Phase I first-in-human dose escalation study of the oral casein kinase 1α and cyclin dependent kinase 7/9 inhibitor BTX A51 in advanced MDS and AML

IF 29.5 1区医学 Q1 HEMATOLOGY

Journal of Hematology & Oncology Pub Date : 2025-07-15 DOI:10.1186/s13045-025-01724-z

Brian J. Ball, Wenbin Xiao, Gautam Borthakur, Le Xuan Truong Nguyen, Melissa Valerio, Avanthika Venkatachalam, Guido Marcucci, Anthony S. Stein, Dung Luong Thai, David N. Cook, Kyle Chan, Sonali Persaud, Ross L. Levine, Omar Abdel-Wahab, Yinon Ben-Neriah, Eytan M. Stein

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Abstract

BTX A51, a first-in-class oral small molecule inhibitor of casein kinase 1α (CK1α) and cyclin-dependent kinase (CDK) 7 and 9, induces apoptosis of leukemic cells by activating p53 and inhibiting expression of Mcl1. Here, we report on the results of the phase 1 clinical trial of BTX A51 in patients with relapsed or refractory AML and MDS. Adult patients with R/R AML and high-risk MDS were enrolled into eight potential doses ranging from 1 to 42 mg dosed orally three days/week for 21 or 28 days out of a 28-day cycle. The maximum tolerated dose, recommended phase 2 dose (RP2D), safety, pharmacokinetics (PK), and pharmacodynamics (PD) of BTX A51 were investigated. Thirty-one patients were enrolled and received treatment with BTX A51. Median age was 75 (range 22- 84) and 55% were male. Most patients (97%) had received prior treatment with venetoclax and hypomethylating agents. The most common treatment-emergent adverse events of any grade were nausea (67%), emesis (63%), hypokalemia (53%), and diarrhea (40%). Two patients experienced hepatic toxicity as DLTs, which resolved upon holding treatment. No treatment-related deaths occurred. The recommended phase 2 dose was 21 mg dosed three days/week for 4 weeks of a 28-day cycle. BTX A51 increased the expression of p53 and reduced the expression of MCL1 and RNA polymerase II phosphorylation in pre- and post-treatment immunocytochemistry studies. Overall, 3 patients (10%) experienced complete remission with incomplete count recovery (CRi). All 3 responding patients had RUNX1 mutations and the CR/CRi rate for RUNX1-mutated patients receiving BTX A51 at efficacious doses (11 mg or higher) was 30%. Ex-vivo studies confirmed higher efficacy of BTX A51 on RUNX1-mutated myeloblasts and demonstrated synergy with azacitidine and venetoclax. Although the overall efficacy was modest, this study lays the groundwork for future studies with improved patient selection and combination approaches. NCT04872166.

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口服酪蛋白激酶1α和细胞周期蛋白依赖性激酶7/9抑制剂BTX A51治疗晚期MDS和AML的I期首次人体剂量递增研究

BTX A51是一种酪蛋白激酶1α (CK1α)和细胞周期蛋白依赖性激酶（CDK） 7和9的口服小分子抑制剂，通过激活p53和抑制Mcl1的表达诱导白血病细胞凋亡。在这里，我们报告BTX A51在复发或难治性AML和MDS患者中的1期临床试验结果。患有R/R AML和高风险MDS的成年患者被纳入8个潜在剂量，范围为1至42毫克，口服3天/周，为期21或28天。研究了BTX A51的最大耐受剂量、推荐2期剂量（RP2D）、安全性、药代动力学（PK）和药效学（PD）。31例患者接受BTX A51治疗。中位年龄为75岁（22- 84岁），55%为男性。大多数患者（97%）之前接受过venetoclax和低甲基化药物的治疗。最常见的治疗不良事件是恶心（67%）、呕吐（63%）、低钾血症（53%）和腹泻（40%）。2例患者作为dlt出现肝毒性，在坚持治疗后消退。无治疗相关死亡发生。推荐的2期剂量为21毫克，每周3天，为期4周，28天周期。在治疗前后的免疫细胞化学研究中，BTX A51增加了p53的表达，降低了MCL1和RNA聚合酶II磷酸化的表达。总体而言，3名患者（10%）经历了完全缓解和不完全计数恢复（CRi）。所有3例应答患者均有RUNX1突变，接受有效剂量（11mg或更高）BTX A51治疗的RUNX1突变患者的CR/CRi率为30%。离体研究证实BTX A51对runx1突变的成髓细胞有更高的疗效，并与阿扎胞苷和venetoclax有协同作用。虽然总体疗效不高，但本研究为未来改进患者选择和联合方法的研究奠定了基础。NCT04872166。

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来源期刊

Journal of Hematology & Oncology 医学-血液学

CiteScore

48.10

自引率

2.10%

发文量

169

审稿时长

6-12 weeks

期刊介绍： The Journal of Hematology & Oncology, an open-access journal, publishes high-quality research covering all aspects of hematology and oncology, including reviews and research highlights on "hot topics" by leading experts. Given the close relationship and rapid evolution of hematology and oncology, the journal aims to meet the demand for a dedicated platform for publishing discoveries from both fields. It serves as an international platform for sharing laboratory and clinical findings among laboratory scientists, physician scientists, hematologists, and oncologists in an open-access format. With a rapid turnaround time from submission to publication, the journal facilitates real-time sharing of knowledge and new successes.