Safety, pharmacokinetics, pharmacodynamics, and antitumor activity of SAR439459, a TGFβ inhibitor, as monotherapy and in combination with cemiplimab in patients with advanced solid tumors: Findings from a phase 1/1b study

IF 3.1 3区医学 Q2 MEDICINE, RESEARCH & EXPERIMENTAL

Cts-Clinical and Translational Science Pub Date : 2024-06-19 DOI:10.1111/cts.13854

Joaquina C. Baranda, Debbie Robbrecht, Ryan Sullivan, Bernard Doger, Armando Santoro, Minal Barve, Jean-Jacques Grob, Oliver Bechter, Maria Vieito, Maria Jose de Miguel, Dirk Schadendorf, Melissa Johnson, Clemence Pouzin, Cathy Cantalloube, Rui Wang, Jooyun Lee, Xiaofei Chen, Brigitte Demers, Amele Amrate, Giovanni Abbadessa, F. Stephen Hodi

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引用次数: 0

Abstract

SAR439459 (SAR'459), a “second-generation” human anti-transforming growth factor beta (TGFβ) monoclonal antibody, enhances the activity of immune checkpoint inhibitors. In this phase I/Ib study, we evaluated the safety, pharmacokinetics (PK), pharmacodynamics, and antitumor activity of SAR'459 ± cemiplimab (intravenous) in patients with advanced solid tumors. Increasing doses of SAR'459 were administered every 2 or 3 weeks (Q2W, Q3W) alone (Part 1A) or with 3 mg/kg cemiplimab Q2W or 350 mg Q3W (Part 1B). In Part 2A (dose expansion), melanoma patients were randomly (1:1) administered 22.5 or 7.5 mg/kg SAR'459. In Part 2B (dose expansion), 22.5 mg/kg SAR'459 and 350 mg cemiplimab Q3W were administered. The primary end points were maximum tolerated dose (MTD) or maximum administered dose (MAD; Part 1), preliminary antitumor activity (Part 2B), and optimal monotherapy dose (Part 2A). Twenty-eight and 24 patients were treated in Parts 1A and 1B, respectively; MTD was not reached, MAD was 15 (Q2W) and 22.5 mg/kg (Q3W) alone and in combination, respectively. Fourteen and 95 patients, including 14 hepatocellular carcinoma (HCC) patients, were treated in Parts 2A and 2B, respectively. The population PK model yielded satisfactory goodness-of-fit plots and adequately described the observed data by a two-compartment PK model with linear elimination. Objective responses were not observed in Parts 1 and 2A. In Part 2B, objective response rate was 8.4% and 7.1% across tumor types and the HCC cohort, respectively. The most frequent treatment-emergent adverse effects were hemorrhagic events (43.5%), keratoacanthoma (6.8%), and skin neoplasms (6.2%). Fatal bleeding occurred in 21.4% HCC patients despite the implementation of mitigation measures. SAR'459 monotherapy and combination with cemiplimab appeared relatively safe and tolerable in limited number of patients in dose escalation. However, the study was discontinued due to the unclear efficacy of SAR'459 and bleeding risk, particularly in HCC patients.

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TGFβ 抑制剂 SAR439459 单药治疗和与 cemiplimab 联合治疗晚期实体瘤患者的安全性、药代动力学、药效学和抗肿瘤活性：1/1b期研究结果。

SAR439459（SAR'459）是一种 "第二代 "人类抗转化生长因子β（TGFβ）单克隆抗体，可增强免疫检查点抑制剂的活性。在这项I/Ib期研究中，我们评估了SAR'459±cemiplimab（静脉注射）在晚期实体瘤患者中的安全性、药代动力学（PK）、药效学和抗肿瘤活性。SAR'459每2周或3周（Q2W、Q3W）单独给药（第1A部分），或与3毫克/千克塞米单抗Q2W或350毫克Q3W一起给药（第1B部分）。在第 2A 部分（剂量扩展）中，黑色素瘤患者随机（1:1）接受 22.5 或 7.5 毫克/千克 SAR'459。在第2B部分（剂量扩展）中，给黑色素瘤患者服用22.5毫克/千克SAR'459和350毫克cemiplimab Q3W。主要终点是最大耐受剂量（MTD）或最大给药剂量（MAD；第1部分）、初步抗肿瘤活性（第2B部分）和最佳单药治疗剂量（第2A部分）。第 1A 部分和第 1B 部分分别治疗了 28 名和 24 名患者；未达到 MTD，单药和联合用药的最大给药剂量分别为 15 毫克/千克（Q2W）和 22.5 毫克/千克（Q3W）。第 2A 部分和第 2B 部分分别治疗了 14 名和 95 名患者，其中包括 14 名肝细胞癌（HCC）患者。群体 PK 模型得出了令人满意的拟合优度图，并通过线性消除的两室 PK 模型充分描述了观察到的数据。在第 1 部分和第 2A 部分中未观察到客观反应。在第 2B 部分中，各肿瘤类型和 HCC 队列的客观反应率分别为 8.4% 和 7.1%。最常见的治疗突发不良反应是出血事件（43.5%）、角化棘皮瘤（6.8%）和皮肤肿瘤（6.2%）。尽管采取了缓解措施，但仍有 21.4% 的 HCC 患者出现致命性出血。在剂量递增过程中，SAR'459 单药治疗和与塞米普利单抗联合治疗在少数患者中显得相对安全和耐受。然而，由于SAR'459的疗效不明确以及出血风险，尤其是对HCC患者的出血风险，研究被迫中止。

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来源期刊

Cts-Clinical and Translational Science 医学-医学：研究与实验

CiteScore

6.70

自引率

2.60%

发文量

234

审稿时长

6-12 weeks

期刊介绍： Clinical and Translational Science (CTS), an official journal of the American Society for Clinical Pharmacology and Therapeutics, highlights original translational medicine research that helps bridge laboratory discoveries with the diagnosis and treatment of human disease. Translational medicine is a multi-faceted discipline with a focus on translational therapeutics. In a broad sense, translational medicine bridges across the discovery, development, regulation, and utilization spectrum. Research may appear as Full Articles, Brief Reports, Commentaries, Phase Forwards (clinical trials), Reviews, or Tutorials. CTS also includes invited didactic content that covers the connections between clinical pharmacology and translational medicine. Best-in-class methodologies and best practices are also welcomed as Tutorials. These additional features provide context for research articles and facilitate understanding for a wide array of individuals interested in clinical and translational science. CTS welcomes high quality, scientifically sound, original manuscripts focused on clinical pharmacology and translational science, including animal, in vitro, in silico, and clinical studies supporting the breadth of drug discovery, development, regulation and clinical use of both traditional drugs and innovative modalities.