2014年1月6日月曜日

新春第一弾はMIT/Harvard連合軍のnature

Nature(2014) 

Received 12 September 2013
Accepted 27 November 2013 
Published online 05 January 2014  

Discovery and saturation analysis of cancer genes across 21 tumour types 

Michael S. Lawrence,Petar Stojanov,Craig H. Mermel,James T. Robinson, Levi A. Garraway, Todd R. Golub,Matthew Meyerson, Stacey B. Gabriel, Eric S. Lander and Gad Getz 

Abstract

Although a few cancer genes are mutated in a high proportion of tumours of a given type (>20%), most are mutated at intermediate frequencies (2–20%). To explore the feasibility of creating a comprehensive catalogue of cancer genes, we analysed somatic point mutations in exome sequences from 4,742 human cancers and their matched normal-tissue samples across 21 cancer types. We found that large-scale genomic analysis can identify nearly all known cancer genes in these tumour types. Our analysis also identified 33 genes that were not previously known to be significantly mutated in cancer, including genes related to proliferation, apoptosis, genome stability, chromatin regulation, immune evasion, RNA processing and protein homeostasis. Down-sampling analysis indicates that larger sample sizes will reveal many more genes mutated at clinically important frequencies. We estimate that near-saturation may be achieved with 600–5,000 samples per tumour type, depending on background mutation frequency. The results may help to guide the next stage of cancer genomics.

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