Targeting 17q23 amplicon to overcome the resistance to anti-HER2 therapy in HER2+ breast cancer.
Yunhua LiuJiangsheng XuHyun Ho ChoiCecil HanYuanzhang FangYujing LiKevin Van der JeughtHanchen XuLu ZhangMichael FriedenLifei WangHaniyeh EyvaniYifan SunGang ZhaoYuntian ZhangSheng LiuJun WanCheng HuangGuang JiXiongbin LuXiaoming HeXinna ZhangPublished in: Nature communications (2018)
Chromosome 17q23 amplification occurs in ~11% of human breast cancers. Enriched in HER2+ breast cancers, the 17q23 amplification is significantly correlated with poor clinical outcomes. In addition to the previously identified oncogene WIP1, we uncover an oncogenic microRNA gene, MIR21, in a majority of the WIP1-containing 17q23 amplicons. The 17q23 amplification results in aberrant expression of WIP1 and miR-21, which not only promotes breast tumorigenesis, but also leads to resistance to anti-HER2 therapies. Inhibiting WIP1 and miR-21 selectively inhibits the proliferation, survival and tumorigenic potential of the HER2+ breast cancer cells harboring 17q23 amplification. To overcome the resistance of trastuzumab-based therapies in vivo, we develop pH-sensitive nanoparticles for specific co-delivery of the WIP1 and miR-21 inhibitors into HER2+ breast tumors, leading to a profound reduction of tumor growth. These results demonstrate the great potential of the combined treatment of WIP1 and miR-21 inhibitors for the trastuzumab-resistant HER2+ breast cancers.
Keyphrases
- cell proliferation
- long non coding rna
- long noncoding rna
- poor prognosis
- nucleic acid
- signaling pathway
- stem cells
- epidermal growth factor receptor
- transcription factor
- climate change
- genome wide
- mesenchymal stem cells
- dna methylation
- intellectual disability
- autism spectrum disorder
- human health
- cell therapy
- metastatic breast cancer
- genome wide analysis
- breast cancer risk