尼洛替尼与舒尼替尼联用可使MCL-1降解并激活自噬,从而克服肾细胞癌对舒尼替尼的耐药性。

IF 4.9 2区 医学 Q2 CELL BIOLOGY
Cellular Oncology Pub Date : 2024-08-01 Epub Date: 2024-02-23 DOI:10.1007/s13402-024-00927-9
Tingyu Liu, Xin Yue, Xue Chen, Ru Yan, Chong Wu, Yunzhi Li, Xianzhang Bu, Hui Han, Ran-Yi Liu
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引用次数: 0

摘要

目的:舒尼替尼是治疗转移性肾细胞癌(RCC)的推荐药物。然而,舒尼替尼的治疗潜力受到毒性和耐药性的影响。因此,我们试图探索一种组合策略,以提高低毒性剂量舒尼替尼的疗效,从而更好地应用于临床:方法:我们通过体外细胞活力评估,从包含 1374 种美国 FDA 批准药物的化合物库中筛选舒尼替尼的协同试剂。方法:我们通过体外细胞活力评估,从包含 1374 种 FDA 批准药物的化合物库中筛选出舒尼替尼协同试剂,并在体外和体内模型中证实了其协同抗增殖和促凋亡作用。通过磷酸化蛋白质组学、共免疫沉淀、免疫荧光和 Western-blot 检测等方法对其分子机制进行了研究。结果:通过四步筛选,尼罗替尼脱颖而出,成为与舒尼替尼联用的潜在协同杀手。随后的功能评估表明,尼洛替尼与舒尼替尼在体外和体内能协同抑制 RCC 细胞增殖并促进细胞凋亡。从机理上讲,尼洛替尼激活E3连接酶HUWE1,与舒尼替尼联用可使MCL-1通过蛋白酶体途径降解,导致Beclin-1从MCL-1/Beclin-1复合物中释放。随后,Beclin-1诱导完整的自噬通路以促进抗肿瘤效果:我们的研究结果揭示了尼洛替尼联合舒尼替尼克服RCC舒尼替尼耐药的新机制。因此,这种新型合理的联合治疗方案为转移性RCC提供了一种前景广阔的治疗途径,也为在临床上评估这种联合治疗方案提供了依据。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Nilotinib in combination with sunitinib renders MCL-1 for degradation and activates autophagy that overcomes sunitinib resistance in renal cell carcinoma.

Nilotinib in combination with sunitinib renders MCL-1 for degradation and activates autophagy that overcomes sunitinib resistance in renal cell carcinoma.

Purpose: Sunitinib is a recommended drug for metastatic renal cell carcinoma (RCC). However, the therapeutic potential of sunitinib is impaired by toxicity and resistance. Therefore, we seek to explore a combinatorial strategy to improve sunitinib efficacy of low-toxicity dose for better clinical application.

Methods: We screen synergistic reagents of sunitinib from a compound library containing 1374 FDA-approved drugs by in vitro cell viability evaluation. The synergistically antiproliferative and proapoptotic effects were demonstrated on in vitro and in vivo models. The molecular mechanism was investigated by phosphoproteomics, co-immunoprecipitation, immunofluorescence and western-blot assays, etc. RESULTS: From the four-step screening, nilotinib stood out as a potential synergistic killer combined with sunitinib. Subsequent functional evaluation demonstrated that nilotinib and sunitinib synergistically inhibit RCC cell proliferation and promote apoptosis in vitro and in vivo. Mechanistically, nilotinib activates E3-ligase HUWE1 and in combination with sunitinib renders MCL-1 for degradation via proteasome pathway, resulting in the release of Beclin-1 from MCL-1/Beclin-1 complex. Subsequently, Beclin-1 induces complete autophagy flux to promote antitumor effect.

Conclusion: Our findings revealed that a novel mechanism that nilotinib in combination with sunitinib overcomes sunitinib resistance in RCC. Therefore, this novel rational combination regimen provides a promising therapeutic avenue for metastatic RCC and rationale for evaluating this combination clinically.

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来源期刊
Cellular Oncology
Cellular Oncology ONCOLOGY-CELL BIOLOGY
CiteScore
10.30
自引率
1.50%
发文量
86
审稿时长
12 months
期刊介绍: The Official Journal of the International Society for Cellular Oncology Focuses on translational research Addresses the conversion of cell biology to clinical applications Cellular Oncology publishes scientific contributions from various biomedical and clinical disciplines involved in basic and translational cancer research on the cell and tissue level, technical and bioinformatics developments in this area, and clinical applications. This includes a variety of fields like genome technology, micro-arrays and other high-throughput techniques, genomic instability, SNP, DNA methylation, signaling pathways, DNA organization, (sub)microscopic imaging, proteomics, bioinformatics, functional effects of genomics, drug design and development, molecular diagnostics and targeted cancer therapies, genotype-phenotype interactions. A major goal is to translate the latest developments in these fields from the research laboratory into routine patient management. To this end Cellular Oncology forms a platform of scientific information exchange between molecular biologists and geneticists, technical developers, pathologists, (medical) oncologists and other clinicians involved in the management of cancer patients. In vitro studies are preferentially supported by validations in tumor tissue with clinicopathological associations.
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