A NOTCH feed-forward loop drives reprogramming from adrenergic to mesenchymal state in neuroblastoma

Tim van Groningen(Amsterdam University Medical Centers), Nurdan Akogul(Amsterdam University Medical Centers), Ellen M. Westerhout(Amsterdam University Medical Centers), Alvin Chan(Amsterdam University Medical Centers), Nancy E. Hasselt(Amsterdam University Medical Centers), Danny A. Zwijnenburg(Amsterdam University Medical Centers), Marloes E.C. Broekmans(Amsterdam University Medical Centers), Peter Stroeken(Amsterdam University Medical Centers), Franciska Haneveld(Amsterdam University Medical Centers), Gerrit K. Hooijer(Amsterdam University Medical Centers), C. Dilara Savci‐Heijink(Amsterdam University Medical Centers), Arjan Lakeman(Amsterdam University Medical Centers), Richard Volckmann(Amsterdam University Medical Centers), Peter van Sluis(Amsterdam University Medical Centers), Linda J. Valentijn(Amsterdam University Medical Centers), Jan Köster(Amsterdam University Medical Centers), Rogier Versteeg(Amsterdam University Medical Centers), Johan van Nes(Amsterdam University Medical Centers)
Nature Communications
April 4, 2019
Cited by 171Open Access
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Abstract

Transition between differentiation states in development occurs swift but the mechanisms leading to epigenetic and transcriptional reprogramming are poorly understood. The pediatric cancer neuroblastoma includes adrenergic (ADRN) and mesenchymal (MES) tumor cell types, which differ in phenotype, super-enhancers (SEs) and core regulatory circuitries. These cell types can spontaneously interconvert, but the mechanism remains largely unknown. Here, we unravel how a NOTCH3 intracellular domain reprogrammed the ADRN transcriptional landscape towards a MES state. A transcriptional feed-forward circuitry of NOTCH-family transcription factors amplifies the NOTCH signaling levels, explaining the swift transition between two semi-stable cellular states. This transition induces genome-wide remodeling of the H3K27ac landscape and a switch from ADRN SEs to MES SEs. Once established, the NOTCH feed-forward loop maintains the induced MES state. In vivo reprogramming of ADRN cells shows that MES and ADRN cells are equally oncogenic. Our results elucidate a swift transdifferentiation between two semi-stable epigenetic cellular states.


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