在具有致癌酪氨酸激酶驱动因子和 MDM2 扩增的肺腺癌中联合使用 MDM2 和靶向激酶抑制剂可延长肿瘤控制时间

IF 5.3 2区医学 Q1 ONCOLOGY

JCO precision oncology Pub Date : 2024-09-01 DOI:10.1200/PO.24.00241

Arielle Elkrief, Igor Odintsov, Roger S Smith, Morana Vojnic, Takuo Hayashi, Inna Khodos, Vladimir Markov, Zebing Liu, Allan J W Lui, Jamie L Bloom, Michael D Offin, Charles M Rudin, Elisa de Stanchina, Gregory J Riely, Romel Somwar, Marc Ladanyi

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引用次数: 0

摘要

目的：MDM2 是 TP53 肿瘤抑制因子的负调控因子，一旦扩增就会致癌。MDM2扩增（MDM2amp）与TP53突变互斥，见于6%的肺腺癌（LUAD）患者，在受体酪氨酸激酶（RTK）驱动基因改变的亚群中有显著的富集。最近的研究表明，在具有 MDM2amp 和 RTK 驱动基因改变的患者衍生 LUAD 模型中，MDM2 和 MEK 抑制具有协同活性。然而，在LUAD中联合使用MDM2和RTK抑制剂的研究尚未开展：我们评估了在 LUAD 患者衍生模型中联合使用 MDM2 和 RTK 抑制剂的效果：结果：在具有MDM2amp的RET融合LUAD患者衍生模型中，使用米拉德米坦或AMG232联合赛帕替尼抑制MDM2，其体内肿瘤的长期控制效果明显优于单独使用其中一种药物。同样，在具有MDM2amp的表皮生长因子受体突变模型中，将米拉德米坦或AMG232与奥希替尼联合使用可获得长期的体内肿瘤控制效果，其效果明显优于单独使用其中一种药物：这些临床前体内数据为这种组合靶向治疗方法的进一步临床开发提供了依据。

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查看原文本刊更多论文

Combination of MDM2 and Targeted Kinase Inhibitors Results in Prolonged Tumor Control in Lung Adenocarcinomas With Oncogenic Tyrosine Kinase Drivers and MDM2 Amplification.

Purpose: MDM2, a negative regulator of the TP53 tumor suppressor, is oncogenic when amplified. MDM2 amplification (MDM2amp) is mutually exclusive with TP53 mutation and is seen in 6% of patients with lung adenocarcinoma (LUAD), with significant enrichment in subsets with receptor tyrosine kinase (RTK) driver alterations. Recent studies have shown synergistic activity of MDM2 and MEK inhibition in patient-derived LUAD models with MDM2amp and RTK driver alterations. However, the combination of MDM2 and RTK inhibitors in LUAD has not been studied.

Methods: We evaluated the combination of MDM2 and RTK inhibition in patient-derived models of LUAD.

Results: In a RET-fusion LUAD patient-derived model with MDM2amp, MDM2 inhibition with either milademetan or AMG232 combined with selpercatinib resulted in long-term in vivo tumor control markedly superior to either agent alone. Similarly, in an EGFR-mutated model with MDM2amp, combining either milademetan or AMG232 with osimertinib resulted in long-term in vivo tumor control, which was strikingly superior to either agent alone.

Conclusion: These preclinical in vivo data provide a rationale for further clinical development of this combinatorial targeted therapy approach.

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来源期刊

JCO precision oncology ONCOLOGY-

CiteScore

9.10

自引率

4.30%

发文量

363