Sun Pharmaceutical Industries Limited (SPIL), 17 B Mahal Industrial Estate, Mahakali Caves Road, Andheri (East), Mumbai, Maharashtra, 400093, India.
Cancer Chemother Pharmacol. 2018 Sep;82(3):521-532. doi: 10.1007/s00280-018-3643-3. Epub 2018 Jul 11.
To compare the pharmacokinetic bioequivalence and safety of a generic pegylated liposomal doxorubicin formulation (SPIL DXR hydrochloride liposome injection) with that of the reference products, Caelyx or Doxil.
Two open-label, two-way reference crossover studies were conducted in patients with ovarian cancer. C, AUC, and AUC, V, and Cl for total, free, and encapsulated DXR were evaluated in 18 blood samples taken pre-dose (t = 0), at increasing time intervals over the following 14 days. A washout period of 28 days was observed before crossing over.
Studies 1 and 2 were completed by 24/29 and 41/60 patients, respectively. Pharmacokinetic data from 24 patients from each study established bioequivalence for free DXR in study 2, and for total and encapsulated DXR in both studies. Data from 29 and 54 patients, respectively, were included in the safety evaluation. Of these, 37 patients experienced 81 post-dose adverse events (40 related to the test product and 41 related to the reference product). In study 1, four patients were withdrawn owing to adverse events. Eleven patients experienced serious adverse events and one death occurred in study 2.
Bioequivalence between the test and the reference products was established for total and encapsulated DXR in both studies, and for free DXR in the study with the larger sample size (study 2). There were no significant differences between the safety profiles of the generic formulation and the reference products. No correlation was found between drug level and adverse events.
Study 1 was registered retrospectively; registration number is NCT03055143, dated February 15, 2017. Study 2 registration number is NCT00862355, dated March 13, 2009.
比较通用型聚乙二醇脂质体阿霉素制剂(SPIL 盐酸多柔比星脂质体注射液)与参比制剂(Caelyx 或 Doxil)的药代动力学生物等效性和安全性。
在卵巢癌患者中进行了两项开放标签、两周期、参比交叉研究。在 18 名患者中,共采集了 18 个血样,在以下 14 天内以递增时间间隔采集,在给药前(t=0)和 14 天内的多个时间点采集,以评估总多柔比星、游离多柔比星、包裹多柔比星的 C、AUC 和 AUC,V 和 Cl。在交叉之前,观察了 28 天的洗脱期。
分别有 24/29 名和 41/60 名患者完成了研究 1 和研究 2。来自每个研究的 24 名患者的药代动力学数据证实了研究 2 中游离多柔比星的生物等效性,以及两项研究中总多柔比星和包裹多柔比星的生物等效性。分别有 29 名和 54 名患者纳入安全性评估。其中,37 名患者发生 81 次给药后不良事件(40 次与试验药物相关,41 次与参比药物相关)。在研究 1 中,4 名患者因不良事件退出。在研究 2 中,11 名患者发生严重不良事件,1 名患者死亡。
在两项研究中,与参比产品相比,通用型制剂的总多柔比星和包裹多柔比星,以及在样本量较大的研究 2 中游离多柔比星,均显示出生物等效性。通用型制剂与参比产品的安全性特征无显著差异。未发现药物水平与不良事件之间存在相关性。
研究 1 是追溯性注册;注册号为 NCT03055143,日期为 2017 年 2 月 15 日。研究 2 的注册号为 NCT00862355,日期为 2009 年 3 月 13 日。
