[Fertility-preserving treatment outcomes in endometrial cancer and atypical hyperplasia patients with different molecular profiles].

W Y Shao, Y T Dong, Q Y Lyu, J B Liao, Y Xue, X J Chen
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Abstract

Objective: To investigate the impact of molecular classification and key oncogenes on the oncologic outcomes in patients with endometrial carcinoma (EC) and atypical endometrial hyperplasia (AEH) receiving fertility-preserving treatment. Methods: Patients with EC and AEH undergoing progestin-based fertility-preserving treatment and receiving molecular classification as well as key oncogenes test at Obstetrics and Gynecology Hospital, Fudan University from January 2021 to March 2023 were reviewed. Hysteroscopic lesion resection and endometrial biopsy were performed before initiating hormone therapy and every 3 months during the treatment to evaluate the efficacy. The risk factors which had impact on the treatment outcomes in EC and AEH patients were further analyzed. Results: Of the 171 patients analyzed, the median age was 32 years, including 86 patients with EC and 85 patients with AEH. The distribution of molecular classification was as follows: 157 cases (91.8%) were classified as having no specific molecular profile (NSMP); 9 cases (5.3%), mismatch repair deficient (MMR-d); 3 cases (1.8%), POLE-mutated; 2 cases (1.2%), p53 abnormal. No difference was found in the cumulative 40-week complete response (CR) rate between the patients having NSMP or MMR-d (61.6% vs 60.0%; P=0.593), while the patients having MMR-d had increased risk than those having NSMP to have recurrence after CR (50.0% vs 14.4%; P=0.005). Multi-variant analysis showed PTEN gene multi-loci mutation (HR=0.413, 95%CI: 0.259-0.658; P<0.001) and PIK3CA gene mutation (HR=0.499, 95%CI: 0.310-0.804; P=0.004) were associated with a lower cumulative 40-week CR rate, and progestin-insensitivity (HR=3.825, 95%CI: 1.570-9.317; P=0.003) and MMR-d (HR=9.014, 95%CI: 1.734-46.873; P=0.009) were independent risk factors of recurrence in EC and AEH patients. Conclusions: No difference in cumulative 40-week CR rate is found in the patients having NSMP or MMR-d who received progestin-based fertility-preserving treatment, where the use of hysteroscopy during the treatment might be the reason, while those having MMR-d have a higher risk of recurrence after CR. Oncogene mutation of PTEN or PIK3CA gene might be associated with a lower response to progestin treatment. The molecular profiles help predict the fertility-preserving treatment outcomes in EC and AEH patients.

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[不同分子特征的子宫内膜癌症和不典型增生患者的保肥治疗结果]。
目的:探讨分子分类和关键癌基因对接受保生育治疗的子宫内膜癌(EC)和不典型子宫内膜增生(AEH)患者肿瘤学结果的影响。方法:对2021年1月至2023年3月在复旦大学妇产科医院接受基于孕激素的保生育治疗并接受分子分类和关键癌基因检测的EC和AEH患者进行回顾性分析。在开始激素治疗前和治疗期间每3个月进行一次宫腔镜病变切除和子宫内膜活检,以评估疗效。进一步分析了影响EC和AEH患者治疗结果的危险因素。结果:在分析的171名患者中,中位年龄为32岁,包括86名EC患者和85名AEH患者。分子分类分布如下:157例(91.8%)为无特异性分子谱(NSMP);错配修复缺陷型9例(5.3%);POLE突变3例(1.8%);p53异常2例(1.2%)。NSMP或MMR-d患者的累积40周完全缓解率(CR)无差异(61.6%对60.0%;P=0.593),而MMR-d患者CR后复发的风险高于NSMP患者(50.0%vs 14.4%;P=0.005)。多变异分析显示PTEN基因多位点突变(HR=0.413,95%CI:0.259-0.658;PHR=0.499,95%CI:0.310-0.804;P=0.004)与较低的40周累积CR率相关,和孕激素不敏感(HR=3.825,95%CI:1.570-9.317;P=0.003)和MMR-d(HR=9.014,95%CI:1.734-46.873;P=0.009)是EC和AEH患者复发的独立危险因素。结论:NSMP或MMR-d患者接受基于孕激素的保生育治疗后,40周累计CR率没有差异,治疗期间使用宫腔镜可能是原因,而MMR-d的患者CR后复发的风险更高。PTEN或PIK3CA基因的癌基因突变可能与对孕激素治疗的低反应有关。分子谱有助于预测EC和AEH患者保留生育能力的治疗结果。
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