摘要P2-17-05:强效雄激素受体(AR)阻滞剂proxalutamide (GT0918)在转移性乳腺癌(mBC)患者中的安全性、药代动力学和药效学评价:I期剂量递增试验

Huiping Li, R. Ran, G. Song, Hanfang Jiang, Ruyan Zhang, Yaxin Liu, Luping Meng, Phoebe Zhang, Ke-qi Chen, Qiaoxia Zhou, K. Zhou, Y. Tong
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The secondary objectives are to assess pharmacokinetics and pharmacodynamics of GT0918 with single and multiple dosage applications. (CTR20170757) Methods: Patients (pts) with historically confirmed mBC who had progressed after either chemotherapy, hormonal or targeted therapy, or could not tolerate currently standard therapies were eligible. With the starting dose at 100 mg of GT0918, the decision of dose escalation in the 3+3 design was based on the safety and tolerability assessments. GT0918 was administered orally once, followed by a 7-day off-treatment period for single dose PK analysis of drug elimination. Then GT0918 oral administration was resumed once daily for 28 consecutive days and multiple dose PK analysis was assessed at the end of first cycle (28 days). The first 28-days on treatment (cycle 1) was defined as DLT period. Pts manifesting an objective response or stable disease and likely to have clinical benefit from continued treatment were continued on GT0918 thereafter until they experienced one of following events of intolerable toxicities, disease progression or withdrew consent. Results: 18 pts were enrolled and treated with GT0918 since 9/6/2017 as defined in protocol at five dose levels: 100 mg (n = 3), 200 mg (n = 4), 300 mg (n = 4), 400 mg (n = 4) and 500 mg (n = 3) (as to 7/2/2019). All pts progressed more than two lines of therapies with 83.3% (15/18) pts were treated ≥3rd lines. Out of 6 confirmed AR positive pts, two (33.3%) at 300 mg cohort had finished 17 and 19 cycles individually and continue treatment (as 7/2/19). No DLT was observed and MTD has not been reached. GT0918 related adverse events (AEs) were grade 1 or 2 as per CTCAE v4.03, including fatigue, hypertriglyceridemia, anemia, hypercholesterolemia, increased LDL, nausea, loss of appetite, increased ALT, increase of weight loss, constipation and thrombocytopenia. PK profile analysis showed that in the single-dose study, GT0918 showed a fast absorption profile. In the multiple-dose study, the steady-state serum concentration level of GT0918 and its main metabolite were attained at 21 days. Conclusions: Proxalutamide (GT0918) administrated orally once a day is well tolerated in late-stage pts. No DLT has occurred at maximum dose 500 mg. Pts with AR positive biomarker could have better clinical outcomes with GT0918 treatment. GT0918 and its main metabolite exhibited a nonlinear pharmacokinetic profile over the dose range from 100mg to 500 mg. 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引用次数: 1

