Lung cancer deficient in the tumor suppressor GATA4 is sensitive to TGFBR1 inhibition.
Lei GaoYong HuYahui TianZhenzhen FanKun WangHongdan LiQian ZhouGuandi ZengXin HuLei YuShiyu ZhouXinyuan TongHsinyi HuangHaiquan ChenQing-Song LiuWanting LiuGong ZhangMu-Sheng ZengGuang-Biao ZhouQing-Yu HeHongbin JiLiang ChenPublished in: Nature communications (2019)
Lung cancer is the leading cause of cancer-related deaths worldwide. Tumor suppressor genes remain to be systemically identified for lung cancer. Through the genome-wide screening of tumor-suppressive transcription factors, we demonstrate here that GATA4 functions as an essential tumor suppressor in lung cancer in vitro and in vivo. Ectopic GATA4 expression results in lung cancer cell senescence. Mechanistically, GATA4 upregulates multiple miRNAs targeting TGFB2 mRNA and causes ensuing WNT7B downregulation and eventually triggers cell senescence. Decreased GATA4 level in clinical specimens negatively correlates with WNT7B or TGF-β2 level and is significantly associated with poor prognosis. TGFBR1 inhibitors show synergy with existing therapeutics in treating GATA4-deficient lung cancers in genetically engineered mouse model as well as patient-derived xenograft (PDX) mouse models. Collectively, our work demonstrates that GATA4 functions as a tumor suppressor in lung cancer and targeting the TGF-β signaling provides a potential way for the treatment of GATA4-deficient lung cancer.
Keyphrases
- transcription factor
- poor prognosis
- mouse model
- genome wide
- long non coding rna
- stem cells
- dna binding
- cell proliferation
- genome wide identification
- transforming growth factor
- dna damage
- small molecule
- endothelial cells
- cancer therapy
- dna methylation
- single cell
- risk assessment
- epithelial mesenchymal transition
- gene expression
- binding protein
- stress induced
- mesenchymal stem cells
- ultrasound guided
- wild type
- replacement therapy
- human health