742双特异性4-1BB和PD-L1抗体INBRX-105单独和联合pembrolizumab在选定实体瘤中的1/2期研究

Jong Chul Park, David Berz, Manish Sharma, Erminia Massarelli, Ralph J Hauke, Frank Yung-Chin Tsai, David Hong, Neal Akhave, Justin A Call, Jennifer Carlisle, Rachel E Sanborn, Naomi B Haas, John Hamm, D Ross Camidge, Alexander I Spira, Vasily Andrianov, Brianne O’Neill, Heather Kinkead, Anthony W Tolcher
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引用次数: 0

摘要

背景4-1BB是一种在肿瘤浸润淋巴细胞上上调的共刺激受体。4-1BB信号传导促进t细胞增殖和活化,减少t细胞衰竭。4-1BB激动剂显示出有希望的抗肿瘤活性,但由于全身4-1BB激活引起的肝毒性而受到限制。INBRX-105是一种4-1BB×PD-L1双特异性抗体,旨在将4-1BB共刺激信号定位到富含pd - l1的环境中。INBRX-105由2个激动性4-1BB单域抗体(sabs)和2个PD-L1单域抗体组成,可锚定PD-L1。INBRX-105将PD-L1与4-1BB交联,导致PD-L1高表达位点有条件的4-1BB激活,潜在地限制了先前4-1BB激动剂相关的毒性。在小鼠肿瘤模型中,INBRX-105替代物(INBRX-105-a)表现出抗肿瘤功效,并增加了肿瘤微环境中的t细胞频率在瘤内和外周血中观察到CD8+ T效应记忆细胞的强劲增殖。INBRX-105-a加PD-1拮抗剂对肿瘤生长有更大的抑制作用。我们描述了在实体瘤患者中单独使用INBRX-105和联合使用pembrolizumab的1/2期研究(NCT03809624)。方法:这项开放标签、4部分的INBRX-105±pembrolizumab治疗局部晚期不可切除/转移性实体瘤(N≈300)的研究正在美国进行(图1)。第3部分(组合)已经完成。INBRX-105正在剂量扩展队列中进行评估(第2部分,INBRX-105单药;第4部分,组合)。首次使用4-1BB激动剂的患者,尽管接受标准治疗,但病情进展或没有其他治疗方案(检查点抑制剂[CPI]初始队列除外)。2a部分(推荐的2期剂量[RP2D]扩大)包括4个队列:非小细胞肺癌(NSCLC;PD-L1+)、黑色素瘤/实体瘤、头颈部鳞状细胞癌(HNSCC)和其他实体瘤(PD-L1+)。2b部分包括pd - l1高的HNSCC(包括鼻咽癌)。除黑色素瘤(非皮肤)/实体瘤外,所有第2部分队列均为CPI复发/难治性。PD-L1+ NSCLC (2a部分)和PD-L1高HNSCC (2b部分)队列基于鼓励早期单药活性而开放。队列正在登记,完整的数据即将公布。第4部分包括cpi复发/难治队列(PD-L1+ NSCLC、皮肤黑色素瘤、PD-L1+ HNSCC、微卫星不稳定性/肿瘤突变负担高或错配修复缺陷的实体肿瘤)和cpi初始队列(PDL1+ NSCLC和HNSCC)。第2部分和第4部分需要PD-L1免疫组织化学评分,每个方案定义阈值评分。主要目标是安全性和确定INBRX-105作为单药和派姆单抗的最大耐受剂量和/或RP2D。次要目标包括药代动力学、免疫原性和RECIST的初步抗肿瘤活性。金凯德,马塞多,张国华,等。与双特异性PD-L1条件4-1BB激动剂抗肿瘤活性相关的关键药代动力学和药效学参数[J]中华肿瘤杂志,2013;抽象的12。本研究方案由各参与机构的机构审查委员会审查并批准;所有患者均提供书面知情同意书。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
742 Phase 1/2 study of the bispecific 4–1BB and PD-L1 antibody INBRX-105 alone and in combination with pembrolizumab in select solid tumors

Background

4–1BB is a costimulatory receptor upregulated on tumor-infiltrating lymphocytes. 4–1BB signaling promotes T-cell proliferation and activation and decreases T-cell exhaustion. 4–1BB agonists have shown promising antitumor activity but have been limited by hepatotoxicity resulting from systemic 4–1BB activation. INBRX-105 is a 4–1BB×PD-L1 bispecific antibody designed to localize 4–1BB costimulatory signaling to PD-L1-rich environments. INBRX-105 consists of 2 agonistic 4–1BB single-domain antibodies (sdAbs) and 2 PD-L1 sdAbs, which allow anchoring to PD-L1. Cross-linking of PD-L1 to 4–1BB by INBRX-105 leads to conditional 4–1BB activation at sites of high PD-L1 expression, potentially limiting toxicities associated with prior 4–1BB agonists. In mouse tumor models, an INBRX-105 surrogate (INBRX-105-a) exhibited antitumor efficacy and increased T-cell frequency in the tumor microenvironment.1 Robust proliferation of CD8+ T effector memory cells was observed intratumorally and in peripheral blood. INBRX-105-a plus a PD-1 antagonist resulted in greater inhibition of tumor growth. We describe a phase 1/2 study (NCT03809624) of INBRX-105 alone and in combination with pembrolizumab in patients with solid tumors.

Methods

This open-label, 4-part study of INBRX-105±pembrolizumab in locally advanced unresectable/metastatic solid tumors (N≈300) is enrolling in the US (figure 1). Dose escalation (part 1, INBRX-105 single agent; part 3, combination) was completed. INBRX-105 is being assessed in dose-expansion cohorts (part 2, INBRX-105 single agent; part 4, combination). Patients naive to 4–1BB agonists with disease that progressed despite standard therapy or who have no alternative treatment options (except checkpoint inhibitor [CPI]-naive cohorts) were included. Part 2a (recommended phase 2 dose [RP2D] expansion) consists of 4 cohorts: non-small cell lung cancer (NSCLC; PD-L1+), melanoma/solid tumors, head and neck squamous cell carcinoma (HNSCC), and other solid tumors (PD-L1+). Part 2b includes PD-L1-high HNSCC (including nasopharyngeal carcinoma). All part 2 cohorts, except melanoma (noncutaneous)/solid tumors, were CPI relapsed/refractory. PD-L1+ NSCLC (part 2a) and PD-L1-high HNSCC (part 2b) cohorts were opened based on encouraging early single-agent activity. Cohorts are enrolling and complete data readouts are forthcoming. Part 4 consists of CPI-relapsed/refractory cohorts (PD-L1+ NSCLC, cutaneous melanoma, PD-L1+ HNSCC, microsatellite instability-/tumor mutation burden-high or mismatch repair-deficient solid tumors) and CPI-naive cohorts (PDL1+ NSCLC and HNSCC). PD-L1 immunohistochemistry scores are required in parts 2 and 4, with threshold scores defined per protocol. Primary objectives are safety and determination of the maximum tolerated dose and/or RP2D of INBRX-105 as monotherapy and with pembrolizumab. Secondary objectives include pharmacokinetics, immunogenicity, and preliminary antitumor activity per RECIST.

Trial Registration

Clinicaltrials.gov identifier, NCT03809624

Reference

Kinkead H, Macedo C, Sanabria A, et al. Key pharmacokinetic and pharmacodynamic parameters that correlate with the anti-tumor activity of a bispecific PD-L1 conditional 4–1BB agonist. J Immunother Cancer. 2021;9. Abstract 12.

Ethics Approval

The study protocol was reviewed and approved by the institutional review board at each participating institution; all patients provided written informed consent.
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