Literature DB >> 21080693

Mass spectrometry mapping of epidermal growth factor receptor phosphorylation related to oncogenic mutations and tyrosine kinase inhibitor sensitivity.

Guolin Zhang1, Bin Fang, Richard Z Liu, Huiyi Lin, Fumi Kinose, Yun Bai, Umut Oguz, Elizabeth R Remily-Wood, Jiannong Li, Soner Altiok, Steven Eschrich, John Koomen, Eric B Haura.   

Abstract

The epidermal growth factor receptor (EGFR) plays an important role in cancer by activating downstream signals important in growth and survival. Inhibitors of EGFR are frequently selected as treatment for cancer including lung cancer. We performed an unbiased and comprehensive search for EGFR phosphorylation events related to somatic activating mutations and EGFR inhibitor (erlotinib) sensitivity. EGFR immunoprecipitation combined with high resolution liquid chromatography-mass spectrometry and label free quantitation characterized EGFR phosphorylation. Thirty (30) phosphorylation sites were identified including 12 tyrosine (pY), 12 serine (pS), and 6 threonine (pT). Site-specific phosphorylation was monitored by comparing ion signals from the corresponding unmodified peptide. Phosphorylation sites related to activating mutations in EGFR as well as sensitivity to erlotinib were identified using 31 lung cancer cell lines. We identified three sites (pY1092, pY1110, pY1172) correlated with activating mutations and three sites (pY1110, pY1172, pY1197) correlated with erlotinib sensitivity. Five sites (pT693, pY1092, pY1110, pY1172, and pY1197) were inhibited by erlotinib in concentration-dependent manner. Erlotinib sensitivity was confirmed using liquid chromatography coupled to multiple reaction monitoring (LC-MRM) and quantitative Western blotting. This LC-MS/MS strategy can quantitatively assess site-specific EGFR phosphorylation and can identify relationships between somatic mutations or drug sensitivity and protein phosphorylation.

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Year:  2010        PMID: 21080693      PMCID: PMC3050523          DOI: 10.1021/pr1006203

Source DB:  PubMed          Journal:  J Proteome Res        ISSN: 1535-3893            Impact factor:   4.466


  76 in total

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4.  Adaptive responses to dasatinib-treated lung squamous cell cancer cells harboring DDR2 mutations.

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Review 7.  Quantitative analysis of global phosphorylation changes with high-resolution tandem mass spectrometry and stable isotopic labeling.

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9.  Oncogenic KRAS and BRAF Drive Metabolic Reprogramming in Colorectal Cancer.

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10.  Autophosphorylation of EGFR at Y954 Facilitated Homodimerization and Enhanced Downstream Signals.

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