Melanoma Genome Sequencing Reveals Frequent PREX2 Mutations

Overview

Journal Nature

Specialty Science

Date 2012 May 25

PMID 22622578

Citations 396

Authors

Michael F Berger

Eran Hodis

Timothy P Heffernan

Yonathan Lissanu Deribe

Michael S Lawrence

Alexei Protopopov

Elena Ivanova

Ian R Watson

Elizabeth Nickerson

Papia Ghosh

Hailei Zhang

Rhamy Zeid

Xiaojia Ren

Kristian Cibulskis

Andrey Y Sivachenko

Nikhil Wagle

Antje Sucker

Carrie Sougnez

Robert Onofrio

Lauren Ambrogio

Daniel Auclair

Timothy Fennell

Scott L Carter

Yotam Drier

Petar Stojanov

Meredith A Singer

Douglas Voet

Rui Jing

Gordon Saksena

Jordi Barretina

Alex H Ramos

Trevor J Pugh

Nicolas Stransky

Melissa Parkin

Wendy Winckler

Scott Mahan

Kristin Ardlie

Jennifer Baldwin

Jennifer Wargo

Dirk Schadendorf

Matthew Meyerson

Stacey B Gabriel

Todd R Golub

Stephan N Wagner

Eric S Lander

Gad Getz

Lynda Chin

Levi A Garraway

Affiliations

Soon will be listed here.

Abstract

Melanoma is notable for its metastatic propensity, lethality in the advanced setting and association with ultraviolet exposure early in life. To obtain a comprehensive genomic view of melanoma in humans, we sequenced the genomes of 25 metastatic melanomas and matched germline DNA. A wide range of point mutation rates was observed: lowest in melanomas whose primaries arose on non-ultraviolet-exposed hairless skin of the extremities (3 and 14 per megabase (Mb) of genome), intermediate in those originating from hair-bearing skin of the trunk (5-55 per Mb), and highest in a patient with a documented history of chronic sun exposure (111 per Mb). Analysis of whole-genome sequence data identified PREX2 (phosphatidylinositol-3,4,5-trisphosphate-dependent Rac exchange factor 2)--a PTEN-interacting protein and negative regulator of PTEN in breast cancer--as a significantly mutated gene with a mutation frequency of approximately 14% in an independent extension cohort of 107 human melanomas. PREX2 mutations are biologically relevant, as ectopic expression of mutant PREX2 accelerated tumour formation of immortalized human melanocytes in vivo. Thus, whole-genome sequencing of human melanoma tumours revealed genomic evidence of ultraviolet pathogenesis and discovered a new recurrently mutated gene in melanoma.

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