Multi-omics analysis defines core genomic alterations in pheochromocytomas and paragangliomas

Luis Jaime Castro‐Vega; Éric Letouzé; Nelly Burnichon; Alexandre Buffet; Pierre-Hélie Disderot; Emmanuel Khalifa; Céline Loriot; Nabila Elarouci; Aurélie Morin; Mélanie Menara; Charlotte Lussey‐Lepoutre; Cécile Badoual; Mathilde Sibony; B. Dousset; Rossella Libé; Franck Zinzindohoué; P.-F. Plouin; Jérôme Bertherat; Laurence Amar; Aurélien de Reyniès; Judith Favier; Anne‐Paule Gimenez‐Roqueplo

doi:10.1038/ncomms7044

Multi-omics analysis defines core genomic alterations in pheochromocytomas and paragangliomas

Luis Jaime Castro‐Vega(Délégation Paris 5), Éric Letouzé(La Ligue Contre le Cancer), Nelly Burnichon(Délégation Paris 5), Alexandre Buffet(Délégation Paris 5), Pierre-Hélie Disderot(Délégation Paris 5), Emmanuel Khalifa(Délégation Paris 5), Céline Loriot(Délégation Paris 5), Nabila Elarouci(La Ligue Contre le Cancer), Aurélie Morin(Délégation Paris 5), Mélanie Menara(Délégation Paris 5), Charlotte Lussey‐Lepoutre(Délégation Paris 5), Cécile Badoual(Délégation Paris 5), Mathilde Sibony(Délégation Paris 5), B. Dousset(Délégation Paris 5), Rossella Libé(Délégation Paris 5), Franck Zinzindohoué(Délégation Paris 5), P.-F. Plouin(Délégation Paris 5), Jérôme Bertherat(Délégation Paris 5), Laurence Amar(Délégation Paris 5), Aurélien de Reyniès(La Ligue Contre le Cancer), Judith Favier(Délégation Paris 5), Anne‐Paule Gimenez‐Roqueplo(Délégation Paris 5)

Nature Communications

January 27, 2015

10.1038/ncomms7044

Cited by 188Open Access

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Abstract

Pheochromocytomas and paragangliomas (PCCs/PGLs) are neural crest-derived tumours with a very strong genetic component. Here we report the first integrated genomic examination of a large collection of PCC/PGL. SNP array analysis reveals distinct copy-number patterns associated with genetic background. Whole-exome sequencing shows a low mutation rate of 0.3 mutations per megabase, with few recurrent somatic mutations in genes not previously associated with PCC/PGL. DNA methylation arrays and miRNA sequencing identify DNA methylation changes and miRNA expression clusters strongly associated with messenger RNA expression profiling. Overexpression of the miRNA cluster 182/96/183 is specific in SDHB-mutated tumours and induces malignant traits, whereas silencing of the imprinted DLK1-MEG3 miRNA cluster appears as a potential driver in a subgroup of sporadic tumours. Altogether, the complete genomic landscape of PCC/PGL is mainly driven by distinct germline and/or somatic mutations in susceptibility genes and reveals different molecular entities, characterized by a set of unique genomic alterations.

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