Neuroblastoma is composed of two super-enhancer-associated differentiation states

增强子 生物 表观遗传学 间充质干细胞 神经母细胞瘤 细胞分化 转录因子 电池类型 基因 遗传学 癌症研究 细胞生物学 细胞 细胞培养
作者
Tim van Groningen,Jan Köster,Linda J. Valentijn,Danny A. Zwijnenburg,Nurdan Akogul,Nancy E. Hasselt,Marloes E.C. Broekmans,Franciska Haneveld,Natalia E. Nowakowska,Johannes Bras,Carel J.M. van Noesel,Aldo Jongejan,Antoine H. C. van Kampen,Linda Köster,Frank Baas,Lianne van Dijk-Kerkhoven,Margriet Huizer-Smit,Maria C. Lecca,Alvin Chan,Arjan Lakeman,Piet Molenaar,Richard Volckmann,Ellen M. Westerhout,Mohamed Hamdi,Peter G. van Sluis,Marli E. Ebus,Jan J. Molenaar,Godelieve A.M. Tytgat,Bart A. Westerman,Johan van Nes,Rogier Versteeg
出处
期刊:Nature Genetics [Springer Nature]
卷期号:49 (8): 1261-1266 被引量:408
标识
DOI:10.1038/ng.3899
摘要

Neuroblastoma and other pediatric tumors show a paucity of gene mutations, which has sparked an interest in their epigenetic regulation. Several tumor types include phenotypically divergent cells, resembling cells from different lineage development stages. It has been proposed that super-enhancer-associated transcription factor (TF) networks underlie lineage identity, but the role of these enhancers in intratumoral heterogeneity is unknown. Here we show that most neuroblastomas include two types of tumor cells with divergent gene expression profiles. Undifferentiated mesenchymal cells and committed adrenergic cells can interconvert and resemble cells from different lineage differentiation stages. ChIP-seq analysis of isogenic pairs of mesenchymal and adrenergic cells identified a distinct super-enhancer landscape and super-enhancer-associated TF network for each cell type. Expression of the mesenchymal TF PRRX1 could reprogram the super-enhancer and mRNA landscapes of adrenergic cells toward a mesenchymal state. Mesenchymal cells were more chemoresistant in vitro and were enriched in post-therapy and relapse tumors. Two super-enhancer-associated TF networks, which probably mediate lineage control in normal development, thus dominate epigenetic control of neuroblastoma and shape intratumoral heterogeneity.
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