Biological and targeting differences between the rare KRAS A146T and canonical KRAS mutants in gastric cancer models.

IF 6 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY Gastric Cancer Pub Date : 2024-05-01 Epub Date: 2024-01-23 DOI:10.1007/s10120-024-01468-8
Elisabetta Puliga, Chiara De Bellis, Sandra Vietti Michelina, Tania Capeloa, Cristina Migliore, Claudia Orrù, Gian Luca Baiocchi, Giovanni De Manzoni, Filippo Pietrantonio, Rossella Reddavid, Uberto Fumagalli Romario, Chiara Ambrogio, Simona Corso, Silvia Giordano
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Abstract

Background: Gastric cancer (GC) is the third leading cause of cancer-related death worldwide, with a poor prognosis for patients with advanced disease. Since the oncogenic role of KRAS mutants has been poorly investigated in GC, this study aims to biochemically and biologically characterize different KRAS-mutated models and unravel differences among KRAS mutants in response to therapy.

Methods: Taking advantage of a proprietary, molecularly annotated platform of more than 200 GC PDXs (patient-derived xenografts), we identified KRAS-mutated PDXs, from which primary cell lines were established. The different mutants were challenged with KRAS downstream inhibitors in in vitro and in vivo experiments.

Results: Cells expressing the rare KRAS A146T mutant showed lower RAS-GTP levels compared to those bearing the canonical G12/13D mutations. Nevertheless, all the KRAS-mutated cells displayed KRAS addiction. Surprisingly, even if the GEF SOS1 is considered critical for the activation of KRAS A146T mutants, its abrogation did not significantly affect cell viability. From the pharmacologic point of view, Trametinib monotherapy was more effective in A146T than in G12D-mutated models, suggesting a vulnerability to MEK inhibition. However, in the presence of mutations in the PI3K pathway, more frequently co-occurrent in A146T models, the association of Trametinib and the AKT inhibitor MK-2206 was required to optimize the response.

Conclusion: A deeper genomic and biological characterization of KRAS mutants might sustain the development of more efficient and long-lasting therapeutic options for patients harbouring KRAS-driven GC.

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胃癌模型中罕见 KRAS A146T 突变体与典型 KRAS 突变体在生物学和靶向方面的差异。
背景:胃癌(GC)是全球癌症相关死亡的第三大原因,晚期患者预后较差。由于对 KRAS 突变体在胃癌中的致癌作用研究较少,本研究旨在从生物化学和生物学角度描述不同的 KRAS 突变模型,并揭示 KRAS 突变体对治疗反应的差异:我们利用一个由 200 多个 GC PDX(患者来源异种移植)组成的专有分子注释平台,确定了 KRAS 突变的 PDX,并从中建立了原代细胞系。在体外和体内实验中,我们用 KRAS 下游抑制剂对不同的突变体进行了挑战:结果:表达罕见的 KRAS A146T 突变体的细胞显示出较低的 RAS-GTP 水平。然而,所有 KRAS 突变细胞都显示出 KRAS 上瘾。令人惊讶的是,即使GEF SOS1被认为是激活KRAS A146T突变体的关键,但它的消减并没有显著影响细胞的活力。从药理学角度来看,曲美替尼单药治疗在 A146T 突变模型中比在 G12D 突变模型中更有效,这表明曲美替尼容易受到 MEK 抑制的影响。然而,如果存在PI3K通路的突变(在A146T模型中更常并发),则需要将曲美替尼与AKT抑制剂MK-2206联合使用,以优化疗效:结论:对 KRAS 突变体进行更深入的基因组学和生物学特征描述可能有助于为 KRAS 驱动的 GC 患者开发更有效、更持久的治疗方案。
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来源期刊
Gastric Cancer
Gastric Cancer 医学-胃肠肝病学
CiteScore
14.70
自引率
2.70%
发文量
80
审稿时长
6-12 weeks
期刊介绍: Gastric Cancer is an esteemed global forum that focuses on various aspects of gastric cancer research, treatment, and biology worldwide. The journal promotes a diverse range of content, including original articles, case reports, short communications, and technical notes. It also welcomes Letters to the Editor discussing published articles or sharing viewpoints on gastric cancer topics. Review articles are predominantly sought after by the Editor, ensuring comprehensive coverage of the field. With a dedicated and knowledgeable editorial team, the journal is committed to providing exceptional support and ensuring high levels of author satisfaction. In fact, over 90% of published authors have expressed their intent to publish again in our esteemed journal.
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