Li Chunze, Wang Bei, Chen Shang-Chiung, Wada Russell, Lu Dan, Wang Xin, Polhamus Daniel, French Jonathan, Vadhavkar Shweta, Strasak Alexander, Smitt Melanie, Joshi Amita, Samant Meghna, Quartino Angelica, Jin Jin, Girish Sandhya
Department of Clinical Pharmacology, Genentech, Inc., 1 DNA Way, South San Francisco, CA, 94080, USA.
Certara Strategic Consulting, Certara, Menlo Park, CA, USA.
Cancer Chemother Pharmacol. 2017 Dec;80(6):1079-1090. doi: 10.1007/s00280-017-3440-4. Epub 2017 Oct 11.
In the phase III EMILIA study, trastuzumab emtansine (T-DM1) significantly improved progression-free survival (PFS) and overall survival (OS) versus capecitabine plus lapatinib (control) in previously treated human epidermal growth factor receptor 2-positive advanced breast cancer. Using EMILIA data, we evaluated the T-DM1 exposure-response relationship.
Exposure-response relationships were examined with four exposure metrics [model-predicted and observed minimum concentration (C ) and area under the concentration-time curve from time zero to day 21 of T-DM1 at cycle 1] and multiple efficacy (OS, PFS, objective response rate) and safety (grade ≥ 3 adverse events, grade ≥ 3 thrombocytopenia, grade ≥ 3 hepatotoxicity) endpoints.
An apparent exposure-response trend was observed between model-predicted exposure metrics and efficacy; trends for observed exposure metrics were shallower and often not significant. Although median OS and PFS were numerically longer in patients with higher versus lower model-predicted cycle 1 C , OS and PFS hazard ratios for T-DM1-treated patients in the lowest exposure quartile (Q1) versus control were < 1 after adjusting for baseline risk factors (e.g., ECOG status, tumor burden, measurable disease, and number of disease sites). No meaningful exposure-response relationship was observed for any safety endpoints.
Exposure-response relationships for efficacy were inconsistent across exposure metrics; model-predicted cycle 1 C showed the strongest exposure-response trend. The Q1 subgroup based on model-predicted cycle 1 C had numerically similar or better OS and PFS versus control following covariate adjustment. The approved T-DM1 dose (3.6 mg/kg every 3 weeks) has a positive benefit-risk ratio versus control, even for the T-DM1 Q1 subgroup.
在III期EMILIA研究中,与卡培他滨联合拉帕替尼(对照)相比,曲妥珠单抗Emtansine(T-DM1)显著改善了既往接受过治疗的人表皮生长因子受体2阳性晚期乳腺癌患者的无进展生存期(PFS)和总生存期(OS)。利用EMILIA研究数据,我们评估了T-DM1的暴露-反应关系。
采用四种暴露指标[模型预测的和观察到的最低浓度(C)以及第1周期T-DM1从第0天至第21天的浓度-时间曲线下面积]以及多个疗效(OS、PFS、客观缓解率)和安全性(≥3级不良事件、≥3级血小板减少、≥3级肝毒性)终点来研究暴露-反应关系。
在模型预测的暴露指标与疗效之间观察到明显的暴露-反应趋势;观察到的暴露指标的趋势较浅且通常不显著。尽管模型预测的第1周期C较高的患者的中位OS和PFS在数值上长于较低者,但在调整基线风险因素(如东部肿瘤协作组状态、肿瘤负荷、可测量疾病和疾病部位数量)后,T-DM1治疗的最低暴露四分位数(Q1)患者与对照相比的OS和PFS风险比<1。对于任何安全性终点均未观察到有意义的暴露-反应关系。
不同暴露指标之间疗效的暴露-反应关系不一致;模型预测的第1周期C显示出最强的暴露-反应趋势。基于模型预测的第1周期C的Q1亚组在协变量调整后与对照相比的OS和PFS在数值上相似或更好。即使对于T-DM1 Q1亚组,批准的T-DM1剂量(每3周3.6mg/kg)与对照相比也具有良好的效益风险比。
