Garcia-Manero Guillermo, Tibes Raoul, Kadia Tapan, Kantarjian Hagop, Arellano Martha, Knight Emily A, Xiong Hao, Qin Qin, Munasinghe Wijith, Roberts-Rapp Lisa, Ansell Peter, Albert Daniel H, Oliver Brian, McKee Mark D, Ricker Justin L, Khoury Hanna Jean
MD Anderson Cancer Center, Houston, TX, USA,
Invest New Drugs. 2015 Aug;33(4):870-80. doi: 10.1007/s10637-015-0242-6. Epub 2015 May 2.
Ilorasertib (ABT-348) is a novel inhibitor of Aurora kinase, vascular endothelial growth factor (VEGF) and platelet-derived growth factor receptors, and the Src families of tyrosine kinases. Ilorasertib alone or in combination with azacitidine demonstrated activity in preclinical models in various hematological malignancies, indicating that pan-Aurora kinase and multiple kinase inhibition may have preferential antileukemic activity. This phase 1 trial determined the safety, pharmacokinetics, and preliminary antitumor activity of ilorasertib alone or combined with azacitidine in advanced hematologic malignancies.
Fifty-two patients (median age, 67 years; 35 % with >4 prior regimens) with acute myelogenous leukaemia (AML; n = 38), myelodysplastic syndrome (n = 12), or chronic myelomonocytic leukaemia (n = 2) received 3 or 6 doses of ilorasertib per 28-day cycle and were assigned to arm A (once-weekly oral), B (twice-weekly oral), C (once-weekly oral plus azacitidine), or D (once-weekly intravenous) treatment.
Maximum tolerated doses were not determined; the recommended phase 2 oral monotherapy doses were 540 mg once weekly and 480 mg twice weekly. The most common grade 3/4 adverse events were hypertension (28.8 %), hypokalemia (15.4 %), anemia (13.5 %), and hypophosphatemia (11.5 %). Oral ilorasertib pharmacokinetics appeared dose proportional, with a 15-hour half-life and no interaction with azacitidine. Ilorasertib inhibited biomarkers for Aurora kinase and VEGF receptors, and demonstrated clinical responses in 3 AML patients.
Ilorasertib exhibited acceptable safety and pharmacokinetics at or below the recommended phase 2 dose, displayed evidence of dual Aurora kinase and VEGF receptor kinase inhibition, and activity in AML.
伊洛拉塞替布(ABT - 348)是一种新型的极光激酶、血管内皮生长因子(VEGF)和血小板衍生生长因子受体以及Src家族酪氨酸激酶抑制剂。伊洛拉塞替布单独使用或与阿扎胞苷联合使用在多种血液系统恶性肿瘤的临床前模型中均显示出活性,表明泛极光激酶和多激酶抑制可能具有优先的抗白血病活性。这项1期试验确定了伊洛拉塞替布单独使用或与阿扎胞苷联合使用在晚期血液系统恶性肿瘤中的安全性、药代动力学和初步抗肿瘤活性。
52例患者(中位年龄67岁;35%接受过4种以上既往治疗方案),其中急性髓系白血病(AML;n = 38)、骨髓增生异常综合征(n = 12)或慢性粒单核细胞白血病(n = 2)患者,每28天周期接受3或6剂伊洛拉塞替布,并被分配到A组(每周一次口服)、B组(每周两次口服)、C组(每周一次口服加阿扎胞苷)或D组(每周一次静脉注射)治疗。
未确定最大耐受剂量;推荐的2期口服单药治疗剂量为每周一次540 mg和每周两次480 mg。最常见的3/4级不良事件为高血压(28.8%)、低钾血症(15.4%)、贫血(13.5%)和低磷血症(11.5%)。口服伊洛拉塞替布的药代动力学呈剂量比例关系,半衰期为15小时,且与阿扎胞苷无相互作用。伊洛拉塞替布抑制极光激酶和VEGF受体的生物标志物,并在3例AML患者中显示出临床反应。
伊洛拉塞替布在推荐的2期剂量或以下表现出可接受的安全性和药代动力学,显示出双重极光激酶和VEGF受体激酶抑制的证据以及在AML中的活性。
