Safety and anti-tumor activity of BAY 2927088 in patients with HER2-mutant NSCLC: Results from an expansion cohort of the SOHO-01 phase I/II study.

IF 2.1 3区工程技术 Q3 CHEMISTRY, MULTIDISCIPLINARY

Journal of Chemical & Engineering Data Pub Date : 2024-06-10 DOI:10.1200/jco.2024.42.17_suppl.lba8598

Nicolas Girard, Tae Min Kim, Hye Ryun Kim, Herbert H. Loong, Y. Shinno, Shun Lu, Yong Fang, Jun Zhao, K. Nishino, Ki Hyeong Lee, Liyun Miao, T. Sakamoto, E. Felip, Tsung-Ying Yang, C. Dooms, Daniel Shao-Weng Tan, X. Le, J. C. Brase, Paolo Grassi, Koichi Goto

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引用次数: 0

Abstract

LBA8598 Background: HER2 ( ERBB2) mutations have been reported in approximately 2-4% of patients (pts) with NSCLC, with exon 20 insertions being the most common. BAY 2927088 is an oral, reversible tyrosine kinase inhibitor that potently inhibits mutant HER2 and mutant EGFR in preclinical models. Encouraging objective responses were observed in pts with NSCLC harboring a HER2-activating mutation and treated with BAY 2927088 in the dose-escalation/backfill part of the Phase I/II SOHO-01 trial (NCT05099172). More recently the FDA has granted Breakthrough Therapy designation for BAY 2927088 for previously treated pts with advanced NSCLC and activating HER2 mutations. Here we report the safety, anti-tumor activity, and longitudinal circulating tumor DNA (ctDNA) data in a cohort of pts treated with BAY 2927088 from the expansion part of this trial. Methods: Pts with advanced NSCLC harboring a HER2-activating mutation and who experienced disease progression after at least 1 systemic therapy, but naïve to HER2-targeted therapy, were enrolled and received BAY 2927088 at 20 mg twice daily. Plasma samples were collected at baseline and several on-treatment time points for longitudinal ctDNA profiling using next-generation sequencing (NGS; Oncomine Precision Assay). Results: As of February 19, 2024, 34 pts were treated with BAY 2927088, with a median follow-up of 8 months. Median age was 62 years, 68% were female, 74% had never smoked, and 53% had received ≥2 lines of systemic anti-cancer therapy. Median duration of treatment with BAY 2927088 was 7.1 months (range 0.2-9.2). Treatment was ongoing in 17 pts (50%). Ten pts had a dose reduction, 8 had dose interruptions, and 3 discontinued study treatment due to a drug-related adverse event. The most common adverse events were diarrhea (85%; mainly grade 1-2) and rash (47%; grade 1-2). In 33 pts evaluable for efficacy, responses were observed in 23 (objective response rate 70%; 95% CI 51.3, 84.4) and 5 (15%) had stable disease for a disease control rate of 82% (95% CI 64.5, 93.0). Responses were rapid (median time to response 5.7 weeks) and durable (median duration of response not reached). Median progression-free survival was 8.1 months (95% CI 4.4, not evaluable). In a subset of 20 pts with successful paired (baseline, on-treatment) blood NGS and detectable HER2 ctDNA at baseline, 19/20 (95%) had a decrease in ctDNA and 1 pt with progressive disease had an increase in ctDNA; 15/20 (75%) had no detectable ctDNA after 6 weeks of treatment (including 3/4 pts with stable disease). Conclusions: BAY 2927088 led to rapid, substantial, and durable responses in pts with pretreated HER2-mutant NSCLC. The safety profile was consistent with previously reported data. These data support the further clinical development of BAY 2927088 in pts with HER2-mutant NSCLC. Clinical trial information: NCT05099172 .

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BAY 2927088对HER2突变NSCLC患者的安全性和抗肿瘤活性：SOHO-01 I/II期研究扩大队列的结果。

LBA8598 背景：据报道，约有 2-4% 的 NSCLC 患者（pts）存在 HER2（ERBB2）突变，其中最常见的是外显子 20 插入。BAY 2927088 是一种口服、可逆的酪氨酸激酶抑制剂，在临床前模型中能有效抑制突变的 HER2 和突变的表皮生长因子受体。在 I/II 期 SOHO-01 试验（NCT05099172）的剂量递增/回补部分，对携带 HER2 激活突变的 NSCLC 患者使用 BAY 2927088 治疗后，观察到了令人鼓舞的客观反应。最近，FDA授予BAY 2927088 "突破性疗法 "称号，用于既往接受过治疗的晚期NSCLC患者和激活HER2突变患者。在此，我们报告了该试验扩展部分中接受 BAY 2927088 治疗的一组患者的安全性、抗肿瘤活性和纵向循环肿瘤 DNA (ctDNA) 数据。研究方法入组患者均为携带HER2激活突变的晚期NSCLC患者，至少接受过一次全身治疗后疾病出现进展，但对HER2靶向疗法还不熟悉，接受BAY 2927088治疗，剂量为20毫克，每天两次。在基线和几个治疗时间点采集血浆样本，使用新一代测序技术（NGS；Oncomine Precision Assay）进行纵向ctDNA分析。结果截至2024年2月19日，34名患者接受了BAY 2927088治疗，中位随访时间为8个月。中位年龄为62岁，68%为女性，74%从未吸烟，53%接受过≥2次全身抗癌治疗。BAY 2927088治疗的中位持续时间为7.1个月（0.2-9.2个月）。17例患者（50%）仍在接受治疗。10例患者减少了剂量，8例患者中断了剂量，3例患者因药物相关不良事件中止了研究治疗。最常见的不良反应是腹泻（85%；主要是1-2级）和皮疹（47%；1-2级）。在33例可进行疗效评估的患者中，23例观察到应答（客观应答率为70%；95% CI为51.3, 84.4），5例（15%）病情稳定，疾病控制率为82%（95% CI为64.5, 93.0）。反应迅速（中位反应时间为 5.7 周）且持久（中位反应持续时间未达到）。中位无进展生存期为 8.1 个月（95% CI 4.4，无法评估）。在成功配对（基线、治疗中）血液 NGS 且基线可检测到 HER2 ctDNA 的 20 例患者中，19/20（95%）例患者的 ctDNA 有所下降，1 例疾病进展患者的 ctDNA 有所上升；15/20（75%）例患者在治疗 6 周后未检测到 ctDNA（包括 3/4 例疾病稳定患者）。结论：BAY 2927088能使预处理的HER2突变NSCLC患者获得快速、实质性和持久的应答。其安全性与之前报告的数据一致。这些数据支持 BAY 2927088 在 HER2 突变 NSCLC 患者中的进一步临床开发。临床试验信息：NCT05099172 .

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来源期刊

Journal of Chemical & Engineering Data 工程技术-工程：化工

CiteScore

5.20

自引率

19.20%

发文量

324

审稿时长

2.2 months

期刊介绍： The Journal of Chemical & Engineering Data is a monthly journal devoted to the publication of data obtained from both experiment and computation, which are viewed as complementary. It is the only American Chemical Society journal primarily concerned with articles containing data on the phase behavior and the physical, thermodynamic, and transport properties of well-defined materials, including complex mixtures of known compositions. While environmental and biological samples are of interest, their compositions must be known and reproducible. As a result, adsorption on natural product materials does not generally fit within the scope of Journal of Chemical & Engineering Data.