Medical Clinic and Policlinic I, Hematology and Cellular Therapy, University Hospital Leipzig, Johannisallee 32, D-04103, Leipzig, Germany.
Department of Hematology and Medical Oncology, University Hospital Frankfurt, Frankfurt, Germany.
BMC Cancer. 2022 May 21;22(1):569. doi: 10.1186/s12885-022-09622-0.
This report summarizes three phase I studies evaluating volasertib, a polo-like kinase inhibitor, plus azacitidine in adults with myelodysplastic syndromes (MDS), chronic myelomonocytic leukemia, or acute myeloid leukemia.
Patients received intravenous volasertib in 28-day cycles (dose-escalation schedules). In Part 1 of 1230.33 (Study 1; NCT01957644), patients received 250-350 mg volasertib on day (D)1 and D15; in Part 2, patients received different schedules [A, D1: 170 mg/m; B, D7: 170 mg/m; C, D1 and D7: 110 mg/m]. In 1230.35 (Study 2; NCT02201329), patients received 200-300 mg volasertib on D1 and D15. In 1230.43 (Study 3; NCT02721875), patients received 110 mg/m volasertib on D1 and D8. All patients in Studies 1 and 2, and approximately half of the patients in Study 3, were scheduled to receive subcutaneous azacitidine 75 mg/m on D1-7.
Overall, 22 patients were treated (17 with MDS; 12 previously untreated). Across Studies 1 and 2 (n = 21), the most common drug-related adverse events were hematological (thrombocytopenia [n = 11]; neutropenia [n = 8]). All dose-limiting toxicities were grade 4 thrombocytopenia. The only treated patient in Study 3 experienced 18 adverse events following volasertib monotherapy. Studies 1 and 2 showed preliminary activity (objective response rates: 25 and 40%).
The safety of volasertib with azacitidine in patients with MDS was consistent with other volasertib studies. All studies were terminated prematurely following the discontinuation of volasertib for non-clinical reasons by Boehringer Ingelheim; however, safety information on volasertib plus azacitidine are of interest for future studies in other diseases.
本报告总结了三项评估伏拉塞替尼(一种 Polo 样激酶抑制剂)联合阿扎胞苷治疗骨髓增生异常综合征(MDS)、慢性粒单核细胞白血病或急性髓系白血病患者的 I 期研究。
患者接受 28 天周期的静脉注射伏拉塞替尼(剂量递增方案)。在 1230.33 研究(研究 1;NCT01957644)的第 1 部分中,患者在第 1 天(D1)和第 15 天(D15)接受 250-350mg 伏拉塞替尼;在第 2 部分中,患者接受不同的方案[A,D1:170mg/m;B,D7:170mg/m;C,D1 和 D7:110mg/m]。在 1230.35 研究(研究 2;NCT02201329)中,患者在 D1 和 D15 接受 200-300mg 伏拉塞替尼。在 1230.43 研究(研究 3;NCT02721875)中,患者在 D1 和 D8 接受 110mg/m 伏拉塞替尼。研究 1 和 2 的所有患者以及研究 3 中的约一半患者均计划在 D1-7 接受皮下阿扎胞苷 75mg/m。
共有 22 名患者接受治疗(17 名患有 MDS;12 名初治)。在研究 1 和 2 中(n=21),最常见的药物相关不良事件是血液学毒性(血小板减少症[n=11];中性粒细胞减少症[n=8])。所有剂量限制性毒性均为 4 级血小板减少症。研究 3 中唯一接受治疗的患者在伏拉塞替尼单药治疗后出现 18 种不良事件。研究 1 和 2 显示出初步疗效(客观缓解率:25%和 40%)。
MDS 患者伏拉塞替尼联合阿扎胞苷的安全性与其他伏拉塞替尼研究一致。所有研究均因勃林格殷格翰公司出于非临床原因停止使用伏拉塞替尼而提前终止;然而,伏拉塞替尼联合阿扎胞苷的安全性信息对于其他疾病的未来研究具有重要意义。
