연구논문

세부과제번호 2014M3A9DSA01073598 단계 1단계 2차년도
세부과제명 IMPC 대사질환 표현형 마우스 오믹스 분석기반 구축 및 정보개발 공동 유/무 N
SCI여부 Y 게재년월 2015-11
논문제목 Proteogenomic study beyond chromosome 9: new Insight into expressed variant proteome and transcriptome in human lung adenocarcinoma tissues.
총저자명 Young-In Kim, Jongan Lee, Young-Jin Choi, Jawon Seo, Jisook Park, Soo-Youn Lee and Je-Yoel Cho
학술지명 J Proteome Res 게재권(호) 14(12)
저널구분 - 페이지수 5007-5016
참여연구원 - 연구책임자 조제열
과제기여도 50 PMID -
사사기관수 - IF (년도) 4.245(15)
제1저자 Yong-In Kim 교신저자 Je-Yeol Cho
공동저자 -
초록
This is a report of a human proteome project (HPP) related to chromosome 9 (Chr 9). To reveal missing proteins and undiscovered features in proteogenomes, both LC-MS/MS analysis and next-generation RNA sequencing (RNA-seq)-based identification and characterization were conducted on five pairs of lung adenocarcinoma tumors and adjacent nontumor tissues. Before our previous Chromosome-Centric Human Proteome Project (C-HPP) special issue, there were 170 remaining missing proteins on Chr 9 (neXtProt 2013.09.26 rel.); 133 remain at present (neXtProt 2015.04.28 rel.). In the proteomics study, we found two missing protein candidates that require follow-up work and one unrevealed protein across all chromosomes. RNA-seq analysis detected RNA expression for four nonsynonymous (NS) single nucleotide polymorphisms (SNPs) (in CDH17, HIST1H1T, SAPCD2, and ZNF695) and three synonymous SNPs (in CDH17, CST1, and HNF1A) in all five tumor tissues but not in any of the adjacent normal tissues. By constructing a cancer patient sample-specific protein database based on individual RNA-seq data and by searching the proteomics data from the same sample, we identified four missense mutations in four genes (LTF, HDLBP, TF, and HBD). Two of these mutations were found in tumor samples but not in paired normal tissues. In summary, our proteogenomic study of human primary lung tumor tissues detected additional and revealed novel missense mutations and synonymous SNP signatures, some of which are specific to lung cancers. Data from mass spectrometry have been deposited in the ProteomeXchange with the identifier PXD002523.
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