PF-06952229, a selective TGF-β-R1 inhibitor: preclinical development and a first-in-human, phase I, dose-escalation study in advanced solid tumors

IF 7.1 2区医学 Q1 ONCOLOGY ESMO Open Pub Date : 2024-09-01 DOI:10.1016/j.esmoop.2024.103653

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引用次数: 0

Abstract

Background

PF-06952229 is a selective small-molecule inhibitor of transforming growth factor-β (TGF-β) receptor 1. We evaluated its antitumor activity in preclinical studies and its safety, tolerability, pharmacokinetics, and pharmacodynamics in a phase I study (NCT03685591).

Patients and methods

In vitro and in vivo preclinical studies were conducted. Patients (aged ≥18 years) received PF-06952229 monotherapy [20-500 mg, oral b.i.d., 7 days on/7 days off, 28-day cycles, Part 1A (P1A)] for advanced/metastatic solid tumors and combination therapy [250/375 mg with enzalutamide, Part 1B (P1B)] for metastatic castration-resistant prostate cancer (mCRPC). Primary endpoints were dose-limiting toxicity (DLT), adverse events (AEs), and laboratory abnormalities. Efficacy, pharmacokinetic parameters, and biomarker modulation were assessed.

Results

PF-06952229 showed activity in preclinical murine tumor models including pSMAD2 modulation in tumors. The study (NCT03685591) enrolled 49 patients (P1A, n = 42; P1B, n = 7). DLTs were reported in 3/35 (8.6%) P1A patients receiving PF-06952229 375 mg (anemia, intracranial tumor hemorrhage, and anemia and hypertension, all grade 3, n = 1 each). The most frequent grade 3 treatment-related AEs (TRAEs) were alanine aminotransferase increased and anemia (9.5% each). There were no grade 4-5 TRAEs. Plasma PF-06952229 exposures were dose proportional between 80 and 375 mg. Pharmacodynamic studies confirmed target modulation of pSMAD2/3 (peripheral monocytes). One P1A patient with prostate cancer receiving PF-06952229 375 mg monotherapy achieved confirmed partial response (31-month duration of response). A total of 8 patients (P1A, n = 6; P1B, n = 2) achieved stable disease.

Conclusions

Antitumor activity of PF-06952229 was observed in preclinical studies. PF-06952229 was generally well tolerated with manageable toxicity; a small group of patients achieved durable responses and/or disease stabilization.

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PF-06952229 是一种选择性 TGF-β-R1 抑制剂：在晚期实体瘤中的临床前开发和首次人体 I 期剂量递增研究

背景PF-06952229是一种转化生长因子-β（TGF-β）受体1的选择性小分子抑制剂。我们在临床前研究中评估了它的抗肿瘤活性，并在一项 I 期研究（NCT03685591）中评估了它的安全性、耐受性、药代动力学和药效学。患者（年龄≥18岁）接受PF-06952229单药治疗[20-500毫克，口服，b.i.d.，7天/7天，28天周期，1A部分（P1A）]治疗晚期/转移性实体瘤，以及联合治疗[250/375毫克与恩杂鲁胺，1B部分（P1B）]治疗转移性耐受性前列腺癌（mCRPC）。主要终点为剂量限制性毒性（DLT）、不良事件（AE）和实验室异常。结果PF-06952229在临床前小鼠肿瘤模型中显示出活性，包括对肿瘤中pSMAD2的调节。该研究（NCT03685591）共招募了 49 名患者（P1A，n = 42；P1B，n = 7）。接受 PF-06952229 375 mg 治疗的 P1A 患者中，3/35（8.6%）例出现 DLT（贫血、颅内肿瘤出血、贫血和高血压，均为 3 级，每例 1 例）。最常见的 3 级治疗相关不良反应（TRAE）是丙氨酸氨基转移酶升高和贫血（各占 9.5%）。没有出现 4-5 级 TRAE。血浆 PF-06952229 暴露量在 80 至 375 毫克之间呈剂量比例关系。药效学研究证实了对 pSMAD2/3（外周单核细胞）的靶向调节作用。一名接受 PF-06952229 375 毫克单药治疗的 P1A 前列腺癌患者获得了证实的部分应答（应答持续时间为 31 个月）。结论在临床前研究中观察到了 PF-06952229 的抗肿瘤活性。PF-06952229的耐受性普遍良好，毒性可控；一小部分患者获得了持久的应答和/或疾病稳定。

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来源期刊

ESMO Open Medicine-Oncology

CiteScore

11.70

自引率

2.70%

发文量

255

审稿时长

10 weeks

期刊介绍： ESMO Open is the online-only, open access journal of the European Society for Medical Oncology (ESMO). It is a peer-reviewed publication dedicated to sharing high-quality medical research and educational materials from various fields of oncology. The journal specifically focuses on showcasing innovative clinical and translational cancer research. ESMO Open aims to publish a wide range of research articles covering all aspects of oncology, including experimental studies, translational research, diagnostic advancements, and therapeutic approaches. The content of the journal includes original research articles, insightful reviews, thought-provoking editorials, and correspondence. Moreover, the journal warmly welcomes the submission of phase I trials and meta-analyses. It also showcases reviews from significant ESMO conferences and meetings, as well as publishes important position statements on behalf of ESMO. Overall, ESMO Open offers a platform for scientists, clinicians, and researchers in the field of oncology to share their valuable insights and contribute to advancing the understanding and treatment of cancer. The journal serves as a source of up-to-date information and fosters collaboration within the oncology community.