摘要

背景:雄激素受体(AR)阻滞剂在治疗BC中越来越受关注,其中约60-80%的患者显示AR阳性。然而,目前还没有AR阻滞剂被批准用于mBC。GT0918是一种新的AR阻滞剂化学实体,可能下调AR。该研究是一项开放标签、单中心、剂量递增的I期试验,旨在评估GT0918在中国接受全身治疗后进展的mBC女性患者中的作用。主要目标是确定最大耐受剂量(MTD)和剂量限制性毒性(dlt)。次要目的是评估GT0918单剂量和多剂量应用的药代动力学和药效学。方法:既往确诊的mBC患者(pts)在化疗、激素或靶向治疗后进展,或不能耐受目前的标准治疗。GT0918起始剂量为100mg,在3+3设计中,剂量递增的决定是基于安全性和耐受性评估。GT0918口服1次,停药7 d,进行单剂量药物消除PK分析。然后恢复GT0918口服,每天1次,连续28 d,在第一个周期(28 d)结束时进行多剂量PK分析。治疗前28天(第1周期)定义为DLT期。表现出客观反应或疾病稳定且可能从继续治疗中获得临床益处的患者此后继续使用GT0918,直到他们经历以下无法忍受的毒性、疾病进展或撤回同意的事件之一。结果:自2017年6月9日起,18名患者入组并接受GT0918治疗,根据方案定义,五个剂量水平:100 mg (n = 3), 200 mg (n = 4), 300 mg (n = 4), 400 mg (n = 4)和500 mg (n = 3)(截至2019年7月2日)。所有患者的治疗进展均超过2条线,其中83.3%(15/18)患者的治疗≥3条线。在6例确诊的AR阳性患者中,2例(33.3%)300 mg组分别完成了17和19个周期并继续治疗(截至7/2/19)。未观察到DLT,未达到MTD。根据CTCAE v4.03, GT0918相关不良事件(ae)为1级或2级,包括疲劳、高甘油三酯血症、贫血、高胆固醇血症、低密度脂蛋白升高、恶心、食欲不振、ALT升高、体重减轻、便秘和血小板减少。PK谱分析显示,在单剂量研究中,GT0918表现出快速吸收谱。在多剂量研究中,在第21天获得GT0918及其主要代谢物的稳态血清浓度水平。结论:替卡鲁胺(GT0918)在晚期患者中具有良好的耐受性。最大剂量500mg未发生DLT。AR生物标志物阳性的患者使用GT0918治疗可获得更好的临床结果。GT0918及其主要代谢物在100mg ~ 500mg剂量范围内呈非线性药代动力学特征。GT0918的抗肿瘤活性和安全性已在中国启动了一项扩展/ Ib期治疗AR阳性mBC患者的研究。分别取200mg和300mg进行剂量扩展。引用格式:李慧萍,冉然,宋国红,蒋汉芳,张汝燕,刘亚欣,孟路平,张菲比,陈珂,周乔霞,周卡尔,童幼智。强效雄激素受体(AR)阻滞剂proxalutamide (GT0918)在转移性乳腺癌(mBC)患者中的安全性、药代动力学和药效学评估:I期剂量递增试验[摘要]。摘自:2019年圣安东尼奥乳腺癌研讨会论文集;2019年12月10日至14日;费城(PA): AACR;中国癌症杂志,2020;31(增刊):02 - 02 - 02。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Abstract P2-17-05: Evaluation of safety, pharmacokinetics and pharmacodynamics of proxalutamide (GT0918), a potent androgen receptor (AR) blocker, in patients with metastatic breast cancer (mBC): Phase I dose escalation trial
Background: Androgen receptor (AR) blocker has become an increased interest in the treatment of BC, in which about 60-80% patients showed AR positive. However, currently no AR blocker has been approved in mBC. GT0918 is a new chemical entity of AR blocker with possible AR down-regulation. This study is an open-label, single-center, dose escalation phase I trial to assess GT0918 in mBC female patients who have progressed after systemic treatments in China. The primary objectives are to identify the maximum tolerated dose (MTD) and dose-limiting toxicities (DLTs). The secondary objectives are to assess pharmacokinetics and pharmacodynamics of GT0918 with single and multiple dosage applications. (CTR20170757) Methods: Patients (pts) with historically confirmed mBC who had progressed after either chemotherapy, hormonal or targeted therapy, or could not tolerate currently standard therapies were eligible. With the starting dose at 100 mg of GT0918, the decision of dose escalation in the 3+3 design was based on the safety and tolerability assessments. GT0918 was administered orally once, followed by a 7-day off-treatment period for single dose PK analysis of drug elimination. Then GT0918 oral administration was resumed once daily for 28 consecutive days and multiple dose PK analysis was assessed at the end of first cycle (28 days). The first 28-days on treatment (cycle 1) was defined as DLT period. Pts manifesting an objective response or stable disease and likely to have clinical benefit from continued treatment were continued on GT0918 thereafter until they experienced one of following events of intolerable toxicities, disease progression or withdrew consent. Results: 18 pts were enrolled and treated with GT0918 since 9/6/2017 as defined in protocol at five dose levels: 100 mg (n = 3), 200 mg (n = 4), 300 mg (n = 4), 400 mg (n = 4) and 500 mg (n = 3) (as to 7/2/2019). All pts progressed more than two lines of therapies with 83.3% (15/18) pts were treated ≥3rd lines. Out of 6 confirmed AR positive pts, two (33.3%) at 300 mg cohort had finished 17 and 19 cycles individually and continue treatment (as 7/2/19). No DLT was observed and MTD has not been reached. GT0918 related adverse events (AEs) were grade 1 or 2 as per CTCAE v4.03, including fatigue, hypertriglyceridemia, anemia, hypercholesterolemia, increased LDL, nausea, loss of appetite, increased ALT, increase of weight loss, constipation and thrombocytopenia. PK profile analysis showed that in the single-dose study, GT0918 showed a fast absorption profile. In the multiple-dose study, the steady-state serum concentration level of GT0918 and its main metabolite were attained at 21 days. Conclusions: Proxalutamide (GT0918) administrated orally once a day is well tolerated in late-stage pts. No DLT has occurred at maximum dose 500 mg. Pts with AR positive biomarker could have better clinical outcomes with GT0918 treatment. GT0918 and its main metabolite exhibited a nonlinear pharmacokinetic profile over the dose range from 100mg to 500 mg. An expanded/phase Ib in AR positive mBC pts has launched in China to evaluate the anti-tumor activity and safety of GT0918. 200 mg and 300 mg were selected for dose expansion. Citation Format: Huiping Li, Ran Ran, Guohong Song, Hanfang Jiang, Ruyan Zhang, Yaxin Liu, Luping Meng, Phoebe Zhang, Ke Chen, Qiaoxia Zhou, Karl Zhou, Youzhi Tong. Evaluation of safety, pharmacokinetics and pharmacodynamics of proxalutamide (GT0918), a potent androgen receptor (AR) blocker, in patients with metastatic breast cancer (mBC): Phase I dose escalation trial [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr P2-17-05.
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