GSK3326595用于髓系肿瘤患者的临床活性和安全性的I/II期研究。
Phase I/II study of the clinical activity and safety of GSK3326595 in patients with myeloid neoplasms.
作者信息
Watts Justin, Minden Mark D, Bachiashvili Kimo, Brunner Andrew M, Abedin Sameem, Crossman Timothy, Zajac Magdalena, Moroz Veronica, Egger Jacqueline L, Tarkar Aarti, Kremer Brandon E, Barbash Olena, Borthakur Gautam
机构信息
Division of Hematology, Sylvester Comprehensive Cancer Center, University of Miami, Miami, FL, USA.
Department of Medical Oncology and Hematology, Princess Margaret Cancer Center, University Health Network, Toronto, ON, Canada.
出版信息
Ther Adv Hematol. 2024 Sep 14;15:20406207241275376. doi: 10.1177/20406207241275376. eCollection 2024.
BACKGROUND
GSK3326595 is a potent, selective, reversible protein arginine methyltransferase 5 (PRMT5) inhibitor under investigation for treatment of myelodysplastic syndrome (MDS), chronic myelomonocytic leukemia (CMML), and acute myeloid leukemia (AML). In preclinical models of AML, PRMT5 inhibition decreased proliferation and increased cell death, supporting additional clinical research in myeloid neoplasms.
OBJECTIVES
To determine the clinical activity, safety, tolerability, dosing, additional measures of clinical activity, pharmacokinetics, and pharmacodynamics of GSK3326595.
DESIGN
In part 1 of this open-label, multicenter, multipart, phase I/II study, adults with relapsed/refractory myeloid neoplasms (e.g., MDS, CMML, and AML) received monotherapy with 400 or 300 mg oral GSK3326595 once daily. Study termination occurred prior to part 2 enrollment.
METHODS
Clinical activity was determined by the clinical benefit rate (CBR; proportion of patients achieving complete remission (CR), complete marrow remission (mCR), partial remission, stable disease (SD) >8 weeks, or hematologic improvement). Adverse events (AEs) were assessed by incidence and severity. Exploratory examination of spliceosome mutations was performed to determine the relationship between genomic profiles and clinical response to GSK3326595.
RESULTS
Thirty patients with a median age of 73.5 years (range, 47-90) were enrolled; 13 (43%) and 17 (57%) received 400 and 300 mg of GSK3326595, respectively. Five (17%) patients met CBR criteria: 4 (13%) with SD >8 weeks and 1 (3%) achieving mCR. Of five patients with clinical benefit: three had SRSF2 mutation, one U2AF1, and one was splicing factor wild-type. Frequent GSK3326595-related AEs were decreased platelet count (27%), dysgeusia (23%), fatigue (20%), and nausea (20%). GSK3326595 had rapid absorption, with a of approximately 2 h and a terminal half-life of 4-6 h.
CONCLUSION
GSK3326595 monotherapy had limited clinical activity in heavily pretreated patients despite robust target engagement. The safety profile was broadly consistent with other published PRMT5 inhibitor studies.
TRIAL REGISTRATION
ClinicalTrials.gov: NCT03614728.
背景
GSK3326595是一种强效、选择性、可逆的蛋白质精氨酸甲基转移酶5(PRMT5)抑制剂,目前正处于研究阶段,用于治疗骨髓增生异常综合征(MDS)、慢性粒单核细胞白血病(CMML)和急性髓系白血病(AML)。在AML的临床前模型中,PRMT5抑制可降低细胞增殖并增加细胞死亡,这为在髓系肿瘤中开展更多临床研究提供了支持。
目的
确定GSK3326595的临床活性、安全性、耐受性、给药剂量、临床活性的其他指标、药代动力学和药效学。
设计
在这项开放标签、多中心、多部分的I/II期研究的第1部分中,复发/难治性髓系肿瘤(如MDS、CMML和AML)的成年患者接受了每日一次口服400或300 mg GSK3326595的单药治疗。在第2部分入组前研究终止。
方法
通过临床获益率(CBR;达到完全缓解(CR)、完全骨髓缓解(mCR)、部分缓解、疾病稳定(SD)>8周或血液学改善的患者比例)来确定临床活性。通过发生率和严重程度评估不良事件(AE)。对剪接体突变进行探索性检查,以确定基因组图谱与GSK3326595临床反应之间的关系。
结果
共纳入30例患者,中位年龄73.5岁(范围47 - 90岁);分别有13例(43%)和17例(57%)接受了400 mg和300 mg的GSK3326595治疗。5例(17%)患者符合CBR标准:4例(13%)疾病稳定>8周,1例(3%)达到mCR。在5例有临床获益的患者中:3例有SRSF2突变,1例有U2AF1突变,1例剪接因子为野生型。常见的与GSK3326595相关的AE包括血小板计数降低(27%)、味觉障碍(23%)、疲劳(20%)和恶心(20%)。GSK3326595吸收迅速,达峰时间约为2小时,终末半衰期为4 - 6小时。
结论
尽管GSK3326595能有效作用于靶点,但其单药治疗在经过大量预处理的患者中临床活性有限。安全性概况与其他已发表的PRMT5抑制剂研究大致一致。
试验注册
ClinicalTrials.gov:NCT03614728。
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