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BRCA1 and BRCA2 mutations correlate with TP53 abnormalities and presence of immune cell infiltrates in ovarian high-grade serous carcinoma

机译:BRCA1和BRCA2突变与卵巢高级浆液性癌中TP53异常和免疫细胞浸润的存在有关

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We characterized BRCA1 and BRCA2 status (mutation/methylation) in a consecutive series of cases of ovarian carcinoma in order to identify differences in clinicopathological features, molecular characteristics, and outcome between the pelvic high-grade serous cancers with (i) germline or somatic mutations in BRCA1 or BRCA2, (ii) methylation of BRCA1, and (iii) normal BRCA1 or BRCA2. In all, 131 women were identified prospectively, who were undergoing surgical staging and agreed to germline testing for BRCA1 and BRCA2 mutations. Histopathology, germline and somatic BRCA1 or BRCA2 mutations, BRCA1 methylation, and BRCA1 and BRCA2 mRNA expression levels distinguished four subgroups. In all, 103 cases were high-grade serous carcinoma and of these 31 (30%) had germline or somatic BRCA1 or BRCA2 mutations (20% BRCA1 and 10% BRCA2) (group 1), 21 (20%) had methylation of BRCA1 (group 2), and in 51 (50%) there was no BRCA loss (group 3). Group 4 consisted of 28 cases of non-high-grade serous, none of which had BRCA loss. BRCA1 and BRCA2 mRNA expression levels correlated with designated group (P=0.0008). Among high-grade serous carcinomas, there were no differences between groups 1–3 with respect to stage, ascites, CA125 level, platinum sensitivity, cytoreduction rate, neoadjuvant chemotherapy, or survival. Tumors with BRCA1 or BRCA2 mutations had increased immune infiltrates (CD20 and TIA-1) compared with high-grade serous without mutations (P=0.034, 0.027). TP53 expression differed between groups (PTP53 expression in 49/50 tumors from groups 1 and 2. Wild-type TP53 expression was associated with worse outcome in high-grade serous (PTP53 abnormalities and increased immune cell infiltrates are significantly more common in high-grade serous with germline and somatic mutations in BRCA1 or BRCA2, compared with tumors lacking BRCA abnormalities.
机译:我们在一系列连续的卵巢癌病例中表征了BRCA1和BRCA2的状态(突变/甲基化),以鉴定具有(i)种系或体细胞突变的骨盆高级浆液性癌的临床病理特征,分子特征和结果之间的差异(ii)BRCA1甲基化,以及(iii)正常BRCA1或BRCA2。总共有131名妇女经过前瞻性鉴定,这些妇女正在接受手术分期,并同意接受BRCA1和BRCA2突变的种系检测。组织病理学,种系和体细胞BRCA1或BRCA2突变,BRCA1甲基化以及BRCA1和BRCA2 mRNA表达水平区分了四个亚组。总共103例是高度浆液性癌,其中31例(30%)有种系或体细胞BRCA1或BRCA2突变(20 %% BRCA1和10 %% BRCA2)(第1组),21例(20%)具有BRCA1的甲基化(第2组),在51个(50%)中没有BRCA丢失(第3组)。第4组由28例非高级别浆液性病例组成,均无BRCA丢失。 BRCA1和BRCA2 mRNA表达水平与指定组相关(P = 0.0008)。在高度浆液性癌中,第1-3组之间在分期,腹水,CA125水平,铂敏感性,细胞减少率,新辅助化疗或生存率方面无差异。与无突变的高级浆液相比,具有BRCA1或BRCA2突变的肿瘤的免疫浸润(CD20和TIA-1)增加(P = 0.034,0.027)。两组之间的TP53表达有所不同(来自1组和2组的49/50肿瘤中的PTP53表达。高级别浆液中的野生型TP53表达与较差的预后相关(高级别浆液中PTP53异常和免疫细胞浸润的增加明显得多)与缺乏BRCA异常的肿瘤相比,BRCA1或BRCA2的浆液具有种系和体细胞突变。

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