Combination of arsenic trioxide and apatinib synergistically inhibits small cell lung cancer by down-regulating VEGFR2/mTOR and Akt/c-Myc signaling pathway via GRB10.

IF 2.7 3区 生物学
Yao Yu, Yu Shang, Si Shi, Yaowu He, Wenchao Shi, Menghan Wang, Qi Wang, Dandan Xu, Ce Shi, Hong Chen
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引用次数: 0

Abstract

Background: Small cell lung carcinoma (SCLC) is characterized by -poor prognosis, -high predilection for -metastasis, -proliferation, and -absence of newer therapeutic options. Elucidation of newer pathways characterizing the disease may allow for development of targeted therapies and consequently favorable outcomes.

Methods: The current study explored the combinatorial action of arsenic trioxide (ATO) and apatinib (APA) in vitro and in vivo. In vitro models were tested using -H446 and -H196 SCLC cell lines. The ability of drugs to reduce -metastasis, -cell proliferation, and -migration were assessed. Using bioinformatic analysis, differentially expressed genes were determined. Gene regulation was assessed using gene knock down models and confirmed using Western blots. The in vivo models were used to confirm the resolution of pathognomic features in the presence of the drugs. Growth factor receptor bound protein (GRB) 10 expression levels of human small cell lung cancer tissues and adjacent tissues were detected by IHC.

Results: In combination, ATO and APA were found to significantly reduce -cell proliferation, -migration, and -metastasis in both the cell lines. Cell proliferation was found to be inhibited by activation of Caspase-3, -7 pathway. In the presence of drugs, it was found that expression of GRB10 was stabilized. The silencing of GRB10 was found to negatively regulate the VEGFR2/Akt/mTOR and Akt/GSK-3β/c-Myc signaling pathway. Concurrently, absence of metastasis and reduction of tumor volume were confirmed in vivo. The immunohistochemical results confirmed that the expression level of GRB10 in adjacent tissues was significantly higher than that in human small cell lung cancer tissues.

Conclusions: Synergistically, ATO and APA have a more significant impact on inhibiting cell proliferation than each drug independently. ATO and APA may be mediating its action through the stabilization of GRB10 thus acting as a tumor suppressor. We thus, preliminarily report the impact of GRB10 stability as a target for SCLC treatment.

三氧化二砷和阿帕替尼通过 GRB10 下调 VEGFR2/mTOR 和 Akt/c-Myc 信号通路,从而协同抑制小细胞肺癌。
背景:小细胞肺癌(SCLC)的特点是预后差、易转移、易扩散以及缺乏新的治疗方案。阐明该疾病的新通路可能有助于开发靶向疗法,从而获得良好的治疗效果:本研究探讨了三氧化二砷(ATO)和阿帕替尼(APA)在体外和体内的联合作用。体外模型使用-H446和-H196 SCLC细胞系进行测试。评估了药物减少转移、细胞增殖和迁移的能力。通过生物信息学分析,确定了差异表达基因。使用基因敲除模型评估基因调控,并使用 Western 印迹进行确认。体内模型用于确认药物存在时病理特征的解析。通过 IHC 检测人小细胞肺癌组织和邻近组织的生长因子受体结合蛋白(GRB)10 表达水平:结果:发现 ATO 和 APA 联合使用可显著减少两种细胞系的细胞增殖、迁移和转移。通过激活 Caspase-3、-7 通路,细胞增殖受到抑制。在药物存在的情况下,发现 GRB10 的表达趋于稳定。研究发现,沉默 GRB10 可负向调节 VEGFR2/Akt/mTOR 和 Akt/GSK-3β/c-Myc 信号通路。同时,在体内证实了无转移和肿瘤体积缩小。免疫组化结果证实,邻近组织中 GRB10 的表达水平明显高于人类小细胞肺癌组织:结论:ATO和APA协同抑制细胞增殖的效果比单独使用两种药物更明显。ATO和APA可能是通过稳定GRB10而发挥抑癌作用的。因此,我们初步报告了 GRB10 稳定性作为 SCLC 治疗靶点的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Hereditas
Hereditas Biochemistry, Genetics and Molecular Biology-Genetics
CiteScore
3.80
自引率
3.70%
发文量
0
期刊介绍: For almost a century, Hereditas has published original cutting-edge research and reviews. As the Official journal of the Mendelian Society of Lund, the journal welcomes research from across all areas of genetics and genomics. Topics of interest include human and medical genetics, animal and plant genetics, microbial genetics, agriculture and bioinformatics.
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