| Literature DB >> 27974212 |
Anna Segerman1, Mia Niklasson2, Caroline Haglund3, Tobias Bergström2, Malin Jarvius3, Yuan Xie2, Ann Westermark2, Demet Sönmez2, Annika Hermansson2, Marianne Kastemar2, Zeinab Naimaie-Ali2, Frida Nyberg3, Malin Berglund3, Magnus Sundström2, Göran Hesselager4, Lene Uhrbom2, Mats Gustafsson3, Rolf Larsson3, Mårten Fryknäs3, Bo Segerman5, Bengt Westermark6.
Abstract
Intratumoral heterogeneity is a hallmark of glioblastoma multiforme and thought to negatively affect treatment efficacy. Here, we establish libraries of glioma-initiating cell (GIC) clones from patient samples and find extensive molecular and phenotypic variability among clones, including a range of responses to radiation and drugs. This widespread variability was observed as a continuum of multitherapy resistance phenotypes linked to a proneural-mesenchymal shift in the transcriptome. Multitherapy resistance was associated with a semi-stable cell state that was characterized by an altered DNA methylation pattern at promoter regions of mesenchymal master regulators and enhancers. The gradient of cell states within the GIC compartment constitutes a distinct form of heterogeneity. Our findings may open an avenue toward the development of new therapeutic rationales designed to reverse resistant cell states.Entities:
Keywords: clones; drug; glioma; heterogeneity; intratumoral; mesenchymal; proneural; radiation; resistant; transition
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Year: 2016 PMID: 27974212 DOI: 10.1016/j.celrep.2016.11.056
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423