Cellular hierarchies of embryonal tumors with multilayered rosettes are shaped by oncogenic microRNAs and receptor-ligand interactions.

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作者:Beck Alexander, Gabler-Pamer Lisa, Alencastro Veiga Cruzeiro Gustavo, Lambo Sander, Englinger Bernhard, Shaw McKenzie L, Hack Olivia A, Liu Ilon, Haase Rebecca D, de Biagi Carlos A O Jr, Baumgartner Alicia, Nascimento Silva Andrezza Do, Klenner Marbod, Freidel Pia S, Herms Jochen, von Baumgarten Louisa, Tonn Joerg C, Thon Niklas, Bruckner Katharina, Madlener Sibylle, Mayr Lisa, Senfter Daniel, Peyrl Andreas, Slavc Irene, Lötsch Daniela, Dorfer Christian, Geyregger Rene, Amberg Nicole, Haberler Christine, Mack Norman, Schwalm Benjamin, Pfister Stefan M, Korshunov Andrey, Baird Lissa C, Yang Edward, Chi Susan N, Alexandrescu Sanda, Gojo Johannes, Kool Marcel, Hovestadt Volker, Filbin Mariella G
Embryonal tumor with multilayered rosettes (ETMR) is a pediatric brain tumor with dismal prognosis. Characteristic alterations of the chromosome 19 microRNA cluster (C19MC) are observed in most ETMR; however, the ramifications of C19MC activation and the complex cellular architecture of ETMR remain understudied. Here we analyze 11 ETMR samples from patients using single-cell transcriptomics and multiplexed spatial imaging. We reveal a spatially distinct cellular hierarchy that spans highly proliferative neural stem-like cells and more differentiated neuron-like cells. C19MC is predominantly expressed in stem-like cells and controls a transcriptional network governing stemness and lineage commitment, as resolved by genome-wide analysis of microRNA-mRNA binding. Systematic analysis of receptor-ligand interactions between malignant cell types reveals fibroblast growth factor receptor and Notch signaling as oncogenic pathways that can be successfully targeted in preclinical models and in one patient with ETMR. Our study provides fundamental insights into ETMR pathobiology and a powerful rationale for more effective targeted therapies.

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