Foran James, Ravandi Farhad, Wierda William, Garcia-Manero Guillermo, Verstovsek Srdan, Kadia Tapan, Burger Jan, Yule Murray, Langford Gillian, Lyons John, Ayrton John, Lock Victoria, Borthakur Gautham, Cortes Jorge, Kantarjian Hagop
University of Alabama at Birmingham Comprehensive Cancer Center, Birmingham, AL.
University of Texas MD Anderson Cancer Center, Houston, TX.
Clin Lymphoma Myeloma Leuk. 2014 Jun;14(3):223-30. doi: 10.1016/j.clml.2013.11.001. Epub 2013 Nov 14.
This study sought to identify the maximum tolerated dose (MTD) of AT9283, an inhibitor of Aurora kinases A and B, in patients with relapsed or refractory leukemias. Other endpoints included pharmacokinetics, safety and tolerability, pharmacodynamics, and preliminary evidence of efficacy.
AT9283 was administered as a continuous 72-hour infusion every 21 days. Doses were escalated by a standard 3 + 3 design. After the MTD for the 72-hour infusion was identified, infusion duration was increased incrementally to 96 hours and 120 hours. In total, 48 patients received ≥ 1 cycle of AT9283. Median age was 61 years (range, 22-86 years); 56% were men; 75% were diagnosed with AML; and 89% had received ≥ 3 (up to 16) prior lines of therapy.
324 mg/m(2)/72 h AT9283 was determined to be the MTD. Dose-limiting toxicities (DLTs) were myocardial infarction, hypertension, cardiomyopathy, tumor lysis syndrome, pneumonia, and multiorgan failure. Other AT9283-related toxicities (non-DLT) included myelosuppression, predominantly leukopenia and mucositis. Bone marrow blasts decreased ≥ 38% after AT9283 treatment in approximately one-third of patients with relapsed/refractory AML; however, this effect was transient and no objective responses were achieved, despite evidence of Aurora kinase B inhibition. Two patients with accelerated-phase chronic myeloid leukemia showed evidence of benefit, manifested as a cytogenetic response in 1 case; 1 patient completed 6 cycles of treatment. Exposure to AT9283 was generally dose proportional.
AT9283 tolerability was strongly dose-dependent, with reversible myelosuppression predominating at lower doses and events such as cardiovascular toxicities manifesting at higher doses. Clinical trials with AT9283 are ongoing in alternative patient populations.
本研究旨在确定Aurora激酶A和B的抑制剂AT9283在复发或难治性白血病患者中的最大耐受剂量(MTD)。其他终点包括药代动力学、安全性和耐受性、药效学以及疗效的初步证据。
AT9283每21天进行一次连续72小时输注给药。剂量按标准的3+3设计递增。确定72小时输注的MTD后,输注持续时间逐步增加至96小时和120小时。共有48例患者接受了≥1个周期的AT9283治疗。中位年龄为61岁(范围22-86岁);56%为男性;75%被诊断为急性髓系白血病(AML);89%曾接受过≥3(最多16)线的前期治疗。
确定324mg/m²/72h的AT9283为MTD。剂量限制性毒性(DLT)为心肌梗死、高血压、心肌病、肿瘤溶解综合征、肺炎和多器官功能衰竭。其他与AT9283相关的毒性(非DLT)包括骨髓抑制,主要是白细胞减少和粘膜炎。在约三分之一的复发/难治性AML患者中,AT9283治疗后骨髓原始细胞减少≥38%;然而,这种效应是短暂的,尽管有Aurora激酶B抑制的证据,但未实现客观缓解。2例加速期慢性髓系白血病患者显示出获益证据,1例表现为细胞遗传学缓解;1例患者完成了6个周期的治疗。AT9283的暴露量一般与剂量成比例。
AT9283的耐受性强烈依赖于剂量,较低剂量时以可逆性骨髓抑制为主,较高剂量时则出现心血管毒性等事件。针对其他患者群体的AT9283临床试验正在进行中。
