Mesenchymal Differentiation Mediated by NF-κB Promotes Radiation Resistance in Glioblastoma

Krishna Bhat ,Howard Colman,Siobhan Conroy,Aditya Raghunathan,Adriana Olar,Ravesanker Ezhilarasan,Lindsey Heathcock,Divya Raj,Lihong Long,Faith Hollingsworth,Khalida Wani,Ganesh Rao,Brian Vaillant,Joy Gumin,Nina Lelic,Yoshinori Kodama,Veerakumar Balasubramaniyan,Karlijn Hummelink,Kenneth Aldape,Kusum Joshi ,Wilfred F A Den Dunnen ,Erik P Sulman ,Lindsey D Goodman ,﻿Ichiro Nakano ,Johanna D James ,Amy B Heimberger ,Heidi S Phillips ,Frederick F Lang ,Christopher E Pelloski ,Shuzhen Wang ,Se Hoon Kim ,Daniel P Cahill ,Hendrikus Boddeke

doi:10.1016/j.ccr.2013.08.001

Abstract

Despite extensive study, few therapeutic targets have been identified for glioblastoma (GBM). Here weshow that patient-derived glioma sphere cultures (GSCs) that resemble either the proneural (PN) or mesenchymal (MES) transcriptomal subtypes differ significantly in their biological characteristics. Moreover, we found that a subset of the PN GSCs undergoes differentiation to a MES state in a TNF-α/NF-κB-dependent manner with an associated enrichment of CD44 subpopulations and radioresistant phenotypes. We present data to suggest that the tumor microenvironment cell types such as macrophages/microglia may play an integral role in this process. We further show that the MES signature, CD44 expression, and NF-κB activation correlate with poor radiation response and shorter survival in patients with GBM.

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