Literature DB >> 21709760

Locostatin Disrupts Association of Raf Kinase Inhibitor Protein With Binding Proteins by Modifying a Conserved Histidine Residue in the Ligand-Binding Pocket.

Anwar B Beshir1, Christian E Argueta, Lochana C Menikarachchi, José A Gascón, Gabriel Fenteany.   

Abstract

Raf kinase inhibitor protein (RKIP) interacts with a number of different proteins and regulates multiple signaling pathways. Here, we show that locostatin, a small molecule that covalently binds RKIP, not only disrupts interactions of RKIP with Raf-1 kinase, but also with G protein-coupled receptor kinase 2. In contrast, we found that locostatin does not disrupt binding of RKIP to two other proteins: inhibitor of κB kinase α and transforming growth factor β-activated kinase 1. These results thus imply that different proteins interact with different regions of RKIP. Locostatin's mechanism of action involves modification of a nucleophilic residue on RKIP. We observed that after binding RKIP, part of locostatin is slowly hydrolyzed, leaving a smaller RKIP-butyrate adduct. We identified the residue alkylated by locostatin as His86, a highly conserved residue in RKIP's ligand-binding pocket. Computational modeling of the binding of locostatin to RKIP suggested that the recognition interaction between small molecule and protein ensures that locostatin's electrophilic site is poised to react with His86. Furthermore, binding of locostatin would sterically hinder binding of other ligands in the pocket. These data provide a basis for understanding how locostatin disrupts particular interactions of RKIP with RKIP-binding proteins and demonstrate its utility as a probe of specific RKIP interactions and functions.

Entities:  

Year:  2011        PMID: 21709760      PMCID: PMC3121171          DOI: 10.1615/forumimmundisther.v2.i1.60

Source DB:  PubMed          Journal:  For Immunopathol Dis Therap        ISSN: 2151-8017


  25 in total

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Review 3.  RKIP structure drives its function: a three-state model for regulation of RKIP.

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Review 4.  Interactions of RKIP with inflammatory signaling pathways.

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5.  RKIP contributes to IFN-γ synthesis by CD8+ T cells after serial TCR triggering in systemic inflammatory response syndrome.

Authors:  Kyle T Wright; Anthony T Vella
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6.  Mapping the interactome of overexpressed RAF kinase inhibitor protein in a gastric cancer cell line.

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Review 7.  RKIP as an Inflammatory and Immune System Modulator: Implications in Cancer.

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8.  Investigation of Marine-Derived Natural Products as Raf Kinase Inhibitory Protein (RKIP)-Binding Ligands.

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Review 10.  RKIP Pleiotropic Activities in Cancer and Inflammatory Diseases: Role in Immunity.

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  10 in total

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