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首页> 外文期刊>Virchows Archiv >PIK3CA mutations and loss of ARID1A protein expression are early events in the development of cystic ovarian clear cell adenocarcinoma
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PIK3CA mutations and loss of ARID1A protein expression are early events in the development of cystic ovarian clear cell adenocarcinoma

机译:PIK3CA突变和ARID1A蛋白表达的丧失是卵巢囊性透明细胞癌发展的早期事件

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摘要

Somatic mutations of PIK3CA and ARID1A are the most common genetic alterations observed in ovarian clear cell adenocarcinomas (CCA). In a previous report, we showed that PIK3CA gene mutations and loss of ARID1A expression occur early during the development of CCA. In the present study, using direct genomic DNA sequencing for exons 9 and 20 of PIK3CA and immunohistochemistry for ARID1A protein expression, we analyzed the association of these molecular alterations with various clinicopathological parameters in a total of 90 cases of primary ovarian CCA, including 42 previously examined cases. The presence of PIK3CA mutations, identified in 34 (39%) of the 88 informative cases, was significantly associated with a grossly cystic tumor, the presence of adjacent endometriosis, prominent papillary architecture of tumor growth, the presence of hyalinized and mucoid stroma, and the absence of clear cell adenofibroma components (P < 0.05, each). There was no significant association of PIK3CA mutations with other clinical variables, such as age, clinical stage, or clinical outcome of the patients. The intensity of immunoreactivity for ARID1A was assigned as negative, weakly positive, and strongly positive in 44%, 22%, and 33% of tumors, respectively. Compared to tumors immunoreactive for ARID1A, ARID1A-negative tumors were significantly associated with the presence of adjacent endometriosis (P = 0.025), but there was no statistically supported association with other examined clinicopathological parameters. Compared with CCAs strongly positive for ARID1A, CCAs negative for ARID1A more frequently harbor PIK3CA mutations (P = 0.013). PIK3CA gene mutations and ARID1A immunohistochemistry lacked prognostic significance. These data further support the idea that these molecular alterations occur as very early events during tumor development of ovarian CCA.
机译:PIK3CA和ARID1A的体细胞突变是在卵巢透明细胞腺癌(CCA)中观察到的最常见的遗传变异。在以前的报告中,我们显示了PIK3CA基因突变和ARID1A表达缺失发生在CCA发生的早期。在本研究中,我们使用PIK3CA外显子9和20的直接基因组DNA测序和ARID1A蛋白表达的免疫组化方法,在总共90例原发性卵巢CCA病例中分析了这些分子改变与各种临床病理学参数的相关性,其中先前42例检查的情况。在88例资料丰富的病例中,有34例(39%)发现存在PIK3CA突变,与大囊性肿瘤,邻近的子宫内膜异位症,显着的乳头状肿瘤生长结构,透明质和黏液样基质以及不存在透明细胞腺纤维瘤成分(每个P <0.05)。 PIK3CA突变与其他临床变量(例如患者的年龄,临床分期或临床结果)没有显着相关性。 ARID1A的免疫反应强度分别在44%,22%和33%的肿瘤中为阴性,弱阳性和强阳性。与对ARID1A具有免疫反应性的肿瘤相比,ARID1A阴性的肿瘤与邻近子宫内膜异位症的存在显着相关(P = 0.025),但是与其他检查过的临床病理参数没有统计学上的关联。与ARID1A呈强阳性的CCA相比,ARID1A呈阴性的CCA更经常携带PIK3CA突变(P = 0.013)。 PIK3CA基因突变和ARID1A免疫组化缺乏预后意义。这些数据进一步支持了这样的想法,即这些分子改变是在卵巢CCA肿瘤发展期间的非常早期的事件中发生的。

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