依维莫司和来曲唑治疗复发性子宫内膜癌的 II 期研究。
Phase II study of everolimus and letrozole in patients with recurrent endometrial carcinoma.
机构信息
Brian M. Slomovitz, Yunyun Jiang, Melinda S. Yates, Pamela T. Soliman, Taren Johnston, Charles Levenback, Qian Zhang, Kari Ring, Mark F. Munsell, David M. Gershenson, Karen H. Lu, and Robert L. Coleman, The University of Texas MD Anderson Cancer Center, Houston, TX; Brian M. Slomovitz and Maureen Nowakowski, Morristown Medical Center, Morristown, NJ; and Brian M. Slomovitz, Sylvester Comprehensive Cancer Center, University of Miami, Miller School of Medicine, Miami, FL.
出版信息
J Clin Oncol. 2015 Mar 10;33(8):930-6. doi: 10.1200/JCO.2014.58.3401. Epub 2015 Jan 26.
PURPOSE
The phosphoinositol-3 kinase (PI3K) pathway is frequently dysregulated in endometrial cancer (EC). Hormonal manipulation leads to response in some patients with EC, but resistance derived from PI3K pathway activation has been documented. Targeting mammalian target of rapamycin (mTOR) may overcome endocrine resistance. We conducted a two-institution phase II trial of everolimus and letrozole in women with recurrent EC.
PATIENTS AND METHODS
Patients were considered incurable, had measurable disease, and were treated with up to two prior cytotoxic regimens. Everolimus was administered orally at 10 mg daily and letrozole was administered orally at 2.5 mg daily. Each cycle consisted of 4 weeks of therapy. Patients were treated until progression, toxicity, or complete response (CR). The primary end point was the clinical benefit rate (CBR), which was defined as CR, partial response, or stable disease (≥ 16 weeks) by RECIST 1.0 criteria. Translational studies were performed to correlate biomarkers with response.
RESULTS
Thirty-eight patients were enrolled (median age, 62 years; range, 24 to 82 years). Thirty-five patients were evaluable for response. The CBR was 40% (14 of 35 patients); the median number of cycles among responders was 15 (range, seven to 29 cycles). The confirmed objective response rate (RR) was 32% (11 of 35 patients; nine CRs and two partial responses; median, 15 cycles; range, eight to 29 cycles). Twenty percent of patients (seven of 35 patients) were taken off treatment after a prolonged CR and at the discretion of the treating clinician. None of the patients discontinued treatment as a result of toxicity. Serous histology was the best predictor of lack of response. Patients with endometrioid histology and CTNNB1 mutations responded well to everolimus and letrozole.
CONCLUSION
Everolimus plus letrozole results in a high CBR and RR in patients with recurrent EC. Further development of this combination in recurrent endometrioid EC is under way.
目的
磷酸肌醇-3 激酶(PI3K)途径在子宫内膜癌(EC)中经常失调。在一些 EC 患者中,激素治疗会导致反应,但已经记录到 PI3K 途径激活导致的耐药性。靶向哺乳动物雷帕霉素靶蛋白(mTOR)可能克服内分泌耐药性。我们在患有复发性 EC 的女性中进行了一项两机构的依维莫司和来曲唑的 II 期试验。
患者和方法
患者被认为无法治愈,有可测量的疾病,并接受了最多两种以前的细胞毒性治疗方案。依维莫司口服,每日 10mg;来曲唑口服,每日 2.5mg。每个周期包括 4 周的治疗。患者继续治疗,直到进展、毒性或完全缓解(CR)。主要终点是临床获益率(CBR),根据 RECIST 1.0 标准,定义为 CR、部分缓解或稳定疾病(≥16 周)。进行了转化研究,以将生物标志物与反应相关联。
结果
38 名患者入组(中位年龄 62 岁;范围 24 至 82 岁)。35 名患者可评估反应。CBR 为 40%(35 名患者中的 14 名);应答者的中位周期数为 15 个(范围 7 至 29 个周期)。确认的客观缓解率(RR)为 32%(35 名患者中的 11 名;9 名 CR 和 2 名部分缓解;中位 15 个周期;范围 8 至 29 个周期)。20%的患者(35 名患者中的 7 名)在延长的 CR 后和根据治疗医生的判断停止治疗。没有患者因毒性而停止治疗。浆液性组织学是反应不佳的最佳预测因素。具有子宫内膜样组织学和 CTNNB1 突变的患者对依维莫司和来曲唑反应良好。
结论
依维莫司加来曲唑在复发性 EC 患者中导致高 CBR 和 RR。正在进行该联合方案在复发性子宫内膜样 EC 中的进一步开发。
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