BRD4 modulates vulnerability of triple-negative breast cancer to targeting of integrin-dependent signaling pathways

被引:17
作者
Zhang, Yang [1 ,2 ,3 ]
Xu, Bingwei [1 ,2 ]
Shi, Junfeng [4 ]
Li, Jieming [1 ,2 ,5 ]
Lu, Xinlan [6 ]
Xu, Li [7 ]
Yang, Helen [1 ,2 ]
Hamad, Nevean [1 ,2 ]
Wang, Chi [1 ,2 ]
Napier, Dana [1 ,2 ]
He, Shuixiang [6 ]
Liu, Chunming [1 ,2 ]
Liu, Zeyi [3 ]
Qian, Hai [5 ]
Chen, Li [1 ,2 ]
Wei, Xiaowei [4 ]
Zheng, Xucai [8 ,9 ]
Huang, Jian-An [3 ]
Thibault, Olivier [1 ,2 ]
Craven, Rolf [1 ,2 ]
Wei, Dongping [4 ]
Pan, Yueyin [8 ,9 ]
Zhou, Binhua P. [1 ,2 ]
Wu, Yadi [1 ,2 ]
Yang, Xiuwei H. [1 ,2 ]
机构
[1] Univ Kentucky, Dept Mol & Cellular Biochem, Dept Pharmacol & Nutr Sci, Lexington, KY 40506 USA
[2] Univ Kentucky, Coll Med, Markey Canc Ctr, Lexington, KY 40506 USA
[3] Soochow Univ, Affiliated Hosp 1, Dept Resp Med, Suzhou, Jiangsu, Peoples R China
[4] Nanjing Med Univ, Dept Oncol, Nanjing, Jiangsu, Peoples R China
[5] China Pharmaceut Univ, Ctr Drug Discovery, Nanjing, Jiangsu, Peoples R China
[6] Xi An Jiao Tong Univ, Affiliated Hosp 1, Dept Med Oncol, Xian, Shaanxi, Peoples R China
[7] Univ Kentucky, Dept Stat, Lexington, KY USA
[8] Univ Sci & Technol China, Affiliated Hosp 1, Hefei, Anhui, Peoples R China
[9] Prov Hosp, Hefei, Anhui, Peoples R China
来源
CELLULAR ONCOLOGY | 2020年 / 43卷 / 06期
关键词
Triple-negative breast cancer; Integrin; BRD4; FAK; Targeted therapy; c-Myc; FOCAL ADHESION KINASE; COMPREHENSIVE MOLECULAR PORTRAITS; FAK INHIBITOR; C-MYC; MAMMARY TUMORIGENESIS; TUMOR-GROWTH; CELL-LINES; STEM-CELLS; PROLIFERATION; AMPLIFICATION;
D O I
10.1007/s13402-020-00537-1
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Purpose Stemming from a myriad of genetic and epigenetic alterations, triple-negative breast cancer (TNBC) is tied to poor clinical outcomes and aspires for individualized therapies. Here we investigated the therapeutic potential of co-inhibiting integrin-dependent signaling pathway and BRD4, a transcriptional and epigenetic mediator, for TNBC. Methods Two independent patient cohorts were subjected to bioinformatic and IHC examination for clinical association of candidate cancer drivers. The efficacy and biological bases for co-targeting these drivers were interrogated using cancer cell lines, a protein kinase array, chemical inhibitors, RNAi/CRISPR/Cas9 approaches, and a 4 T1-Balb/c xenograft model. Results We found that amplification of the chromosome 8q24 region occurred in nearly 20% of TNBC tumors, and that it coincided with co-upregulation or amplification of c-Myc and FAK, a key effector of integrin-dependent signaling. This co-upregulation at the mRNA or protein level correlated with a poor patient survival (p < 0.0109 orp < 0.0402, respectively). Furthermore, we found that 14 TNBC cell lines exhibited high vulnerabilities to the combination of JQ1 and VS-6063, potent pharmacological antagonists of the BRD4/c-Myc and integrin/FAK-dependent pathways, respectively. We also observed a cooperative inhibitory effect of JQ1 and VS-6063 on tumor growth and infiltration of Ly6G(+)myeloid-derived suppressor cells in vivo. Finally, we found that JQ1 and VS-6063 cooperatively induced apoptotic cell death by altering XIAP, Bcl2/Bcl-xl and Bim levels, impairing c-Src/p130Cas-, PI3K/Akt- and RelA-associated signaling, and were linked to EMT-inducing transcription factor Snail- and Slug-dependent regulation. Conclusion Based on our results, we conclude that the BRD4/c-Myc- and integrin/FAK-dependent pathways act in concert to promote breast cancer cell survival and poor clinical outcomes. As such, they represent promising targets for a synthetic lethal-type of therapy against TNBC.
引用
收藏
页码:1049 / 1066
页数:18
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