A Phase 1/1B Trial of Pembrolizumab and Trametinib in Advanced NSCLC Enriched for KRAS Mutations

IF 3 Q2 ONCOLOGY

JTO Clinical and Research Reports Pub Date : 2025-02-12 DOI:10.1016/j.jtocrr.2025.100806

Jonathan W. Riess MD, MS , Matthew S. Lara BS , Guillaume Luxardi PhD , Miguel Lopez de Rodas MD , Michiko Shimoda PhD , Karen Kelly MD , Primo N. Lara MD , Laurel Beckett PhD , Arta Monjazeb MD, PhD , Kurt A. Schalper MD, PhD , Emanual Maverakis MD , David R. Gandara MD

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Abstract

Introduction

MEK inhibition (MEKi) combined with programmed death ligand 1 inhibition (immune checkpoint inhibitor [ICI]) modulates the tumor immune microenvironment. This phase 1 study evaluated sequencing schemes of MEKi and ICI with trametinib and pembrolizumab in NSCLC.

Methods

In this 3+3 dose escalation study, patients with advanced NSCLC were treated with lead-in trametinib (arm A) or lead-in pembrolizumab (arm B) for cycle 1, followed by a 1.5 to 2 mg oral daily dose of trametinib (d 1–10) with pembrolizumab 200 mg intravenously every 21 days. Eligible patients with progressive disease on or after platinum-based chemotherapy were enrolled. Prior ICI was allowed. Tumor tissue was analyzed with quantitative immunofluorescence. High-parameter flow cytometry was performed on blood. Adverse events were graded using the Common Terminology Criteria for Adverse Events version 4 and efficacy was evaluated by Response Evaluation Criteria in Solid Tumors version 1.1.

Results

Fifteen patients enrolled (nine arm A and six arm B) with 13 (86%) harboring KRAS mutations and 10 (66%) receiving prior ICI. Five patients (33%) experienced at least one grade greater than or equal to 3 treatment-related adverse event including one dose-limiting toxicity (grade 3 esophagitis). Two patients had a partial response (ORR = 14%). Trametinib lead-in was associated with decreased T-regulatory cells and myeloid-derived suppressor cells (p = 0.002 and p = 0.05, respectively).

Conclusions

The activity of trametinib and pembrolizumab is modest in NSCLC with increased toxicity compared with programmed death ligand 1 blockade alone. The recommended phase 2 dose for the combination is 2 mg of oral trametinib (d 1–10) and 200 mg of intravenous pembrolizumab every 21 days, with lead-in trametinib. Adverse events were comparable with other MEKi and ICI combination studies. Though limited clinical activity was observed, lead-in MEKi may induce favorable immune cell alterations.

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Pembrolizumab和Trametinib治疗晚期NSCLC富集KRAS突变的1/1B期临床试验

mek抑制（MEKi）联合程序性死亡配体1抑制（免疫检查点抑制剂[ICI]）调节肿瘤免疫微环境。该i期研究评估了MEKi和ICI联合曲美替尼和派姆单抗治疗NSCLC的测序方案。方法在这项3+3剂量递增研究中，晚期NSCLC患者在第1周期内接受引入曲美替尼（A组）或引入派姆单抗（B组）治疗，随后每天口服1.5至2mg剂量的曲美替尼（d 1 - 10），每21天静脉注射200 mg派姆单抗。符合条件的进展性疾病患者接受或接受铂类化疗。事先ICI是允许的。用定量免疫荧光法分析肿瘤组织。对血液进行高参数流式细胞术检测。使用不良事件通用术语标准第4版对不良事件进行分级，根据实体瘤反应评价标准第1.1版对疗效进行评价。结果纳入的15例患者（9例A组和6例B组）中，13例（86%）携带KRAS突变，10例（66%）既往接受过ICI。5名患者（33%）经历了至少1级大于或等于3级的治疗相关不良事件，包括1级剂量限制性毒性（3级食管炎）。2例患者部分缓解（ORR = 14%）。引入曲美替尼与t调节性细胞和髓源性抑制细胞减少相关（p = 0.002和p = 0.05）。结论曲美替尼和派姆单抗在非小细胞肺癌中的活性是温和的，与单独的程序性死亡配体1阻断相比，毒性增加。推荐的2期联合用药剂量为口服曲美替尼2mg （d 1-10）和静脉注射派姆单抗200mg，每21天一次，引入曲美替尼。不良事件与其他MEKi和ICI联合研究相当。虽然观察到有限的临床活性，但引入MEKi可能诱导有利的免疫细胞改变。

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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