Precise characterization of KRAS4b proteoforms in human colorectal cells and tumors reveals mutation/modification cross-talk

Ntai Ioanna; Fornelli Luca; DeHart Caroline J.Hutton Josiah E.Doubleday Peter F.LeDuc Richard D.van Nispen Alexandra J.Fellers Ryan T.Whiteley GordonBoja Emily S.Rodriguez HenryKelleher Neil L.

首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America. >Precise characterization of KRAS4b proteoforms in human colorectal cells and tumors reveals mutation/modification cross-talk

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Precise characterization of KRAS4b proteoforms in human colorectal cells and tumors reveals mutation/modification cross-talk

机译：Precise characterization of KRAS4b proteoforms in human colorectal cells and tumors reveals mutation/modification cross-talk

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Mutations of the KRAS gene are found in human cancers with high frequency and result in the constitutive activation of its protein products. This leads to aberrant regulation of downstream pathways, promoting cell survival, proliferation, and tumorigenesis that drive cancer progression and negatively affect treatment outcomes. Here, we describe a workflow that can detect and quantify mutation-specific consequences of KRAS biochemistry, namely linked changes in post-translational modifications (PTMs). We combined immunoaffinity enrichment with detection by top-down mass spectrometry to discover and quantify proteoforms with or without the Gly13Asp mutation (G13D) specifically in the KRAS4b isoform. The workflow was applied first to isogenic KRAS colorectal cancer (CRC) cell lines and then to patient CRC tumors with matching KRAS genotypes. In two cellular models, a direct link between the knockout of the mutant G13D allele and the complete nitrosylation of cysteine 118 of the remaining WT KRAS4b was observed. Analysis of tumor samples quantified the percentage of mutant KRAS4b actually present in cancer tissue and identified major differences in the levels of C-terminal carboxymethylation, a modification critical for membrane association. These data from CRC cells and human tumors suggest mechanisms of posttranslational regulation that are highly context-dependent and which lead to preferential production of specific KRAS4b proteoforms.

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《Proceedings of the National Academy of Sciences of the United States of America.》 |2018年第16期|4140-4145|共6页
作者
Ntai Ioanna; Fornelli Luca; DeHart Caroline J.Hutton Josiah E.Doubleday Peter F.LeDuc Richard D.van Nispen Alexandra J.Fellers Ryan T.Whiteley GordonBoja Emily S.Rodriguez HenryKelleher Neil L.;
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作者单位

Northwestern Univ, Dept Chem, Prote Ctr Excellence, 2145 Sheridan Rd, Evanston, IL 60208 USA;

Leidos Biomed Res Inc, Frederick Natl Lab Canc Res, Frederick, MD 21701 USA;

NCI, Off Canc Clin Prote Res, Bethesda, MD 20892 USA;

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收录信息美国《科学引文索引》(SCI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
原文格式 PDF
正文语种英语
中图分类自然科学总论;
关键词
RAS; KRAS; posttranslational modification; top-down proteomics; immunoprecipitation;

Precise characterization of KRAS4b proteoforms in human colorectal cells and tumors reveals mutation/modification cross-talk

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