Yale School of Public Health, Yale University, New Haven, CT, USA.
Yale New Haven Hospital, Yale University, New Haven, CT, USA.
Support Care Cancer. 2021 Jul;29(7):3439-3459. doi: 10.1007/s00520-020-05935-7. Epub 2021 Jan 13.
The aim of this study is to rigorously review the efficacy and safety of olanzapine in defined hematology oncology settings including (1) the setting of highly emetogenic chemotherapy (HEC) and moderately emetogenic chemotherapy (MEC) settings (2) at 5 mg and 10 mg doses, and (3) for response rates for use in the acute, delayed, and overall settings post-MEC and HEC.
Ovid MEDLINE, Embase, and Cochrane Central Register of Controlled Trials were searched through April 23, 2020. The primary efficacy endpoints were the rate of complete response, in the acute (0-24 h post-chemotherapy), delayed (24-120 h post-chemotherapy), and overall (0-120 h post-chemotherapy) phases. The secondary efficacy endpoints were the rates of no nausea and no emesis, for each phase. Safety endpoints were the rate of no serious adverse events (i.e., no grade 3 or 4 toxicities), as assessed by Common Terminology Criteria for Adverse Events (CTCAE) criteria. The Mantel-Haenszel, random-effects analysis model was used to compute risk ratios and accompanying 95% confidence intervals for each endpoint. For endpoints that statistically favored one arm, absolute risk differences were computed to assess whether there is a 10% or greater difference, used as the threshold for clinical significance by MASCC/ESMO. Fragility indices were also calculated for each statistically significant endpoint, to quantitatively assess the robustness of the summary estimate. A cumulative meta-analysis was conducted for each efficacy meta-analysis with more than 5 studies, also using the Mantel-Haenszel random-effects analysis model.
Three studies reported on olanzapine for the rescue of breakthrough chemotherapy-induced nausea and vomiting (CINV); 22 studies reported on olanzapine in the prophylactic setting. For studies reporting on HEC patients, olanzapine-containing regimens were statistically and clinically superior in seven of nine efficacy endpoints in the prophylaxis setting. When olanzapine is administered at a 10-mg dose, it is statistically and clinically superior to control patients in eight of nine endpoints among adults. Olanzapine may be effective in the MEC setting and when administered at 5-mg doses, but the paucity of data leads to notable uncertainty.
Further RCTs are needed in the setting of MEC patients and administration of olanzapine at a lower 5-mg dose, which may be given to reduce the sedative effect of olanzapine at 10 mg.
本研究旨在严格评估奥氮平在特定血液肿瘤学环境中的疗效和安全性,包括(1)高度致吐性化疗(HEC)和中度致吐性化疗(MEC)环境;(2)5mg 和 10mg 剂量;(3)MEC 和 HEC 后急性、延迟和总体缓解率。
通过 Ovid MEDLINE、Embase 和 Cochrane 对照试验中心注册库检索,截至 2020 年 4 月 23 日。主要疗效终点为完全缓解率,包括急性(化疗后 0-24 小时)、延迟(化疗后 24-120 小时)和总体(化疗后 0-120 小时)期。次要疗效终点为每个阶段无恶心和无呕吐的发生率。安全性终点为根据不良事件常用术语标准(CTCAE)评估的无严重不良事件(即无 3 或 4 级毒性)发生率。采用 Mantel-Haenszel、随机效应分析模型计算每个终点的风险比及其相应的 95%置信区间。对于统计学上有利于某一臂的终点,计算绝对风险差异,以评估是否存在 10%或更大的差异,MASCC/ESMO 将其用作临床意义的阈值。还对每个具有统计学意义的终点进行了脆弱性指数计算,以定量评估汇总估计的稳健性。对于每个疗效荟萃分析,如果有超过 5 项研究,还使用 Mantel-Haenszel 随机效应分析模型进行累积荟萃分析。
有 3 项研究报告了奥氮平用于解救突破性化疗引起的恶心和呕吐(CINV);22 项研究报告了奥氮平在预防中的应用。对于报告 HEC 患者的研究,奥氮平联合方案在预防环境中的 9 个疗效终点中有 7 个在统计学和临床上优于对照组。当奥氮平以 10mg 剂量给药时,在 9 个成人终点中的 8 个在统计学和临床上优于对照组。奥氮平可能在 MEC 环境中有效,且在 5mg 剂量下给药,但数据的缺乏导致了显著的不确定性。
需要在 MEC 患者中进行更多的 RCT 研究,以及奥氮平在较低的 5mg 剂量下给药,这可能有助于降低 10mg 奥氮平的镇静作用。
