Yum, MK; Han, S; Fink, J; Wu, SHS; Dabrowska, C; Trendafilova, T; Mustata, R; ... Simons, BD; + view all Yum, MK; Han, S; Fink, J; Wu, SHS; Dabrowska, C; Trendafilova, T; Mustata, R; Chatzeli, L; Azzarelli, R; Pshenichnaya, I; Lee, E; England, F; Kim, JK; Stange, DE; Philpott, A; Lee, JH; Koo, BK; Simons, BD; - view fewer (2021) Tracing oncogene-driven remodelling of the intestinal stem cell niche. Nature , 594 (7863) pp. 442-447. 10.1038/s41586-021-03605-0.

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Abstract

Interactions between tumour cells and the surrounding microenvironment contribute to tumour progression, metastasis and recurrence1–3. Although mosaic analyses in Drosophila have advanced our understanding of such interactions4,5, it has been difficult to engineer parallel approaches in vertebrates. Here we present an oncogene-associated, multicolour reporter mouse model—the Red2Onco system—that allows differential tracing of mutant and wild-type cells in the same tissue. By applying this system to the small intestine, we show that oncogene-expressing mutant crypts alter the cellular organization of neighbouring wild-type crypts, thereby driving accelerated clonal drift. Crypts that express oncogenic KRAS or PI3K secrete BMP ligands that suppress local stem cell activity, while changes in PDGFRloCD81+ stromal cells induced by crypts with oncogenic PI3K alter the WNT signalling environment. Together, these results show how oncogene-driven paracrine remodelling creates a niche environment that is detrimental to the maintenance of wild-type tissue, promoting field transformation dominated by oncogenic clones.

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