Literature DB >> 14676314

High-throughput analysis of protein/peptide complexes by immunoprecipitation and automated LC-MS/MS.

Zhaosheng Lin1, David K Crockett, Megan S Lim, Kojo S J Elenitoba-Johnson.   

Abstract

BACKGROUND: The identification of interacting proteins within protein complexes is key to understanding the transduction and regulation of cell signaling pathways, and is also a useful tool for identifying novel disease markers. Immunoprecipitation of protein complexes followed by liquid chromatography-tandem mass spectrometry (LC-MS/MS) has been used to identify targets that bind to a protein of interest. Here, we report a high-throughput nanoflow LC-MS/MS method for analysis of protein/peptide complexes. APPROACH: To overcome the large dwell volume from connecting lines and the injector when using an autosampler in microcapillary LC-MS/MS, we employed a valve-controlled variable flow method with a peptide trap. This method enables fast trapping of peptides from samples injected by an autosampler within minutes followed by a split-controlled nanoflow of acetonitrile gradient through a microcapillary C18 column to separate and elute peptides into the ion-trap MS/MS. Over 40 protein/peptide samples at femtomole levels could be analyzed continuously using the same in-house packed microcapillary C18 column. The p38 mitogen-activated protein kinase (p38 MAP kinase) is a signaling protein that is involved in transduction of extracellular signals including oxidative stress, growth factors, and cytokines, with diverse cellular consequences such as cell proliferation, differentiation, or apoptosis. Immunocomplex of monoclonal anti-p38 beta antibodies from 2 mg total lysates from the OCI LY-1 lymphoma cell line was resolved in 1D-PAGE gel followed by silver staining of the gel. Protein bands were excised and digested with trypsin. Peptides were extracted and analyzed using the automated LC-MS/MS method. RESULTS AND
CONCLUSIONS: From 37 excised protein bands in the 1D-PAGE gel, we identified more than 50 proteins, including cytoskeletal proteins, ribosomal proteins, transcription factors, and KIAA potential signaling proteins. These proteins are the potential targets that may interact directly or indirectly with the p38 MAP kinase proteins. Our studies demonstrate the utility of automated nanoflow LC-MS/MS for sensitive and high-throughput analysis of protein/peptide complexes. Utilization of methods based on this principle would greatly facilitate peptide interaction mapping and other proteomic studies requiring high-throughput pre-analytical sample preparation.

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Year:  2003        PMID: 14676314      PMCID: PMC2279905     

Source DB:  PubMed          Journal:  J Biomol Tech        ISSN: 1524-0215


  11 in total

1.  Identification of novel MAP kinase pathway signaling targets by functional proteomics and mass spectrometry.

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Journal:  Mol Cell       Date:  2000-12       Impact factor: 17.970

Review 2.  Regulation of Na-K-2Cl cotransport by phosphorylation and protein-protein interactions.

Authors:  Peter W Flatman
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3.  Identification of CDK4 sequences involved in cyclin D1 and p16 binding.

Authors:  K G Coleman; B S Wautlet; D Morrissey; J Mulheron; S A Sedman; P Brinkley; S Price; K R Webster
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4.  Induction of p27(KIP1) as a mechanism underlying NS398-induced growth inhibition in human lung cancer cells.

Authors:  W C Hung; H C Chang; M R Pan; T H Lee; L Y Chuang
Journal:  Mol Pharmacol       Date:  2000-12       Impact factor: 4.436

Review 5.  Protein-protein interactions required during translation.

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6.  Development of a multiplexed microcapillary liquid chromatography system for high-throughput proteome analysis.

Authors:  Hookeun Lee; Timothy J Griffin; Steven P Gygi; Beate Rist; Ruedi Aebersold
Journal:  Anal Chem       Date:  2002-09-01       Impact factor: 6.986

7.  Evaluation of multidimensional chromatography coupled with tandem mass spectrometry (LC/LC-MS/MS) for large-scale protein analysis: the yeast proteome.

Authors:  Junmin Peng; Joshua E Elias; Carson C Thoreen; Larry J Licklider; Steven P Gygi
Journal:  J Proteome Res       Date:  2003 Jan-Feb       Impact factor: 4.466

Review 8.  p21: structure and functions associated with cyclin-CDK binding.

Authors:  K L Ball
Journal:  Prog Cell Cycle Res       Date:  1997

9.  Protein kinase C epsilon signaling complexes include metabolism- and transcription/translation-related proteins: complimentary separation techniques with LC/MS/MS.

Authors:  Ricky D Edmondson; Thomas M Vondriska; Kelli J Biederman; Jun Zhang; Richard C Jones; Yuting Zheng; David L Allen; Joanne X Xiu; Ernest M Cardwell; Michael R Pisano; Peipei Ping
Journal:  Mol Cell Proteomics       Date:  2002-06       Impact factor: 5.911

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Authors:  H Kiyokawa; R D Kineman; K O Manova-Todorova; V C Soares; E S Hoffman; M Ono; D Khanam; A C Hayday; L A Frohman; A Koff
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  6 in total

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Authors:  David K Crockett; Charles E Seiler; Kojo S J Elenitoba-Johnson; Megan S Lim
Journal:  J Biomol Tech       Date:  2005-12

2.  Splice variants of neuronal nitric oxide synthase are present in the rat kidney.

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3.  Increased oxidation and degradation of cytosolic proteins in alcohol-exposed mouse liver and hepatoma cells.

Authors:  Bong-Jo Kim; Brian L Hood; Richard A Aragon; James P Hardwick; Thomas P Conrads; Timothy D Veenstra; Byoung J Song
Journal:  Proteomics       Date:  2006-02       Impact factor: 3.984

4.  Deoxynivalenol induces p38 interaction with the ribosome in monocytes and macrophages.

Authors:  Hee Kyong Bae; James J Pestka
Journal:  Toxicol Sci       Date:  2008-05-22       Impact factor: 4.849

5.  Proteomic-based identification of CD4-interacting proteins in human primary macrophages.

Authors:  Rui André Saraiva Raposo; Benjamin Thomas; Gabriela Ridlova; William James
Journal:  PLoS One       Date:  2011-04-13       Impact factor: 3.240

6.  Epigenetic modulation of immune synaptic-cytoskeletal networks potentiates γδ T cell-mediated cytotoxicity in lung cancer.

Authors:  Rueyhung R Weng; Hsuan-Hsuan Lu; Chien-Ting Lin; Chia-Chi Fan; Rong-Shan Lin; Tai-Chung Huang; Shu-Yung Lin; Yi-Jhen Huang; Yi-Hsiu Juan; Yi-Chieh Wu; Zheng-Ci Hung; Chi Liu; Xuan-Hui Lin; Wan-Chen Hsieh; Tzu-Yuan Chiu; Jung-Chi Liao; Yen-Ling Chiu; Shih-Yu Chen; Chong-Jen Yu; Hsing-Chen Tsai
Journal:  Nat Commun       Date:  2021-04-12       Impact factor: 14.919

  6 in total

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