The genomics and genetics of endometrial cancer.

Advances in genomics and genetics Pub Date : 2012-03-01 DOI:10.2147/AGG.S28953

Andrea J O'Hara, Daphne W Bell

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Abstract

Most sporadic endometrial cancers (ECs) can be histologically classified as endometrioid, serous, or clear cell. Each histotype has a distinct natural history, clinical behavior, and genetic etiology. Endometrioid ECs have an overall favorable prognosis. They are typified by high frequency genomic alterations affecting PIK3CA, PIK3R1, PTEN, KRAS, FGFR2, ARID1A (BAF250a), and CTNNB1 (β-catenin), as well as epigenetic silencing of MLH1 resulting in microsatellite instability. Serous and clear cell ECs are clinically aggressive tumors that are rare at presentation but account for a disproportionate fraction of all endometrial cancer deaths. Serous ECs tend to be aneuploid and are typified by frequent genomic alterations affecting TP53 (p53), PPP2R1A, HER-2/ERBB2, PIK3CA, and PTEN; additionally, they display dysregulation of E-cadherin, p16, cyclin E, and BAF250a. The genetic etiology of clear cell ECs resembles that of serous ECs, but it remains relatively poorly defined. A detailed discussion of the characteristic patterns of genomic alterations that distinguish the three major histotypes of endometrial cancer is reviewed herein.

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子宫内膜癌的基因组学和遗传学。

大多数散发性子宫内膜癌（EC）在组织学上可分为子宫内膜样癌、浆液性癌和透明细胞癌。每种组织类型都有不同的自然史、临床表现和遗传病因。子宫内膜样癌的总体预后较好。它们的典型特征是高频率的基因组改变，影响 PIK3CA、PIK3R1、PTEN、KRAS、FGFR2、ARID1A（BAF250a）和 CTNNB1（β-catenin），以及 MLH1 的表观遗传沉默导致微卫星不稳定。浆液性和透明细胞性子宫内膜癌是临床上侵袭性很强的肿瘤，发病时很少见，但在所有子宫内膜癌死亡病例中却占很大比例。浆液性EC往往是非整倍体，其典型特征是频繁发生影响TP53（p53）、PPP2R1A、HER-2/ERBB2、PIK3CA和PTEN的基因组改变；此外，它们还表现出E-adherin、p16、细胞周期蛋白E和BAF250a的失调。透明细胞癌变的遗传病因与浆液性癌变相似，但相对来说还不太明确。本文详细讨论了区分子宫内膜癌三种主要组织类型的基因组改变特征模式。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Advances in genomics and genetics

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