RNA sequencing of pancreatic circulating tumour cells implicates WNT signalling in metastasis |
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| Authors: | Min Yu David T Ting Shannon L Stott Ben S Wittner Fatih Ozsolak Suchismita Paul Jordan C Ciciliano Malgorzata E Smas Daniel Winokur Anna J Gilman Matthew J Ulman Kristina Xega Gianmarco Contino Brinda Alagesan Brian W Brannigan Patrice M Milos David P Ryan Lecia V Sequist Nabeel Bardeesy Sridhar Ramaswamy Mehmet Toner Shyamala Maheswaran Daniel A Haber |
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| Affiliation: | Massachusetts General Hospital Cancer Center, Harvard Medical School, Boston, Massachusetts 02114, USA. |
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| Abstract: | Circulating tumour cells (CTCs) shed into blood from primary cancers include putative precursors that initiate distal metastases. Although these cells are extraordinarily rare, they may identify cellular pathways contributing to the blood-borne dissemination of cancer. Here, we adapted a microfluidic device for efficient capture of CTCs from an endogenous mouse pancreatic cancer model and subjected CTCs to single-molecule RNA sequencing, identifying Wnt2 as a candidate gene enriched in CTCs. Expression of WNT2 in pancreatic cancer cells suppresses anoikis, enhances anchorage-independent sphere formation, and increases metastatic propensity in vivo. This effect is correlated with fibronectin upregulation and suppressed by inhibition of MAP3K7 (also known as TAK1) kinase. In humans, formation of non-adherent tumour spheres by pancreatic cancer cells is associated with upregulation of multiple WNT genes, and pancreatic CTCs revealed enrichment for WNT signalling in 5 out of 11 cases. Thus, molecular analysis of CTCs may identify candidate therapeutic targets to prevent the distal spread of cancer. |
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