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Title
Proteogenomic Characterization of Human Early-Onset Gastric Cancer
Issued Date
2019-01
Citation
Mun, Dong-Gi. (2019-01). Proteogenomic Characterization of Human Early-Onset Gastric Cancer. Cancer Cell, 35(1), 111-124.e10. doi: 10.1016/j.ccell.2018.12.003
Type
Article
Author Keywords
cancer subtypescorrelation between mRNA and protein abundance changescorrelation between mutation and phosphorylationdiffuse gastric cancerproteogenomicssomatic nonsynonymous mutations
Keywords
MICROSATELLITE INSTABILITYMOLECULAR SUBTYPESSIGNALING PATHWAYDATABASE SEARCHACCURATE MASSIDENTIFICATIONMUTATIONSDISCOVERYGENEKINASE
ISSN
1535-6108
Abstract
We report proteogenomic analysis of diffuse gastric cancers (GCs) in young populations. Phosphoproteome data elucidated signaling pathways associated with somatic mutations based on mutation-phosphorylation correlations. Moreover, correlations between mRNA and protein abundances provided potential oncogenes and tumor suppressors associated with patient survival. Furthermore, integrated clustering of mRNA, protein, phosphorylation, and N-glycosylation data identified four subtypes of diffuse GCs. Distinguishing these subtypes was possible by proteomic data. Four subtypes were associated with proliferation, immune response, metabolism, and invasion, respectively; and associations of the subtypes with immune- and invasion-related pathways were identified mainly by phosphorylation and N-glycosylation data. Therefore, our proteogenomic analysis provides additional information beyond genomic analyses, which can improve understanding of cancer biology and patient stratification in diffuse GCs. © 2018 Elsevier Inc.Mun et al. perform proteogenomic analysis of diffuse gastric cancers (DGC) in a young population, identifying that correlations of mRNA-protein abundance associate with survival and defining four subtypes of DGC. The associations of some subtypes with related pathways are identified mainly by the proteomic data. © 2018 Elsevier Inc.
URI
http://hdl.handle.net/20.500.11750/9527
DOI
10.1016/j.ccell.2018.12.003
Publisher
Cell Press
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