Martinelli Giovanni, Oehler Vivian G, Papayannidis Cristina, Courtney Rachel, Shaik M Naveed, Zhang Xiaoxi, O'Connell Ashleigh, McLachlan Karen R, Zheng Xianxian, Radich Jerald, Baccarani Michele, Kantarjian Hagop M, Levin Wendy J, Cortes Jorge E, Jamieson Catriona
Department of Experimental, Diagnostic and Specialty Medicine (DIMES), University of Bologna, Bologna, Italy.
Clinical Research Division, Fred Hutchinson Cancer Research Center, Seattle, WA, USA.
Lancet Haematol. 2015 Aug;2(8):e339-46. doi: 10.1016/S2352-3026(15)00096-4. Epub 2015 Jul 26.
Activation of the Hedgehog signalling pathway contributes to cancer progression and the development of myeloid leukaemia stem cell therapeutic resistance. We aimed to identify the maximum tolerated dose (MTD) and the recommended phase 2 dose of the selective Hedgehog antagonist PF-04449913 in myeloid malignancies.
We undertook an open-label, dose-finding, standard 3+3 design phase 1 study of PF-04449913 in adult patients with acute myeloid leukaemia, chronic myeloid leukaemia, chronic myelomonocytic leukaemia, myelodysplastic syndrome, or myelofibrosis who were refractory, resistant, or intolerant to previous treatments, at three centres in the USA and one in Italy. Patients who had newly diagnosed, untreated disease were included if they were not eligible for standard treatment options or if standard treatments were not deemed appropriate. Patients received PF-04449913 once daily continuously until disease progression, unacceptable toxic effects, or patient withdrawal for up to 12 28-day cycles. Additional cycles were given if patients showed evidence of clinical benefit. The starting dose was 5 mg and was increased by 100% until the first dose-limiting toxic effect (DLT) and by 50% thereafter, in keeping with a 3+3 clinical trial statistical design. The primary endpoint was first-cycle DLTs. Secondary endpoints were safety, tolerability, pharmacokinetics, pharmacodynamics, and preliminary clinical activity. This trial is registered with ClinicalTrials.gov, number NCT00953758.
Between March 24, 2010, and Sept 7, 2012, 47 patients were enrolled and included in the study: 28 with acute myeloid leukaemia, six with myelodysplastic syndrome, five with chronic myeloid leukaemia (two with chronic-phase and three with blast-phase disease), one with chronic myelomonocytic leukaemia, and seven with myelofibrosis. Patients received PF-04449913 once daily at 5 mg (n=3), 10 mg (n=3), 20 mg (n=4), 40 mg (n=4), 80 mg (n=8), 120 mg (n=3), 180 mg (n=3), 270 mg (n=5), 400 mg (n=9), and 600 mg (n=5). Two patients experienced DLTs (one each in the 80 mg and 600 mg dose groups). The MTD for PF-04449913 was established to be 400 mg once daily. Of the 47 patients enrolled, 28 (60%) experienced treatment-related adverse events, three of which were grade 4 in severity. The most common treatment-related adverse events included dysgeusia (13 [28%] patients), decreased appetite (nine [19%]), and alopecia (seven [15%]). None of the 15 deaths reported were treatment related. Pharmacokinetics seemed to be dose proportional. The mean half-life was 23·9 h (SD 14·0) in the MTD group. Some suggestion of clinical activity was noted in 23 (49%) of 47 patients with haematological malignancies. Based on these results, the recommended phase 2 dose was 200 mg or lower once daily.
Based on these findings, PF-04449913 is being tested in phase 2 studies in patients with myelodysplastic syndrome, acute myeloid leukaemia, and myelofibrosis.
Pfizer.
刺猬信号通路的激活有助于癌症进展以及髓系白血病干细胞治疗耐药性的发展。我们旨在确定选择性刺猬拮抗剂PF - 04449913在髓系恶性肿瘤中的最大耐受剂量(MTD)和推荐的2期剂量。
我们在美国的三个中心和意大利的一个中心,对患有急性髓系白血病、慢性髓系白血病、慢性粒单核细胞白血病、骨髓增生异常综合征或骨髓纤维化且对先前治疗难治、耐药或不耐受的成年患者,开展了一项开放标签、剂量探索、标准3 + 3设计的PF - 04449913 1期研究。如果新诊断、未接受治疗的患者不符合标准治疗方案或标准治疗被认为不合适,则将其纳入研究。患者持续每日接受一次PF - 04449913治疗,直至疾病进展、出现不可接受的毒性作用或患者退出,最长可达12个28天周期。如果患者显示出临床获益的证据,则给予额外的周期。起始剂量为5 mg,按照3 + 3临床试验统计设计,在出现首个剂量限制性毒性作用(DLT)之前每次剂量增加100%,之后每次增加50%。主要终点是首个周期的DLT。次要终点是安全性、耐受性、药代动力学、药效学和初步临床活性。本试验已在ClinicalTrials.gov注册,编号为NCT00953758。
在2010年3月24日至2012年9月7日期间,47例患者入组并纳入研究:28例急性髓系白血病患者、6例骨髓增生异常综合征患者、5例慢性髓系白血病患者(2例慢性期和3例急变期)、1例慢性粒单核细胞白血病患者和7例骨髓纤维化患者。患者每日接受一次PF - 04449913治疗,剂量分别为5 mg(n = 3)、10 mg(n = 3)、20 mg(n = 4)、40 mg(n = 4)、80 mg(n = 8)、120 mg(n = 3)、180 mg(n = 3)、270 mg(n = 5)、400 mg(n = 9)和600 mg(n = 5)。2例患者出现DLT(80 mg和600 mg剂量组各1例)。确定PF - 04449913的MTD为每日一次400 mg。在入组的47例患者中,28例(60%)经历了与治疗相关的不良事件,其中3例严重程度为4级。最常见的与治疗相关的不良事件包括味觉障碍(13例[28%]患者)、食欲减退(9例[19%])和脱发(7例[15%])。报告的15例死亡均与治疗无关。药代动力学似乎呈剂量比例关系。MTD组的平均半衰期为23.9小时(标准差14.0)。在47例血液系统恶性肿瘤患者中的23例(49%)观察到了一些临床活性迹象。基于这些结果,推荐的2期剂量为每日一次200 mg或更低。
基于这些发现,PF - 04449913正在针对骨髓增生异常综合征、急性髓系白血病和骨髓纤维化患者进行2期研究测试。
辉瑞公司。
