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BRAF和KRAS的突变先于卵巢浆液性交界性肿瘤的发生。

Mutations of BRAF and KRAS precede the development of ovarian serous borderline tumors.

作者信息

Ho Chung-Liang, Kurman Robert J, Dehari Reiko, Wang Tian-Li, Shih Ie-Ming

机构信息

Department of Pathology, Johns Hopkins Medical Institutions, Baltimore, Maryland 21231, USA.

出版信息

Cancer Res. 2004 Oct 1;64(19):6915-8. doi: 10.1158/0008-5472.CAN-04-2067.

Abstract

Molecular genetic changes that are associated with the initiating stage of tumor development are important in tumorigenesis. Ovarian serous borderline tumors (SBTs), putative precursors of low-grade serous carcinomas, are among the few human neoplasms with a high frequency of activating mutations in BRAF and KRAS genes. However, it remains unclear as to how these mutations contribute to tumor progression. To address this issue, we compared the mutational status of BRAF and KRAS in both SBTs and the adjacent epithelium from cystadenomas, the presumed precursor of SBTs. We found that three of eight SBTs contained mutant BRAF, and four SBTs contained mutant KRAS. All specimens with mutant BRAF harbored wild-type KRAS and vice versa. Thus, seven (88%) of eight SBTs contained either BRAF or KRAS mutations. The same mutations detected in SBTs were also identified in the cystadenoma epithelium adjacent to the SBTs in six (86%) of seven informative cases. As compared to SBTs, the cystadenoma epithelium, like ovarian surface epithelium, lacks cytological atypia. Our findings provide cogent evidence that mutations of BRAF and KRAS occur in the epithelium of cystadenomas adjacent to SBTs and strongly suggest that they are very early events in tumorigenesis, preceding the development of SBT.

摘要

与肿瘤发生起始阶段相关的分子遗传学改变在肿瘤发生过程中至关重要。卵巢浆液性交界性肿瘤(SBTs)是低级别浆液性癌的假定前体,是少数在BRAF和KRAS基因中具有高频激活突变的人类肿瘤之一。然而,这些突变如何促进肿瘤进展仍不清楚。为了解决这个问题,我们比较了SBTs以及来自囊腺瘤(SBTs的假定前体)的相邻上皮组织中BRAF和KRAS的突变状态。我们发现,8个SBTs中有3个含有BRAF突变,4个SBTs含有KRAS突变。所有含有BRAF突变的标本都携带野生型KRAS,反之亦然。因此,8个SBTs中有7个(88%)含有BRAF或KRAS突变。在7个可提供信息的病例中,有6个(86%)在与SBTs相邻的囊腺瘤上皮中也检测到了与SBTs中相同的突变。与SBTs相比,囊腺瘤上皮与卵巢表面上皮一样,缺乏细胞学异型性。我们的研究结果提供了有力证据,表明BRAF和KRAS突变发生在与SBTs相邻的囊腺瘤上皮中,并强烈表明它们是肿瘤发生过程中非常早期的事件,早于SBTs的发生。

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