表明,BRIP1中的截短变异,尤其是p.Arg798Ter,与乳腺癌风险的大幅增加无关。这些观察结果对乳腺癌筛查panel结果的报告具有重要意义。
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