BC Cancer Agency, Vancouver Clinic, Vancouver, BC, Canada.
Gynecol Oncol. 2013 Aug;130(2):269-74. doi: 10.1016/j.ygyno.2013.05.008. Epub 2013 May 11.
HPV infection has been associated with deregulation of the PI3K-Akt-mTOR pathway in invasive cervical carcinomas. This 2-stage phase II study assessed the activity of the mTOR inhibitor, temsirolimus, in patients with measurable metastatic and/or locally advanced, recurrent carcinoma of the cervix.
Temsirolimus 25mg i.v. was administered weekly in 4 week cycles. One response among the first 18 patients was required to proceed to the second stage of accrual. Correlative molecular studies were performed on archival tumor tissue.
Thirty-eight patients were enrolled. Thirty-seven patients were evaluable for toxicity and 33 for response. One patient experienced a partial response (3.0%). Nineteen patients had stable disease (57.6%) [median duration 6.5 months (range 2.4-12.0mo)]. The 6-month progression free survival rate was 28% (95% CI: 14-43%). The median progression free survival was 3.52 months [95% CI (1.81-4.70)]. Adverse effects were mild-moderate in most cases and similar to other temsirolimus studies. No toxicity>grade 3 was observed. Assessment of PTEN and PIK3CA by IHC, copy number analyses and PTEN promoter methylation status did not reveal subsets associated with disease stability.
Single agent temsirolimus has modest activity in cervical carcinoma with about two-thirds of patients exhibiting stable disease. Molecular markers for treatment benefit remain to be identified.
HPV 感染与浸润性宫颈癌中 PI3K-Akt-mTOR 通路的失调有关。本研究为两阶段 II 期临床试验,评估了 mTOR 抑制剂替西罗莫司在可测量的转移性和/或局部晚期、复发性宫颈癌患者中的活性。
每周静脉给予替西罗莫司 25mg,每 4 周为一个周期。在前 18 例患者中需要有 1 例出现应答,才能进入第二阶段入组。对存档的肿瘤组织进行了相关的分子研究。
共入组 38 例患者。37 例患者可评估毒性,33 例患者可评估疗效。1 例患者出现部分缓解(3.0%)。19 例患者疾病稳定(57.6%)[中位持续时间 6.5 个月(范围 2.4-12.0mo)]。6 个月无进展生存率为 28%(95%CI:14-43%)。无进展生存的中位时间为 3.52 个月[95%CI(1.81-4.70)]。大多数不良反应为轻中度,与其他替西罗莫司研究相似。未观察到>3 级毒性。通过 IHC、拷贝数分析和 PTEN 启动子甲基化状态评估 PTEN 和 PIK3CA ,未发现与疾病稳定相关的亚组。
替西罗莫司单药治疗宫颈癌活性适度,约三分之二的患者疾病稳定。仍需要确定治疗获益的分子标志物。
