Objective: To investigate the clinicopathological and molecular genetic features of POLE mutant endometrioid carcinoma. Methods: Genetic test data of 230 cases of endometrial carcinoma that underwent surgical resection and molecular typing by next generation sequencing in the First Medical Center of Chinese PLA General Hospital from January 2021 to June 2023 were retrospectively analyzed. Seventeen cases of endometrioid carcinoma with POLE mutation were selected. Clinical and prognostic information was collected. The paraffin-embedded tissue and immunohistochemical sections were reviewed, and the gene detection data were analyzed. Results: In the 17 cases of endometrioid carcinoma with POLE mutations, 16 cases (16/230, 6.9%) had mutations at known pathogenic sites, and 1 case had a mutation site (S459Y) that had not been reported, which was inferred to be pathogenic based on clinical prognosis. The 17 patients aged from 48 to 79 years (median 56 years, mean 58 years). All cases had typical histological features of endometrioid carcinoma, including 7 cases (7/17) of poorly-differentiated, 4 cases (4/17) of moderately-differentiated and 6 cases (6/17) of well-differentiated. Squamous differentiation was noted, mucous differentiation was less commonly found and often accompanied by superficial muscle infiltration. The number of stromal lymphocyte infiltration was variable. Lymph-vascular embolus was found in 6 cases, and lymph node metastasis was only detected in 1 case. According to the FIGO staging system for endometrial cancer in 2023, all the cases were in FIGO stage ⅠAm-POLEmut except for one case in FIGO stage ⅢC1. There were 8 cases with genetic co-mutation, 5 cases with TP53 mutation (immunohistochemically subclonal expression pattern), 1 case with MSI-H, and 2 cases with both TP53 mutation and MSI-H. Five of 7 patients with POLE mutation (poorly-differentiated) received postoperative chemotherapy and/or radiotherapy, 4 patients received endocrine therapy, and 8 patients had no treatment after surgery. One of the stage ⅠAm-POLEmut tumor patients was found to have pelvic recurrence one year after surgery, and the other 16 patients were followed up for 10-38 months without recurrence or metastasis. Conclusions: POLE mutant endometrioid carcinoma may have different differentiation, and most patients have good prognosis. Correct interpretation of molecular results, accurate identification and classification are important for predicting prognosis and avoiding overtreatment. However, a small number of cases may have recurrence and metastasis, and therefore it is necessary to make a reasonable treatment plan based on the comprehensive judgment of other high risk factors.
目的: 探讨POLE突变型子宫内膜样癌的临床病理及分子遗传学特征。 方法: 回顾性分析解放军总医院第一医学中心2021年1月至2023年6月行手术切除且采用二代测序方法完成分子分型的230例子宫内膜癌患者的基因检测数据,筛选出17例伴有POLE突变的子宫内膜样癌病例纳入研究队列,收集临床及预后信息,复阅石蜡及免疫组织化学切片,分析其基因检测数据,并复习相关文献。 结果: 17例伴有POLE突变的子宫内膜样癌中,16例(16/230,6.9%)突变发生在已知的致病性位点,1例突变位点为S459Y。17例患者年龄48~79岁(中位年龄56岁,平均年龄58岁),均具有典型的子宫内膜样癌组织形态特点,低分化7例(7/17),中分化4例(4/17),高分化6例(6/17),可见鳞化,黏液分化较少见,多伴浅肌层浸润,间质淋巴细胞浸润多少不一,6例见脉管癌栓,仅1例伴有淋巴结转移。参考2023版内膜癌国际妇产科联盟(FIGO)分期标准,除1例为ⅢC1期,其余均为ⅠAm-POLEmut期。存在基因共突变者8例,合并TP53突变者5例(免疫组织化学均显示为亚克隆性表达模式),合并高度微卫星不稳定(MSI-H)者1例,同时合并TP53突变及MSI-H者2例。7例POLE突变型低分化子宫内膜样癌患者中5例接受了术后化疗和/或放疗,4例术后行内分泌治疗,8例术后未接受治疗。其中1例ⅠAm-POLEmut期肿瘤患者术后1年发现盆腔复发,其余16例随访10~38个月无复发及转移。 结论: POLE突变型子宫内膜样癌可具有不同分化的组织学形态,患者大多预后良好,正确解读分子检测结果、准确识别及分型对判断预后、避免过度治疗有重要意义,少数病例可能也会出现复发转移,临床需结合其他高危因素综合判断来制定合理的治疗方案。.