STAT3-mediated IGF-2 secretion in the tumour microenvironment elicits innate resistance to anti-IGF-1R antibody.
Ji-Sun LeeJu-Hee KangHye-Jin BooSu-Jung HwangSungyoul HongSu-Chan LeeYoung-Jun ParkTae-Moon ChungHyewon YounSeung Mi LeeByoung Jae KimJune-Key ChungYeonseok ChungWilliam N WilliamYoung Kee ShinHyo-Jong LeeSeung-Hyun OhHo-Young LeePublished in: Nature communications (2015)
Drug resistance is a major impediment in medical oncology. Recent studies have emphasized the importance of the tumour microenvironment (TME) to innate resistance, to molecularly targeted therapies. In this study, we investigate the role of TME in resistance to cixutumumab, an anti-IGF-1R monoclonal antibody that has shown limited clinical efficacy. We show that treatment with cixutumumab accelerates tumour infiltration of stromal cells and metastatic tumour growth, and decreases overall survival of mice. Cixutumumab treatment stimulates STAT3-dependent transcriptional upregulation of IGF-2 in cancer cells and recruitment of macrophages and fibroblasts via paracrine IGF-2/IGF-2R activation, resulting in the stroma-derived CXCL8 production, and thus angiogenic and metastatic environment. Silencing IGF-2 or STAT3 expression in cancer cells or IGF-2R or CXCL8 expression in stromal cells significantly inhibits the cancer-stroma communication and vascular endothelial cells' angiogenic activities. These findings suggest that blocking the STAT3/IGF-2/IGF-2R intercellular signalling loop may overcome the adverse consequences of anti-IGF-1R monoclonal antibody-based therapies.
Keyphrases
- binding protein
- pi k akt
- growth hormone
- monoclonal antibody
- cell proliferation
- poor prognosis
- immune response
- endothelial cells
- signaling pathway
- healthcare
- small cell lung cancer
- gene expression
- type diabetes
- transcription factor
- metabolic syndrome
- skeletal muscle
- lymph node metastasis
- combination therapy
- long non coding rna
- smoking cessation
- squamous cell