ABCB1-dependent collateral sensitivity of multidrug-resistant colorectal cancer cells to the survivin inhibitor MX106-4C

IF 15.8 1区 医学 Q1 PHARMACOLOGY & PHARMACY
Zi-Ning Lei , Najah Albadari , Qiu-Xu Teng , Hadiar Rahman , Jing-Quan Wang , Zhongzhi Wu , Dejian Ma , Suresh V. Ambudkar , John N.D. Wurpel , Yihang Pan , Wei Li , Zhe-Sheng Chen
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引用次数: 0

Abstract

Aims

To investigate the collateral sensitivity (CS) of ABCB1-positive multidrug resistant (MDR) colorectal cancer cells to the survivin inhibitor MX106–4C and the mechanism.

Methods

Biochemical assays (MTT, ATPase, drug accumulation/efflux, Western blot, RT-qPCR, immunofluorescence, flow cytometry) and bioinformatic analyses (mRNA-sequencing, reversed-phase protein array) were performed to investigate the hypersensitivity of ABCB1 overexpressing colorectal cancer cells to MX106–4C and the mechanisms. Synergism assay, long-term selection, and 3D tumor spheroid test were used to evaluate the anti-cancer efficacy of MX106–4C.

Results

MX106–4C selectively killed ABCB1-positive colorectal cancer cells, which could be reversed by an ABCB1 inhibitor, knockout of ABCB1, or loss-of-function ABCB1 mutation, indicating an ABCB1 expression and function-dependent mechanism. MX106–4C's selective toxicity was associated with cell cycle arrest and apoptosis through ABCB1-dependent survivin inhibition and activation on caspases-3/7 as well as modulation on p21-CDK4/6-pRb pathway. MX106–4C had good selectivity against ABCB1-positive colorectal cancer cells and retained this in multicellular tumor spheroids. In addition, MX106–4C could exert a synergistic anti-cancer effect with doxorubicin or re-sensitize ABCB1-positive cancer cells to doxorubicin by reducing ABCB1 expression in the cell population via long-term exposure.

Conclusions

MX106–4C selectively kills ABCB1-positive MDR colorectal cancer cells via a novel ABCB1-dependent survivin inhibition mechanism, providing a clue for designing CS compound as an alternative strategy to overcome ABCB1-mediated colorectal cancer MDR.

耐多药结肠直肠癌细胞对存活素抑制剂 MX106-4C 的 ABCB1 依赖性附带敏感性
目的 研究ABCB1阳性多药耐药(MDR)结直肠癌细胞对存活素抑制剂MX106-4C的附带敏感性(CS)及其机制。方法通过生化检测(MTT、ATPase、药物蓄积/外流、Western印迹、RT-qPCR、免疫荧光、流式细胞术)和生物信息学分析(mRNA测序、反相蛋白质阵列)研究ABCB1过表达结直肠癌细胞对MX106-4C的超敏性及其机制。结果MX106-4C能选择性杀伤ABCB1阳性结直肠癌细胞,ABCB1抑制剂、ABCB1基因敲除或ABCB1功能缺失突变均能逆转其杀伤作用,表明MX106-4C具有ABCB1表达和功能依赖性机制。MX106-4C的选择性毒性与细胞周期停滞和细胞凋亡有关,它是通过依赖于ABCB1的survivin抑制和caspases-3/7激活以及p21-CDK4/6-pRb通路调节实现的。MX106-4C对ABCB1阳性结直肠癌细胞具有良好的选择性,并在多细胞肿瘤球中保持了这种选择性。此外,MX106-4C 还能与多柔比星发挥协同抗癌作用,或通过长期暴露降低细胞群中 ABCB1 的表达,使 ABCB1 阳性癌细胞对多柔比星重新敏感。
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来源期刊
Drug Resistance Updates
Drug Resistance Updates 医学-药学
CiteScore
26.20
自引率
11.90%
发文量
32
审稿时长
29 days
期刊介绍: Drug Resistance Updates serves as a platform for publishing original research, commentary, and expert reviews on significant advancements in drug resistance related to infectious diseases and cancer. It encompasses diverse disciplines such as molecular biology, biochemistry, cell biology, pharmacology, microbiology, preclinical therapeutics, oncology, and clinical medicine. The journal addresses both basic research and clinical aspects of drug resistance, providing insights into novel drugs and strategies to overcome resistance. Original research articles are welcomed, and review articles are authored by leaders in the field by invitation. Articles are written by leaders in the field, in response to an invitation from the Editors, and are peer-reviewed prior to publication. Articles are clear, readable, and up-to-date, suitable for a multidisciplinary readership and include schematic diagrams and other illustrations conveying the major points of the article. The goal is to highlight recent areas of growth and put them in perspective. *Expert reviews in clinical and basic drug resistance research in oncology and infectious disease *Describes emerging technologies and therapies, particularly those that overcome drug resistance *Emphasises common themes in microbial and cancer research
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