Defining the landscape of circular RNAs in neuroblastoma unveils a global suppressive function of MYCN

Steffen Fuchs(Centre National de la Recherche Scientifique), Clara Danßmann(Charité - Universitätsmedizin Berlin), Filippos Klironomos(Charité - Universitätsmedizin Berlin), Annika Winkler(Charité - Universitätsmedizin Berlin), Jörg Fallmann(Telstra (Australia)), Louisa-Marie Kruetzfeldt(Charité - Universitätsmedizin Berlin), Annabell Szymansky(Charité - Universitätsmedizin Berlin), Julian Naderi(Max Planck Institute for Molecular Genetics), Stephan Wolf(Telstra (Australia)), Laura Grunewald(German Cancer Research Center), Konstantin Helmsauer(Max Delbrück Center), Elias Rodríguez-Fos(Max Delbrück Center), Marieluise Kirchner(Max Delbrück Center), Philipp Mertins(Max Delbrück Center), Kathy Astrahantseff(Charité - Universitätsmedizin Berlin), Christin Suenkel(Max Delbrück Center), Joern Toedling(German Cancer Research Center), Fabienne Meggetto(Centre National de la Recherche Scientifique), Marc Remke(Düsseldorf University Hospital), Peter F. Stadler(Telstra (Australia)), Patrick Hundsdoerfer(Helios Hospital Berlin-Buch), Hedwig E. Deubzer(German Cancer Research Center), Annette Künkele(German Cancer Research Center), Peter Lang(University Children's Hospital Tübingen), Jörg Fuchs(University Children's Hospital Tübingen), Anton G. Henssen(German Cancer Research Center), Angelika Eggert(German Cancer Research Center), Nikolaus Rajewsky(Max Delbrück Center), Falk Hertwig(German Cancer Research Center), Johannes H. Schulte(German Cancer Research Center)
Nature Communications
July 4, 2023
Cited by 19Open Access
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Abstract

Circular RNAs (circRNAs) are a regulatory RNA class. While cancer-driving functions have been identified for single circRNAs, how they modulate gene expression in cancer is not well understood. We investigate circRNA expression in the pediatric malignancy, neuroblastoma, through deep whole-transcriptome sequencing in 104 primary neuroblastomas covering all risk groups. We demonstrate that MYCN amplification, which defines a subset of high-risk cases, causes globally suppressed circRNA biogenesis directly dependent on the DHX9 RNA helicase. We detect similar mechanisms in shaping circRNA expression in the pediatric cancer medulloblastoma implying a general MYCN effect. Comparisons to other cancers identify 25 circRNAs that are specifically upregulated in neuroblastoma, including circARID1A. Transcribed from the ARID1A tumor suppressor gene, circARID1A promotes cell growth and survival, mediated by direct interaction with the KHSRP RNA-binding protein. Our study highlights the importance of MYCN regulating circRNAs in cancer and identifies molecular mechanisms, which explain their contribution to neuroblastoma pathogenesis.


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