作者
Bing Zhang, Jing Wang, Xiaojing Wang, Jing Zhu, Qi Liu, Zhiao Shi, Matthew C Chambers, Lisa J Zimmerman, Kent F Shaddox, Sangtae Kim, Sherri R Davies, Sean Wang, Pei Wang, Christopher R Kinsinger, Robert C Rivers, Henry Rodriguez, R Reid Townsend, Matthew JC Ellis, Steven A Carr, David L Tabb, Robert J Coffey, Robbert JC Slebos, Daniel C Liebler
发表日期
2014/9/18
期刊
Nature
卷号
513
期号
7518
页码范围
382-387
出版商
Nature Publishing Group UK
简介
Extensive genomic characterization of human cancers presents the problem of inference from genomic abnormalities to cancer phenotypes. To address this problem, we analysed proteomes of colon and rectal tumours characterized previously by The Cancer Genome Atlas (TCGA) and perform integrated proteogenomic analyses. Somatic variants displayed reduced protein abundance compared to germline variants. Messenger RNA transcript abundance did not reliably predict protein abundance differences between tumours. Proteomics identified five proteomic subtypes in the TCGA cohort, two of which overlapped with the TCGA ‘microsatellite instability/CpG island methylation phenotype’ transcriptomic subtype, but had distinct mutation, methylation and protein expression patterns associated with different clinical outcomes. Although copy number alterations showed strong cis- and trans-effects on mRNA …
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B Zhang, J Wang, X Wang, J Zhu, Q Liu, Z Shi… - Nature, 2014