Pasritamig, a First-in-Class, Bispecific T-Cell Engager Targeting Human Kallikrein 2, in Metastatic Castration-Resistant Prostate Cancer: A Phase I Study.

IF 42.1 1区医学 Q1 ONCOLOGY

Journal of Clinical Oncology Pub Date : 2025-06-01 DOI:10.1200/JCO-25-00678

Mark N Stein, Armelle Vinceneux, Debbie Robbrecht, Bernard Doger, Karen A Autio, Michael T Schweizer, Emiliano Calvo, Laura Medina, Marloes Van Dongen, Jean-Laurent Deville, Alice Bernard-Tessier, Debopriya Ghosh, Kristin Shotts, Fei Shen, Pharavee Jaiprasart, Ruchi Chaudhary, Shujian Wu, Leanne Cartee, Robert Schnepp, Daria Gaut, Josh Lauring, Sherry C Wang, Victor M Villalobos, Capucine Baldini

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引用次数: 0

Abstract

Purpose: We report phase I trial results for pasritamig, a first-in-class, T-cell-engaging bispecific antibody targeting human kallikrein 2 (KLK2) expressed on the surface of prostate cancer (PC) cells.

Methods: Participants had metastatic castration-resistant PC and ≥1 prior therapy. Pasritamig was escalated from 0.5 mg to 2,000 mg for subcutaneous administration and from 150 mg to 900 mg for intravenous (IV) administration at dosing frequencies ranging from once every week to once every 6 weeks with different step-up dosing schedules. The primary objectives were to determine safety and the recommended phase II dose (RP2D) of pasritamig. Secondary objectives included preliminary assessment of antitumor activity.

Results: One hundred seventy-four participants received pasritamig, with a median of 4 prior lines of systemic therapy. Treatment-related adverse events (TRAEs) occurred in 144 of 174 (82.8%) participants, with 17 of 174 (9.8%) experiencing grade ≥3 TRAEs. The RP2D was determined to be 3.5 mg (day 1), 18 mg (day 8), 300 mg (day 15), and then 300 mg IV once every 6 weeks. In the RP2D safety population (n = 45), infusion-related reactions (11/45, 24.4%), fatigue (7/45, 15.6%), cytokine release syndrome (CRS; 4/45, 8.9%, all grade 1), and lipase increase (4/45, 8.9%) were the most frequent TRAEs; all were grade 1 or 2. In the RP2D efficacy population (n = 33), median radiographic progression-free survival was 7.85 (95% CI, 2.89 to not estimable) months, and 14 of 33 (42.4%) participants achieved a ≥50% decrease from baseline in prostate-specific antigen.

Conclusion: Pasritamig demonstrated a favorable safety profile with very low rates of CRS and could be safely administered in an outpatient setting. Preliminary antitumor activity demonstrated proof of concept for KLK2 as a target in PC, warranting further development of pasritamig.

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Pasritamig，一种一流的双特异性t细胞结合剂，靶向人Kallikrein 2，用于转移性去势抵抗性前列腺癌：1期研究

pasritamig是一种一流的t细胞双特异性抗体，靶向表达在前列腺癌（PC）细胞表面的人钾化因子2 （KLK2）。方法：参与者有转移性去势抵抗性PC，既往治疗≥1次。Pasritamig皮下给药从0.5 mg增加到2000 mg，静脉（IV）给药从150 mg增加到900 mg，给药频率从每周到每6周，不同的加速给药计划。主要目的是确定pasritamig的安全性和推荐的2期剂量（RP2D）。次要目的包括初步评估抗肿瘤活性。结果：174名参与者接受了帕西坦格治疗，平均既往接受4次全身治疗。144/174（82.8%）名参与者发生了治疗相关不良事件（TRAEs）， 17/174（9.8%）名参与者发生了≥3级TRAEs。RP2D测定为3.5 mg（第1天），18 mg（第8天），300 mg（第15天），然后每6周300 mg IV。在RP2D安全人群（N=45）中，输注相关反应（11/45,24.4%）、疲劳（7/45,15.6%）、细胞因子释放综合征(CRS；4/45（8.9%，均为1级）和脂肪酶升高（4/45,8.9%）是最常见的TRAEs；都是一年级或二年级学生。在RP2D有效人群（N=33）中，中位放射无进展生存期为7.85个月（95% CI 2.89，不可估计），14/33（42.4%）参与者的前列腺特异性抗原下降≥50%。结论：Pasritamig具有良好的安全性，CRS发生率极低，可以安全地用于门诊。初步的抗肿瘤活性证明了KLK2作为PC靶点的概念，为pasritamig的进一步开发提供了依据。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Clinical Oncology 医学-肿瘤学

CiteScore

41.20

自引率

2.20%

发文量

8215

审稿时长

2 months

期刊介绍： The Journal of Clinical Oncology serves its readers as the single most credible, authoritative resource for disseminating significant clinical oncology research. In print and in electronic format, JCO strives to publish the highest quality articles dedicated to clinical research. Original Reports remain the focus of JCO, but this scientific communication is enhanced by appropriately selected Editorials, Commentaries, Reviews, and other work that relate to the care of patients with cancer.