首页> 外文期刊>American Journal of Pathology >{beta}-Catenin Expression Pattern in Stage I and II Ovarian Carcinomas : Relationship with {beta}-Catenin Gene Mutations,Clinicopathological Features, and Clinical Outcome
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{beta}-Catenin Expression Pattern in Stage I and II Ovarian Carcinomas : Relationship with {beta}-Catenin Gene Mutations,Clinicopathological Features, and Clinical Outcome

机译:I期和II期卵巢癌中的{beta} -Catenin表达模式:与{beta} -Catenin基因突变,临床病理特征和临床结果的关系

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摘要

The immunohistochemical expression pattern of ß-catenin has been correlated with ß-catenin gene mutations, clinicopathological features, and disease outcome in 69 stage I and II ovarian carcinomas. ß-Catenin expression was localized in the nuclei, in addition to the cytoplasm and membrane, in 11 tumors (16%): nine endometrioid carcinomas with widespread nuclear expression and two serous carcinomas with focal nuclear expression. The remaining 58 carcinomas (84%) only had membranous ß-catenin expression. All but one of the endometrioid carcinomas with nuclear ß-catenin expression had considerable squamous metaplasia, and five of these cases had large areas of endometrioid tumor of low malignant potential. In addition, ß-catenin nuclear expression was observed in atypical epithelial cells in endometriotic glands adjacent to an endometrioid carcinoma. Sequencing was performed on 25 tumors and corresponding normal tissue: all 13 endometrioid tumors as well as 12 carcinomas of other histological types (four serous, two clear cell, two mucinous, and two mixed). There were oncogenic mutations in the phosphorylation sequence for GSK-3ß in exon 3 of the ß-catenin gene in seven endometrioid carcinomas with ß-catenin nuclear expression. Three mutations affected codon 32 (D32G, D32Y, and D32Y), one affected codon 33 (S33C), two affected codon 37 (S37C and S37F), and one affected codon 41 (T41A). No mutations were observed in the other 18 carcinomas analyzed, comprising two endometrioid and two serous carcinomas with ß-catenin nuclear expression, and 14 carcinomas of different histological types with only membranous expression. In the univariate and multivariate survival analyses, ß-catenin nuclear expression was selected as an indicator of good prognosis, because no patient whose tumor expressed ß-catenin in the nuclei showed relapses or died, in contrast to the 19 relapses and deaths among patients with tumors that only had ß-catenin membranous expression, including three of the four patients with endometrioid carcinomas. Oncogenic ß-catenin mutation is characteristic of a group of endometrioid carcinomas with a good prognosis, most of which originate from previous benign or borderline lesions. Endometrioid carcinomas with exclusively membranous expression of ß-catenin seem to represent a different subgroup of carcinomas that probably have a worse prognosis. In early-stage ovarian cancer, determination of the ß-catenin expression pattern could prove to be a useful marker for selecting low-risk patients.
机译:ß-catenin 的免疫组化表达模式与ß-catenin基因突变,临床病理特征, 和69例I,II期卵巢癌的疾病预后相关。 ß-连环蛋白的表达位于11个肿瘤(16%)中,除了细胞质和膜之外,还位于细胞核中:9个子宫内膜样异位癌表达和两个具有局灶性核表达的浆液性 癌。其余58例癌 (84%)仅具有膜性ß-catenin表达。呈核ß-catenin 表达的子宫内膜样癌中只有一个 有鳞状上皮化生, 的这些病例中有五个子宫内膜样肿瘤面积大低恶性 电位。此外,在子宫内膜异位癌附近的子宫内膜异位腺的非典型上皮细胞中观察到了β-catenin的核表达 。对25个肿瘤和相应的正常组织进行了测序:全部13个子宫内膜样异位肿瘤以及其他12种其他组织学类型的癌(四个浆液,两个透明细胞,两个粘液,两个混合)。 在七个中,β-catenin基因外显子3的GSK-3ß的磷酸化序列 有致癌突变。 > 具有ß-catenin核表达的子宫内膜样癌。 三个突变影响第32位密码子(D32G,D32Y和D32Y),一个 影响第33位密码子(S33C),两个受影响的密码子37(S37C和S37F), 和一个受影响的密码子41(T41A)。在分析的其他18种癌症中未观察到 突变,包括2个子宫内膜异位 和2个具有ß-catenin核表达的浆液性癌, 和14个癌变。仅 膜表达的不同组织学类型。在单因素和多因素生存分析中,选择 ß-catenin核表达作为良好预后的指标 ,因为没有患者表达肿瘤 ß核中的-catenin显示复发或死亡,而 与仅有 具有β-catenin膜性表达的肿瘤患者中的19次复发和死亡相反,其中包括<-sup> sup> 4名子宫内膜样癌患者。致癌性ß-catenin突变 是一组子宫内膜样癌的特征,预后良好,其中大多数起源于先前的良性 或边缘性病变。子宫内膜样癌仅以s-catenin膜表达,似乎代表了 个不同的亚组,预后可能更差。在早期卵巢癌中,确定 ß-catenin表达模式可能是选择低危患者的有用 标记。

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  • 来源
    《American Journal of Pathology》 |1999年第2期|527-536|共10页
  • 作者单位

    From Departamento de Anatomía Patológica,Hospital La Paz, Madrid, Spain;

    From Departamento de Anatomía Patológica,Hospital La Paz, Madrid, Spain;

    From Departamento de Anatomía Patológica,Hospital La Paz, Madrid, Spain;

    From Departamento de Anatomía Patológica,Hospital La Paz, Madrid, Spain;

    From Departamento de Anatomía Patológica,Hospital La Paz, Madrid, Spain;

    and Departamento de Ginecología y Obstetricia,Hospital La Paz, Madrid, Spain;

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  • 入库时间 2022-08-17 14:17:18

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