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MYC and Twist1 cooperate to drive metastasis by eliciting crosstalk between cancer and innate immunity.

Renumathy DhanasekaranVirginie BaylotMinsoon KimSibu KuruvillaDavid I BellovinNia AdenijiAnand Rajan KdIan LaiMeital GabayLing TongMaya KrishnanJangho ParkTheodore HuMustafa A BarbhuiyaAndrew J GentlesKasthuri KannanPhuoc T TranDean W Felsher
Published in: eLife (2020)
Metastasis is a major cause of cancer mortality. We generated an autochthonous transgenic mouse model whereby conditional expression of MYC and Twist1 enables hepatocellular carcinoma (HCC) to metastasize in >90% of mice. MYC and Twist1 cooperate and their sustained expression is required to elicit a transcriptional program associated with the activation of innate immunity, through secretion of a cytokinome that elicits recruitment and polarization of tumor associated macrophages (TAMs). Systemic treatment with Ccl2 and Il13 induced MYC-HCCs to metastasize; whereas, blockade of Ccl2 and Il13 abrogated MYC/Twist1-HCC metastasis. Further, in 33 human cancers (n = 9502) MYC and TWIST1 predict poor survival (p=4.3×10-10), CCL2/IL13 expression (p<10-109) and TAM infiltration (p<10-96). Finally, in the plasma of patients with HCC (n = 25) but not cirrhosis (n = 10), CCL2 and IL13 were increased and IL13 predicted invasive tumors. Therefore, MYC and TWIST1 generally appear to cooperate in human cancer to elicit a cytokinome that enables metastasis through crosstalk between cancer and immune microenvironment.
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