奥拉帕利联合卡铂治疗携 BRCA1 或 BRCA2 突变的乳腺癌或卵巢癌的 I/ Ib 期研究及生物标志物分析。
Phase I/Ib study of olaparib and carboplatin in BRCA1 or BRCA2 mutation-associated breast or ovarian cancer with biomarker analyses.
机构信息
Affiliations of authors: Medical Oncology Branch, Center for Cancer Research (J-ML, JLH, CMA, AMN, LM, JAZ, MY, NG, TMS, WDF, NA, ECK), National Clinical Target Validation Laboratory, Leidos Biomedical Research, Frederick National Laboratory for Cancer Research (JJ), Center for Interventional Oncology, Radiology, and Imaging Sciences, Clinical Center and National Cancer Institute (BJW), and Division of Cancer Treatment and Diagnosis, National Cancer Institute (JD), National Institutes of Health, Bethesda, MD.
出版信息
J Natl Cancer Inst. 2014 May 19;106(6):dju089. doi: 10.1093/jnci/dju089. Print 2014 Jun.
BACKGROUND
Olaparib has single-agent activity against breast/ovarian cancer (BrCa/OvCa) in germline BRCA1 or BRCA2 mutation carriers (gBRCAm). We hypothesized addition of olaparib to carboplatin can be administered safely and yield preliminary clinical activity.
METHODS
Eligible patients had measurable or evaluable disease, gBRCAm, and good end-organ function. A 3 + 3 dose escalation tested daily oral capsule olaparib (100 or 200mg every 12 hours; dose level1 or 2) with carboplatin area under the curve (AUC) on day 8 (AUC3 day 8), then every 21 days. For dose levels 3 to 6, patients were given olaparib days 1 to 7 at 200 and 400 mg every 12 hours, with carboplatin AUC3 to 5 on day 1 or 2 every 21 days; a maximum of eight combination cycles were permitted, after which daily maintenance of olaparib 400mg every12 hours continued until progression. Dose-limiting toxicity was defined in the first two cycles. Peripheral blood mononuclear cells were collected for polymorphism analysis and polyADP-ribose incorporation. Paired tumor biopsies (before/after cycle 1) were obtained for biomarker proteomics and apoptosis endpoints.
RESULTS
Forty-five women (37 OvCa/8 BrCa) were treated. Dose-limiting toxicity was not reached on the intermittent schedule. Expansion proceeded with olaparib 400mg every 12 hours on days 1 to 7/carboplatin AUC5. Grade 3/4 adverse events included neutropenia (42.2%), thrombocytopenia (20.0%), and anemia (15.6%). Responses included 1 complete response (1 BrCa; 23 months) and 21 partial responses (50.0%; 15 OvCa; 6 BrCa; median = 16 [4 to >45] in OvCa and 10 [6 to >40] months in BrCa). Proteomic analysis suggests high pretreatment pS209-eIF4E and FOXO3a correlated with duration of response (two-sided P < .001; Pearson's R (2) = 0.94).
CONCLUSIONS
Olaparib capsules 400mg every 12 hours on days 1 to 7/carboplatin AUC5 is safe and has activity in gBRCAm BrCa/OvCa patients. Exploratory translational studies indicate pretreatment tissue FOXO3a expression may be predictive for response to therapy, requiring prospective validation.
背景
奥拉帕利对携带生殖系 BRCA1 或 BRCA2 突变(gBRCAm)的乳腺癌/卵巢癌(BrCa/OvCa)患者具有单药活性。我们假设奥拉帕利联合卡铂治疗可安全应用并获得初步的临床疗效。
方法
符合条件的患者具有可测量或可评估的疾病、gBRCAm 和良好的终末器官功能。采用 3+3 剂量递增法,每天口服奥拉帕利胶囊(100 或 200mg,每 12 小时 1 次;剂量水平 1 或 2)联合卡铂第 8 天(AUC3 第 8 天)的曲线下面积(AUC3 第 8 天),然后每 21 天 1 次。对于剂量水平 3 至 6,患者在第 1 至 7 天接受 200 和 400mg 每 12 小时 1 次的奥拉帕利治疗,卡铂 AUC3 至 5 每天 1 或 2 次,每 21 天 1 次;最多允许 8 个联合周期,之后继续每天维持奥拉帕利 400mg 每 12 小时,直至疾病进展。在前两个周期中定义了剂量限制毒性。收集外周血单核细胞进行多态性分析和多聚 ADP-核糖基化掺入。在第 1 周期前后(治疗前/后)获得配对肿瘤活检标本,用于生物标志物蛋白质组学和细胞凋亡终点分析。
结果
共 45 例女性(37 例卵巢癌/8 例乳腺癌)接受了治疗。间歇性方案未达到剂量限制毒性。奥拉帕利 400mg 每 12 小时持续治疗 1 至 7 天/卡铂 AUC5 剂量水平得到了扩展。3/4 级不良事件包括中性粒细胞减少症(42.2%)、血小板减少症(20.0%)和贫血(15.6%)。疗效包括完全缓解 1 例(1 例乳腺癌;23 个月)和部分缓解 21 例(50.0%;15 例卵巢癌;6 例乳腺癌;卵巢癌的中位缓解时间为 16[4 至 >45]个月,乳腺癌的中位缓解时间为 10[6 至 >40]个月)。蛋白质组学分析表明,高预处理 pS209-eIF4E 和 FOXO3a 与缓解持续时间相关(双侧 P<0.001;Pearson's R(2)=0.94)。
结论
奥拉帕利胶囊 400mg 每天 1 至 7 次/卡铂 AUC5 联合治疗是安全的,对携带生殖系 BRCA1 或 BRCA2 突变的乳腺癌/卵巢癌患者具有活性。探索性转化研究表明,治疗前组织 FOXO3a 表达可能是预测治疗反应的指标,需要前瞻性验证。
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