| Literature DB >> 27479119 |
Barbara C Worst1, Cornelis M van Tilburg2, Gnana Prakash Balasubramanian3, Petra Fiesel4, Ruth Witt5, Angelika Freitag6, Miream Boudalil7, Christopher Previti8, Stephan Wolf9, Sabine Schmidt10, Sasithorn Chotewutmontri11, Melanie Bewerunge-Hudler12, Matthias Schick13, Matthias Schlesner14, Barbara Hutter15, Lenka Taylor16, Tobias Borst17, Christian Sutter18, Claus R Bartram19, Till Milde20, Elke Pfaff21, Andreas E Kulozik22, Arend von Stackelberg23, Roland Meisel24, Arndt Borkhardt25, Dirk Reinhardt26, Jan-Henning Klusmann27, Gudrun Fleischhack28, Stephan Tippelt29, Uta Dirksen30, Heribert Jürgens31, Christof M Kramm32, Andre O von Bueren33, Frank Westermann34, Matthias Fischer35, Birgit Burkhardt36, Wilhelm Wößmann37, Michaela Nathrath38, Stefan S Bielack39, Michael C Frühwald40, Simone Fulda41, Thomas Klingebiel42, Ewa Koscielniak43, Matthias Schwab44, Roman Tremmel45, Pablo Hernáiz Driever46, Johannes H Schulte47, Benedikt Brors48, Andreas von Deimling49, Peter Lichter50, Angelika Eggert51, David Capper52, Stefan M Pfister53, David T W Jones54, Olaf Witt55.
Abstract
The 'Individualized Therapy for Relapsed Malignancies in Childhood' (INFORM) precision medicine study is a nationwide German program for children with high-risk relapsed/refractory malignancies, which aims to identify therapeutic targets on an individualised basis. In a pilot phase, reported here, we developed the logistical and analytical pipelines necessary for rapid and comprehensive molecular profiling in a clinical setting. Fifty-seven patients from 20 centers were prospectively recruited. Malignancies investigated included sarcomas (n = 25), brain tumours (n = 23), and others (n = 9). Whole-exome, low-coverage whole-genome, and RNA sequencing were complemented with methylation and expression microarray analyses. Alterations were assessed for potential targetability according to a customised prioritisation algorithm and subsequently discussed in an interdisciplinary molecular tumour board. Next-generation sequencing data were generated for 52 patients, with the full analysis possible in 46 of 52. Turnaround time from sample receipt until first report averaged 28 d. Twenty-six patients (50%) harbored a potentially druggable alteration with a prioritisation score of 'intermediate' or higher (level 4 of 7). Common targets included receptor tyrosine kinases, phosphoinositide 3-kinase-mammalian target of rapamycin pathway, mitogen-activated protein kinase pathway, and cell cycle control. Ten patients received a targeted therapy based on these findings, with responses observed in some previously treatment-refractory tumours. Comparative primary relapse analysis revealed substantial tumour evolution as well as one case of unsuspected secondary malignancy, highlighting the importance of re-biopsy at relapse. This study demonstrates the feasibility of comprehensive, real-time molecular profiling for high-risk paediatric cancer patients. This extended proof-of-concept, with examples of treatment consequences, expands upon previous personalised oncology endeavors, and presents a model with considerable interest and practical relevance in the burgeoning era of personalised medicine.Entities:
Keywords: Brain; Cancer; Deep sequencing; Molecular targeted therapy; Oncology; Paediatrics; Personalised medicine; Precision medicine; Sarcoma
Mesh:
Year: 2016 PMID: 27479119 DOI: 10.1016/j.ejca.2016.06.009
Source DB: PubMed Journal: Eur J Cancer ISSN: 0959-8049 Impact factor: 9.162