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染色质重塑和DNA修复基因在子宫内膜样子宫内膜癌中经常发生突变。

Chromatin remodelling and DNA repair genes are frequently mutated in endometrioid endometrial carcinoma.

作者信息

García-Sanz Pablo, Triviño Juan Carlos, Mota Alba, Pérez López María, Colás Eva, Rojo-Sebastián Alejandro, García Ángel, Gatius Sonia, Ruiz María, Prat Jaime, López-López Rafael, Abal Miguel, Gil-Moreno Antonio, Reventós Jaume, Matias-Guiu Xavier, Moreno-Bueno Gema

机构信息

MD Anderson International Foundation, Madrid, Spain.

Departamento de Bioquímica, Universidad Autónoma de Madrid (UAM), Instituto de Investigaciones Biomédicas "Alberto Sols" (CSIC-UAM), Madrid, Spain.

出版信息

Int J Cancer. 2017 Apr 1;140(7):1551-1563. doi: 10.1002/ijc.30573. Epub 2017 Feb 2.

DOI:10.1002/ijc.30573
PMID:27997699
Abstract

In developed countries, endometrial carcinoma is the most common cancer that affects the female genital tract. Endometrial carcinoma is divided into two main histological types, type I or endometrioid and type II or non-endometrioid, each of which have characteristic, although not exclusive, molecular alterations and mutational profiles. Nevertheless, information about the implication and relevance of some of these genes in this disease is lacking. We sought here to identify new recurrently mutated genes in endometrioid cancers that play a role in tumourigenesis and that influence the clinical outcome. We focused on low-grade, non-ultramutated tumours as these tumours have a worse prognosis than the ultramutated POLE-positive endometrioid endometrial carcinomas (EECs). We performed exome-sequencing of 11 EECs with matched normal tissue and subsequently validated 15 candidate genes in 76 samples. For the first time, we show that mutations in chromatin remodelling-related genes (KMT2D, KMT2C, SETD1B and BCOR) and in DNA-repair-related genes (BRCA1, BRCA2, RAD50 and CHD4) are frequent in this subtype of endometrial cancer. The alterations to these genes occurred with frequencies ranging from 35.5% for KMT2D to 10.5% for BRCA1 and BCOR, with some showing a tendency toward co-occurrence (RAD50-KMT2D and RAD50-SETD1B). All these genes harboured specific mutational hotspots. In addition, the mutational status of KMT2C, KMT2D and SETD1B helps to predict the degree of myometrial invasion, a critical prognostic feature. These results highlight the possible implication of these genes in this disease, creating opportunities for new therapeutic approaches.

摘要

在发达国家,子宫内膜癌是影响女性生殖道的最常见癌症。子宫内膜癌主要分为两种组织学类型,I型或子宫内膜样癌和II型或非子宫内膜样癌,每种类型都有其特征性的(尽管不是排他性的)分子改变和突变谱。然而,关于其中一些基因在这种疾病中的作用和相关性的信息仍然缺乏。我们在此试图鉴定在子宫内膜样癌中反复发生突变的新基因,这些基因在肿瘤发生中起作用并影响临床结局。我们聚焦于低级别、非超突变肿瘤,因为这些肿瘤的预后比超突变的POLE阳性子宫内膜样癌(EEC)更差。我们对11例EEC及其匹配的正常组织进行了外显子组测序,随后在76个样本中验证了15个候选基因。我们首次表明,染色质重塑相关基因(KMT2D、KMT2C、SETD1B和BCOR)以及DNA修复相关基因(BRCA1、BRCA2、RAD50和CHD4)的突变在这种子宫内膜癌亚型中很常见。这些基因的改变发生率从KMT2D的35.5%到BRCA1和BCOR的10.5%不等,有些显示出共发生的趋势(RAD50-KMT2D和RAD50-SETD1B)。所有这些基因都有特定的突变热点。此外,KMT2C、KMT2D和SETD1B的突变状态有助于预测肌层浸润程度,这是一个关键的预后特征。这些结果突出了这些基因在这种疾病中的可能作用,为新的治疗方法创造了机会。

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