一项纳博替尼联合瑞特替尼或曲美替尼治疗晚期和转移性 KRAS 或 BRAF 突变型非小细胞肺癌患者的 Ib 期研究。
A phase Ib study of the combination of naporafenib with rineterkib or trametinib in patients with advanced and metastatic KRAS- or BRAF-mutant non-small cell lung cancer.
机构信息
Department of Medical Oncology, Thoracic Group and International Center for Thoracic Cancers (CICT), Villejuif, France; Faculty of Medicine, Paris-Saclay University, Paris, France.
Center for Integrated Oncology, University Hospital Köln, Köln, Germany.
出版信息
Lung Cancer. 2024 Nov;197:107964. doi: 10.1016/j.lungcan.2024.107964. Epub 2024 Sep 26.
BACKGROUND
Genetic alterations activating the MAPK pathway are common in non-small cell lung cancer (NSCLC). Patients with NSCLC may benefit from treatment with the pan-RAF inhibitor naporafenib (LXH254) plus the ERK1/2 inhibitor rineterkib (LTT462) or MEK1/2 inhibitor trametinib.
METHODS
This first-in-human phase 1b dose-escalation/dose-expansion study investigated the combinations of naporafenib (50-350 mg once daily [QD] or 300-600 mg twice daily [BID]) with rineterkib (100-300 mg QD) in patients with KRAS-/BRAF-mutant NSCLC and naporafenib (200 mg BID or 400 mg BID) with trametinib (0.5 mg QD, 1 mg QD or 1 mg QD 2 weeks on/2 weeks off) in patients with KRAS-/BRAF-mutant NSCLC and NRAS-mutant melanoma. The primary objectives were to identify the recommended dose for expansion (RDE) and evaluate tolerability and safety. Secondary objectives included antitumor activity and pharmacodynamics.
RESULTS
Overall, 216 patients were treated with naporafenib plus rineterkib (NSCLC: n = 101) or naporafenib plus trametinib (NSCLC: n = 79; melanoma: n = 36). In total, 10 of 62 (16%) patients experienced at least one dose-limiting toxicity. The RDEs were established as naporafenib 400 mg BID plus rineterkib 200 mg QD, naporafenib 200 mg BID plus trametinib 1 mg QD and naporafenib 400 mg BID plus trametinib 0.5 mg QD. The most frequent grade ≥ 3 treatment-related adverse event was increased lipase (8/101 [7.9%] patients) for naporafenib plus rineterkib and rash (22/115 [19.1%] patients) for naporafenib plus trametinib. Among patients with NSCLC, partial response was observed in three patients (one with KRAS-mutant, two with BRAF-mutant NSCLC) treated with naporafenib plus rineterkib and two patients (both with KRAS-mutant NSCLC) treated with naporafenib plus trametinib. On-treatment median reductions in DUSP6 mRNA levels from baseline were 45.5% and 76.1% with naporafenib plus rineterkib or trametinib, respectively.
CONCLUSIONS
Both naporafenib combinations had acceptable safety profiles. Antitumor activity was limited in patients with NSCLC, despite the observed on-target pharmacodynamic effect.
CLINICALTRIALS
gov identifier: NCT02974725.
背景
MAPK 通路的基因改变在非小细胞肺癌(NSCLC)中很常见。患有 NSCLC 的患者可能受益于使用泛 RAF 抑制剂纳博替尼(LXH254)联合 ERK1/2 抑制剂瑞替替尼(LTT462)或 MEK1/2 抑制剂曲美替尼的治疗。
方法
这是一项首次人体 1b 期剂量递增/剂量扩展研究,在 KRAS-/BRAF 突变型 NSCLC 患者中,研究了纳博替尼(50-350mg 每日一次[QD]或 300-600mg 每日两次[BID])联合瑞替替尼(100-300mg QD)的组合,在 KRAS-/BRAF 突变型 NSCLC 和 NRAS 突变型黑色素瘤患者中,研究了纳博替尼(200mg BID 或 400mg BID)联合曲美替尼(0.5mg QD、1mg QD 或 1mg QD 2 周/2 周停药)的组合。主要目的是确定扩展推荐剂量(RDE)并评估耐受性和安全性。次要目标包括抗肿瘤活性和药代动力学。
结果
共有 216 名患者接受了纳博替尼加瑞替替尼(NSCLC:n=101)或纳博替尼加曲美替尼(NSCLC:n=79;黑色素瘤:n=36)治疗。共有 62 例(16%)患者发生至少 1 例剂量限制性毒性。RDE 确定为纳博替尼 400mg BID 加瑞替替尼 200mg QD、纳博替尼 200mg BID 加曲美替尼 1mg QD 和纳博替尼 400mg BID 加曲美替尼 0.5mg QD。最常见的≥3 级治疗相关不良事件是纳博替尼加瑞替替尼(7.9%[101 例患者中的 8 例])的脂肪酶升高和纳博替尼加曲美替尼(19.1%[115 例患者中的 22 例])的皮疹。在 NSCLC 患者中,纳博替尼加瑞替替尼治疗的 3 名患者(1 名 KRAS 突变型,2 名 BRAF 突变型 NSCLC)和纳博替尼加曲美替尼治疗的 2 名患者(均为 KRAS 突变型 NSCLC)观察到部分缓解。纳博替尼加瑞替替尼或曲美替尼治疗时,DUSP6mRNA 水平从基线的中位降低分别为 45.5%和 76.1%。
结论
两种纳博替尼联合用药的安全性都可以接受。尽管观察到了针对靶点的药效学效应,但在 NSCLC 患者中抗肿瘤活性有限。
临床试验
gov 标识符:NCT02974725。
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