以USP47为靶点，通过控制c-Myc的去泛素化，增强KRAS抑制剂在KRASG12C突变的非小细胞肺癌中的疗效

IF 9.1 2区医学 Q1 PHARMACOLOGY & PHARMACY

Pharmacological research Pub Date : 2025-04-01 DOI:10.1016/j.phrs.2025.107722

Hyungkyung Shin , SuA Hwang , Jeong Hyun Jeong , Sang Chul Shin , Yeonji Oh , Jinhyeok Kim , Inah Hwang , Eunice EunKyeong Kim , Hyunah Choo , Eun Joo Song

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引用次数: 0

摘要

fda批准的KRASG12C抑制剂，如Sotorasib，靶向NSCLC中g12c突变的KRAS。然而，不敏感和耐药的问题已经出现，需要开发新的联合疗法来克服这些限制。USP47已被确定为癌症相关信号通路（如Wnt、Hippo和p53）的调节因子。然而，它在KRAS信号通路中的作用在很大程度上仍未被探索，并且USP47抑制剂的开发程度低于靶向其同源物USP7的抑制剂。在这里，我们发现USP47是krasg12c突变的NSCLC的一个新的治疗靶点，并报道了选择性USP47抑制剂K-552作为一种潜在的治疗策略。我们证明USP47通过去泛素化阻止其蛋白酶体降解来稳定c-Myc，从而促进非小细胞肺癌细胞增殖。此外，通过虚拟筛选鉴定的USP47抑制剂K-552有效地破坏c-Myc的稳定性并抑制krasg12c突变的NSCLC细胞增殖。此外，通过siRNA敲低或K-552处理抑制USP47，可以增强Sotorasib在体外和体内的疗效。总之，我们的研究结果确定了USP47是KRASG12C突变的NSCLC的一个有希望的治疗靶点，并介绍了K-552作为USP47抑制剂与KRASG12C抑制剂联合治疗的潜力。

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Targeting USP47 enhances the efficacy of KRAS inhibitor in KRASG12C mutated non-small cell lung cancer by controlling deubiquitination of c-Myc

FDA-approved KRAS^G12C inhibitors, like Sotorasib, target G12C-mutated KRAS in NSCLC. However, issues with insensitivity and drug resistance have emerged, requiring the development of new combination therapies to overcome these limitations. USP47 has been identified as a regulator of cancer-related signaling pathways such as Wnt, Hippo, and p53. However, its role in the KRAS signaling pathway remains largely unexplored and USP47 inhibitors are less developed than those targeting its homolog, USP7. Here, we identify USP47 as a novel therapeutic target in KRAS^G12C-mutated NSCLC and report K-552, a selective USP47 inhibitor, as a potential treatment strategy. We demonstrate that USP47 stabilizes c-Myc by preventing its proteasomal degradation through deubiquitination, thereby promoting NSCLC cell proliferation. Additionally, the compound K-552, a USP47 inhibitor identified through virtual screening, effectively destabilizes c-Myc and inhibits KRAS^G12C-mutated NSCLC cell proliferation. Furthermore, USP47 inhibition—either by siRNA knockdown or K-552 treatment—enhances the efficacy of Sotorasib in vitro and in vivo. Together, our findings establish USP47 as a promising therapeutic target in KRAS^G12C-mutated NSCLC and introduce K-552 as a USP47 inhibitor with potential for combination therapy with KRAS^G12C inhibitors.

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来源期刊

Pharmacological research 医学-药学

CiteScore

18.70

自引率

3.20%

发文量

491

审稿时长

8 days

期刊介绍： Pharmacological Research publishes cutting-edge articles in biomedical sciences to cover a broad range of topics that move the pharmacological field forward. Pharmacological research publishes articles on molecular, biochemical, translational, and clinical research (including clinical trials); it is proud of its rapid publication of accepted papers that comprises a dedicated, fast acceptance and publication track for high profile articles.