| Literature DB >> 30905762 |
Verena Körber1, Jing Yang2, Pankaj Barah3, Yonghe Wu4, Damian Stichel5, Zuguang Gu6, Michael Nai Chung Fletcher7, David Jones8, Bettina Hentschel9, Katrin Lamszus10, Jörg Christian Tonn11, Gabriele Schackert12, Michael Sabel13, Jörg Felsberg14, Angela Zacher14, Kerstin Kaulich14, Daniel Hübschmann3, Christel Herold-Mende15, Andreas von Deimling5, Michael Weller16, Bernhard Radlwimmer7, Matthias Schlesner17, Guido Reifenberger18, Thomas Höfer19, Peter Lichter20.
Abstract
We studied how intratumoral genetic heterogeneity shapes tumor growth and therapy response for isocitrate dehydrogenase (IDH)-wild-type glioblastoma, a rapidly regrowing tumor. We inferred the evolutionary trajectories of matched pairs of primary and relapsed tumors based on deep whole-genome-sequencing data. This analysis suggests both a distant origin of de novo glioblastoma, up to 7 years before diagnosis, and a common path of early tumorigenesis, with one or more of chromosome 7 gain, 9p loss, or 10 loss, at tumor initiation. TERT promoter mutations often occurred later as a prerequisite for rapid growth. In contrast to this common early path, relapsed tumors acquired no stereotypical pattern of mutations and typically regrew from oligoclonal origins, suggesting sparse selective pressure by therapeutic measures.Entities:
Keywords: cancer evolution; clonal dynamics; glioblastoma; selective advantage; tumor growth; tumor phylogenetics; tumor recurrence
Year: 2019 PMID: 30905762 DOI: 10.1016/j.ccell.2019.02.007
Source DB: PubMed Journal: Cancer Cell ISSN: 1535-6108 Impact factor: 31.743