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Metastatic Group 3 Medulloblastoma is Driven by PRUNE1 Targeting NME1-TGF-β-OTX2-SNAIL Via PTEN Inhibition

Overview
Journal Brain
Publisher Oxford University Press
Specialty Neurology
Date 2018 Mar 1
PMID 29490009
Citations 18
Authors
Veronica Ferrucci
Pasqualino De Antonellis
Francesco Paolo Pennino
Fatemeh Asadzadeh
Antonella Virgilio
Donatella Montanaro
Aldo Galeone
Iolanda Boffa
Ida Pisano
Iolanda Scognamiglio
Luigi Navas
Donatella Diana
Emilia Pedone
Sara Gargiulo
Matteo Gramanzini
Arturo Brunetti
Laura Danielson
Marianeve Carotenuto
Lucia Liguori
Antonio Verrico
Lucia Quaglietta
Maria Elena Errico
Valentina Del Monaco
Valeria DArgenio
Felice Tirone
Angela Mastronuzzi
Vittoria Donofrio
Felice Giangaspero
Daniel Picard
Marc Remke
Livia Garzia
Craig Daniels
Olivier Delattre
Fredrik J Swartling
William A Weiss
Francesco Salvatore
Roberto Fattorusso
Louis Chesler
Michael D Taylor
Giuseppe Cinalli
Massimo Zollo
Affiliations
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Abstract

Genetic modifications during development of paediatric groups 3 and 4 medulloblastoma are responsible for their highly metastatic properties and poor patient survival rates. PRUNE1 is highly expressed in metastatic medulloblastoma group 3, which is characterized by TGF-β signalling activation, c-MYC amplification, and OTX2 expression. We describe the process of activation of the PRUNE1 signalling pathway that includes its binding to NME1, TGF-β activation, OTX2 upregulation, SNAIL (SNAI1) upregulation, and PTEN inhibition. The newly identified small molecule pyrimido-pyrimidine derivative AA7.1 enhances PRUNE1 degradation, inhibits this activation network, and augments PTEN expression. Both AA7.1 and a competitive permeable peptide that impairs PRUNE1/NME1 complex formation, impair tumour growth and metastatic dissemination in orthotopic xenograft models with a metastatic medulloblastoma group 3 cell line (D425-Med cells). Using whole exome sequencing technology in metastatic medulloblastoma primary tumour cells, we also define 23 common 'non-synonymous homozygous' deleterious gene variants as part of the protein molecular network of relevance for metastatic processes. This PRUNE1/TGF-β/OTX2/PTEN axis, together with the medulloblastoma-driver mutations, is of relevance for future rational and targeted therapies for metastatic medulloblastoma group 3.10.1093/brain/awy039_video1awy039media15742053534001.

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