Whole-genome sequencing of acral melanoma reveals genomic complexity and diversity.

Felicity Newell,James S. Wilmott,Peter Johansson,Katia Nones,Venkateswar Addala,Pamela Mukhopadhyay,Natasa Broit,Carol M Amato,Robert Van Gulick,Stephen Kazakoff,Ann-Marie Patch,Lambros T. Koufariotis,Vanessa Lakis,Conrad Leonard,Scott Wood,Oliver Holmes,Qinying Xu,Karl D. Lewis,Theresa Medina,Rene Gonzalez,Robyn P. M. Saw,Andrew J. Spillane,Jonathan R. Stretch,Robert V. Rawson,Peter M. Ferguson,Tristan J. Dodds,John F. Thompson,Georgina V. Long,Mitchell P. Levesque,William A. Robinson,John V. Pearson,Graham J. Mann,Richard A. Scolyer,Nicola Waddell,Nicholas K. Hayward

Whole-genome sequencing of acral melanoma reveals genomic complexity and diversity.

2020

To increase understanding of the genomic landscape of acral melanoma, a rare form of melanoma occurring on palms, soles or nail beds, whole genome sequencing of 87 tumors with matching transcriptome sequencing for 63 tumors was performed. Here we report that mutational signature analysis reveals a subset of tumors, mostly subungual, with an ultraviolet radiation signature. Significantly mutated genes are BRAF, NRAS, NF1, NOTCH2, PTEN and TYRP1. Mutations and amplification of KIT are also common. Structural rearrangement and copy number signatures show that whole genome duplication, aneuploidy and complex rearrangements are common. Complex rearrangements occur recurrently and are associated with amplification of TERT, CDK4, MDM2, CCND1, PAK1 and GAB2, indicating potential therapeutic options.

Keywords:

TYRP1
Melanoma
Gene
PTEN
Biology
Genetics
Whole genome sequencing
Aneuploidy
Mdm2
Neuroblastoma RAS viral oncogene homolog

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