Department of Supportive Oncology, Institute for Oncology and Radiology of Serbia, Belgrade, Serbia.
Helsinn Healthcare SA, Lugano/Pazzallo, Switzerland.
Int J Gynecol Cancer. 2018 Jul;28(6):1153-1161. doi: 10.1097/IGC.0000000000001292.
Patients with gynecological cancers are at high risk for chemotherapy-induced nausea and vomiting (CINV) after platinum-based chemotherapy (CT). NEPA (300-mg netupitant, 0.50-mg palonosetron) is the first oral fixed-combination antiemetic. Pivotal trials demonstrated the superiority of oral NEPA over intravenous palonosetron in preventing CINV after highly emetogenic (anthracycline-cyclophosphamide-based [AC] and cisplatin-based [non-AC]) CT. This post hoc subset analysis considered patients with gynecological cancer receiving cisplatin- or carboplatin-based CT from 1 pivotal trial and from 1 multicycle safety trial to evaluate the efficacy of oral NEPA in preventing CINV.
Single-dose NEPA was given before CT in combination with dexamethasone. The efficacy end points for the acute (0-24 hours), delayed (25-120 hours), and overall (0-120 hours) CINV phases after CT included complete response (CR; no emesis, no rescue medication) and no significant nausea (<25 mm on a 0- to 100-mm visual analog scale). Safety was also assessed.
For cisplatin-induced CINV, NEPA achieved high CR rates (acute phase: >90%; delayed, overall phases: ≥85%). For carboplatin-induced CINV, NEPA was also highly effective, with high acute, delayed, and overall CR rates (cycle 1: >75%; cycles 2-4: >95%). No significant nausea rates were more than 90% and more than 80% in the acute and delayed phases, respectively, for patients receiving cisplatin or carboplatin. NEPA was well tolerated.
Results suggest that oral NEPA is effective and safe in preventing CINV in patients with gynecological cancers treated with cisplatin- or carboplatin-based CT. Single fixed-combination NEPA is a convenient option for CINV prevention in high-risk CINV patients.
接受铂类化疗(CT)的妇科癌症患者发生化疗引起的恶心和呕吐(CINV)的风险较高。NEPA(300mg 奈妥吡坦、0.50mg 帕洛诺司琼)是首个口服固定剂量组合止吐药。关键性试验显示,与静脉用帕洛诺司琼相比,口服 NEPA 可预防高度致吐性化疗(蒽环类环磷酰胺[AC]和顺铂[非 AC])后 CINV。该事后亚组分析考虑了来自 1 项关键性试验和 1 项多周期安全性试验的接受顺铂或卡铂 CT 的妇科癌症患者,以评估口服 NEPA 预防 CINV 的疗效。
在 CT 前给予单剂量 NEPA,联合地塞米松。CT 后急性(0-24 小时)、延迟(25-120 小时)和总体(0-120 小时)CINV 期的疗效终点包括完全缓解(CR;无呕吐,无解救药物)和无显著恶心(0-100mm 视觉模拟量表上<25mm)。还评估了安全性。
对于顺铂引起的 CINV,NEPA 达到了高 CR 率(急性期:>90%;延迟期和总体期:≥85%)。对于卡铂引起的 CINV,NEPA 也非常有效,具有高急性、延迟和总体 CR 率(第 1 周期:>75%;第 2-4 周期:>95%)。在接受顺铂或卡铂的患者中,无显著恶心率在急性和延迟期分别超过 90%和 80%。NEPA 耐受良好。
结果表明,在接受顺铂或卡铂 CT 的妇科癌症患者中,口服 NEPA 对预防 CINV 有效且安全。单一固定剂量组合的 NEPA 是高风险 CINV 患者预防 CINV 的便捷选择。
