Intratumoral genome diversity parallels progression and predicts outcome in pediatric cancer

Linda Holmquist Mengelbier(Lund University), Jenny Karlsson(Lund University), David Lindgren(Lund University), Anders Valind(Lund University), Henrik Lilljebjörn(Lund University), Caroline Jansson(Lund University), Daniel Bexell(Lund University), Noémie Braekeveldt(Medicon Village), Adam Ameur(Uppsala University), Tord Jonson(Lund University), Hanna Göransson Kultima(Uppsala University), Anders Isaksson(Uppsala University), Jurate Ásmundsson(Karolinska University Hospital), Rogier Versteeg(Academic Medical Center), Marianne Rissler(Lund University), Thoas Fioretos(Lund University), Bengt Sandstedt(Karolinska Institutet), Anna Börjesson(Lund University), Torbjörn Backman(Lund University), Niklas Pal(Karolinska University Hospital), Ingrid Øra(Lund University), Markus Mayrhofer(Uppsala University), David Gisselsson
Nature Communications
January 27, 2015
Cited by 75Open Access
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Abstract

Genetic differences among neoplastic cells within the same tumour have been proposed to drive cancer progression and treatment failure. Whether data on intratumoral diversity can be used to predict clinical outcome remains unclear. We here address this issue by quantifying genetic intratumoral diversity in a set of chemotherapy-treated childhood tumours. By analysis of multiple tumour samples from seven patients we demonstrate intratumoral diversity in all patients analysed after chemotherapy, typically presenting as multiple clones within a single millimetre-sized tumour sample (microdiversity). We show that microdiversity often acts as the foundation for further genome evolution in metastases. In addition, we find that microdiversity predicts poor cancer-specific survival (60%; P=0.009), independent of other risk factors, in a cohort of 44 patients with chemotherapy-treated childhood kidney cancer. Survival was 100% for patients lacking microdiversity. Thus, intratumoral genetic diversity is common in childhood cancers after chemotherapy and may be an important factor behind treatment failure.


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