Histologic and Molecular Type Changes in Endometrial Cancer Recurrences in Comparison With Their Corresponding Primary Tumors.

IF 4.5 1区 医学 Q1 PATHOLOGY American Journal of Surgical Pathology Pub Date : 2024-09-13 DOI:10.1097/PAS.0000000000002308
Esther Moreno-Moreno, Tamara Caniego-Casas, Irene Carretero-Barrio, Alfonso Cortés, Alfonso Muriel, José Antonio Domínguez-Rullán, Carmen Martín-Gromaz, Gema Moreno-Bueno, Xavier Matías-Guiu, José Palacios, Belén Pérez-Mies
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Abstract

In this study, molecular alterations in endometrial carcinoma (EC) recurrences were analyzed. We aimed to identify genes implicated in tumor progression and to evaluate whether histologic and molecular type shifting occurs in recurrences. Thus, we analyzed 50 samples corresponding to 24 primary ECs (15 low-grade endometrioid endometrial carcinomas [LG-EECs] and 9 high-grade endometrial carcinomas) and their corresponding 26 recurrences. These were studied by immunohistochemistry, next-generation sequencing, and MLH1 promoter methylation. We observed shared mutations in all primary tumors and their recurrences, indicating a clonal relationship between both lesions. Most morphologic and molecular changes associated with progression were found in LG-EEC. In this group, 6 patients (40%) presented additional mutations in the recurrence. These mutations more frequently affected genes of the PI3K/AKT/PTEN pathway, implicating this pathway not only in tumor initiation but also in progression. In addition, 2 patients (13%) in which the primary tumor belonged to the nonspecific molecular profile subtype, shifted to the mismatch repair deficient (MMRd) subtype after the acquisition of MLH1 promoter methylation in the recurrence lesions. In 3 patients (20%) with MMRd, there was a change from LG-EEC to G3-EEC. One TP53-mutated LG-EEC transformed into an undifferentiated carcinoma in a mediastinal lymph node metastasis after losing the expression of SMARCA2 while preserving SMARCA4 and SMARCB1. Morphologic and molecular changes in EC recurrences, especially dedifferentiation and the acquisition of MMRd, should be considered for a correct diagnosis and treatment. MMRd should be tested in metastatic lesions, if available, in patients with primary tumors reported to be of a molecular subtype different from MMRd.

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子宫内膜癌复发的组织学和分子类型变化与相应原发肿瘤的比较
本研究分析了子宫内膜癌(EC)复发的分子改变。我们的目的是确定与肿瘤进展有关的基因,并评估复发中是否会发生组织学和分子类型的转变。因此,我们分析了 50 份样本,分别对应 24 例原发性子宫内膜癌(15 例低度子宫内膜样内膜癌 [LG-EECs] 和 9 例高级别子宫内膜癌)及其相应的 26 例复发。我们通过免疫组化、新一代测序和 MLH1 启动子甲基化对这些肿瘤进行了研究。我们在所有原发肿瘤及其复发瘤中都观察到了共同的突变,这表明这两种病变之间存在克隆关系。大多数与进展相关的形态学和分子变化都出现在 LG-EEC 中。在这组患者中,有6名患者(40%)的复发出现了额外的突变。这些突变更频繁地影响到 PI3K/AKT/PTEN 通路的基因,表明该通路不仅与肿瘤的发生有关,还与肿瘤的进展有关。此外,2 名患者(13%)的原发肿瘤属于非特异性分子特征亚型,在复发病灶中出现 MLH1 启动子甲基化后,转为错配修复缺陷(MMRd)亚型。3例(20%)MMRd患者从LG-EEC转变为G3-EEC。一名TP53突变的LG-EEC在失去SMARCA2的表达而保留SMARCA4和SMARCB1后,在纵隔淋巴结转移中转变为未分化癌。为了进行正确的诊断和治疗,应考虑EC复发的形态学和分子学变化,尤其是去分化和获得MMRd。据报道,原发肿瘤的分子亚型与 MMRd 不同,如有可能,应在转移病灶中检测 MMRd。
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来源期刊
CiteScore
10.30
自引率
5.40%
发文量
295
审稿时长
1 months
期刊介绍: The American Journal of Surgical Pathology has achieved worldwide recognition for its outstanding coverage of the state of the art in human surgical pathology. In each monthly issue, experts present original articles, review articles, detailed case reports, and special features, enhanced by superb illustrations. Coverage encompasses technical methods, diagnostic aids, and frozen-section diagnosis, in addition to detailed pathologic studies of a wide range of disease entities. Official Journal of The Arthur Purdy Stout Society of Surgical Pathologists and The Gastrointestinal Pathology Society.
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