SCI

11 October 2024

Mechanisms of Response and Tolerance to Active RAS Inhibition in KRAS-Mutant Non–Small Cell Lung Cancer

(Cancer Discovery, IF: 29.7)

  • Haniel A. Araujo, Ximo Pechuan-Jorge, Teng Zhou, Minh Truong Do, Xin Hu, Frank R. Rojas Alvarez, Maria E. Salvatierra, Heladio P. Ibarguen, Richard Lee, Rashi Raghulan, Harshit Shah, Mariela A. Moreno Ayala, Kevin Chen, Nataliya Tovbis Shifrin, Shuhong Wu, Luisa M. Solis Soto, Marcelo V. Negrao, Don L. Gibbons, David S. Hong, Jack A. Roth, John V. Heymach, Jianjun Zhang, Jingjing Jiang, Mallika Singh, Jacqueline A.M. Smith, Elsa Quintana, and Ferdinandos Skoulidis

  • CORRESPONDENCE TO: fskoulidis@mdanderson.org

Abstract 摘要

Resistance to inactive state-selective RASG12C inhibitors frequently entails accumulation of RASGTP, rendering effective inhibition of active RAS potentially desirable. Here, we evaluated the antitumor activity of the RAS(ON) multi selective tricomplex inhibitor RMC-7977 and dissected mechanisms of response and tolerance in KRASG12C-mutant non–small cell lung cancer (NSCLC). Broad-spectrum reversible RASGTP inhibition with or without concurrent covalent targeting of active RASG12C yielded superior and differentiated antitumor activity across diverse co-mutational KRASG12C-mutant NSCLC mouse models of primary or acquired RASG12C(ON) or RASG12C(OFF) inhibitor resistance. Interrogation of time-resolved single-cell transcriptional responses established an in vivo atlas of multimodal acute and chronic RAS pathway inhibition in the NSCLC ecosystem and uncovered a regenerative mucinous transcriptional program that supports long-term tumor cell persistence. In patients with advanced KRASG12C-mutant NSCLC, the presence of mucinous histologic features portended poor response to sotorasib or adagrasib. Our results have potential implications for personalized medicine and the development of rational RAS inhibitor-anchored therapeutic strategies.

对非活性状态选择性 RASG12C 抑制剂的耐药性通常会导致 RASGTP 的积累,从而可能需要有效抑制活性RAS。在此,我们评估了RAS(ON)多选择性三复合物抑制剂RMC-7977的抗肿瘤活性,并分析了其在 KRASG12C- 突变非小细胞肺癌(NSCLC)的反应和耐受机制。广谱可逆 RASGTP 抑制,同时或不同时共价靶向活性 RASG12C,在原发性或获得性 RASG12C(ON) 或 RASG12C(OFF) 抑制剂抗性的多种共突变 KRASG12C 突变NSCLC小鼠模型中产生了优异和分化的抗肿瘤活性。对时间分辨单细胞转录反应的研究中建立了NSCLC生态系统中多模式的急性和慢性RAS通路抑制的体内图谱,并揭示了支持肿瘤细胞长期存在的再生粘液转录程序。在晚期 KRASG12C 突变型非小细胞肺癌患者中,粘液组织学特征的存在预示着对Sotorasib或Adagrasib的反应不佳。我们的研究结果对个性化医疗和开发合理的RAS抑制剂锚定治疗策略具备有潜力的意义。

 

Significance 意义

Our work reveals robust and durable antitumor activity of the preclinical RAS(ON) multi-selective inhibitor RMC-7977 against difficult-to-treat subsets of KRASG12C-mutant NSCLC with primary or acquired RASG12C inhibitor resistance and identifies a conserved mucinous transcriptional state that supports RAS inhibitor tolerance.

我们的工作揭示了临床前RAS(ON)多选择性抑制剂RMC-7977对具有原发性或获得性RASG12C 抑制剂耐药性的难治 KRASG12C 突变NSCLC亚群的强大和持久的抗肿瘤活性,并鉴定了一种支持RAS抑制剂耐受的保守粘液转录状态。

 

AI全文解析
这篇文章主要探讨了KRAS突变非小细胞肺癌(NSCLC)对KRASG12C抑制剂的反应机制及耐受性,具体重点如下:

 

1. KRASG12C抑制剂的挑战:虽然KRASG12C抑制剂如sotorasib和adagrasib对KRASG12C突变的NSCLC患者有疗效,但疗效有限,许多患者表现出原发或获得性耐药性。耐药的出现主要由RAS/MAPK通路的反馈激活引起,并且还涉及其他基因如KEAP1、SMARCA4和CDKN2A的共突变。

 

2. 新型抑制剂RMC-7977:文章评估了一种新的多选择性RAS(ON)抑制剂RMC-7977,该抑制剂针对多种突变和野生型RAS蛋白,能够有效抑制KRASG12C突变肿瘤的生长。研究表明,RMC-7977单独或与选择性KRASG12C抑制剂RMC-4998联合使用,在小鼠模型中展示了优异的抗肿瘤效果,尤其在一些难治性和预后较差的KRASG12C突变亚型中效果显著。

 

3. 耐药机制的探索:文章进一步分析了RMC-7977在克服KRASG12C抑制剂耐药性方面的潜力。通过实验发现,肿瘤细胞会通过上调GTP结合的RAS蛋白来绕过KRASG12C抑制剂的抑制作用。RMC-7977可以有效抑制这种耐药肿瘤的生长。

 

4. 免疫微环境影响:RMC-7977的使用还重新塑造了肿瘤的免疫微环境,减少了免疫抑制细胞(如中性粒细胞和髓源性抑制细胞),并增加了效应T细胞和NK细胞的浸润,进一步促进了抗肿瘤免疫反应。

 

5. 长期耐药和持久细胞存活:研究发现,RMC-7977虽然能够显著抑制肿瘤,但肿瘤细胞可能会进入一种药物耐受的持久状态,这些细胞在治疗停止后仍能存活,并且表现出再生和增殖的能力。

 

总体而言,该研究为开发更有效的KRAS突变抑制策略提供了新的见解,尤其是对那些对传统KRASG12C抑制剂耐药的NSCLC患者。文章提出了联合疗法和更广泛的RAS抑制剂在克服耐药性和改善临床结局方面的潜力 。