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MDM2拮抗剂与靶向基本致癌信号通路的化合物广泛且强烈地协同作用。

MDM2 antagonists synergize broadly and robustly with compounds targeting fundamental oncogenic signaling pathways.

作者信息

Saiki Anne Y, Caenepeel Sean, Yu Dongyin, Lofgren Julie A, Osgood Tao, Robertson Rebecca, Canon Jude, Su Cheng, Jones Adrie, Zhao Xiaoning, Deshpande Chetan, Payton Marc, Ledell Jebediah, Hughes Paul E, Oliner Jonathan D

机构信息

Department of Oncology Research, Amgen, Thousand Oaks, CA.

出版信息

Oncotarget. 2014 Apr 30;5(8):2030-43. doi: 10.18632/oncotarget.1918.

Abstract

While MDM2 inhibitors hold great promise as cancer therapeutics, drug resistance will likely limit their efficacy as single agents. To identify drug combinations that might circumvent resistance, we screened for agents that could synergize with MDM2 inhibition in the suppression of cell viability. We observed broad and robust synergy when combining MDM2 antagonists with either MEK or PI3K inhibitors. Synergy was not limited to cell lines harboring MAPK or PI3K pathway mutations, nor did it depend on which node of the PI3K axis was targeted. MDM2 inhibitors also synergized strongly with BH3 mimetics, BCR-ABL antagonists, and HDAC inhibitors. MDM2 inhibitor-mediated synergy with agents targeting these mechanisms was much more prevalent than previously appreciated, implying that clinical translation of these combinations could have far-reaching implications for public health. These findings highlight the importance of combinatorial drug targeting and provide a framework for the rational design of MDM2 inhibitor clinical trials.

摘要

虽然MDM2抑制剂作为癌症治疗药物具有很大的前景,但耐药性可能会限制其作为单一药物的疗效。为了确定可能规避耐药性的药物组合,我们筛选了能够在抑制细胞活力方面与MDM2抑制协同作用的药物。当将MDM2拮抗剂与MEK或PI3K抑制剂联合使用时,我们观察到广泛而强大的协同作用。协同作用不仅限于携带MAPK或PI3K途径突变的细胞系,也不取决于PI3K轴的哪个节点被靶向。MDM2抑制剂还与BH3模拟物、BCR-ABL拮抗剂和HDAC抑制剂强烈协同。MDM2抑制剂与靶向这些机制的药物介导的协同作用比以前认识到的更为普遍,这意味着这些组合的临床转化可能对公共卫生产生深远影响。这些发现突出了联合药物靶向的重要性,并为MDM2抑制剂临床试验的合理设计提供了框架。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3465/4039142/62643cbf98bf/oncotarget-05-2030-g001.jpg

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