Literature DB >> 17165815

Assay principle for modulators of protein-protein interactions and its application to non-ATP-competitive ligands targeting protein kinase A.

S Adrian Saldanha1, Gregory Kaler, Howard B Cottam, Ruben Abagyan, Susan S Taylor.   

Abstract

Targeting sites that modulate protein-protein interactions represents an ongoing challenge for drug discovery. We have devised an assay principle, named ligand-regulated competition (LiReC), in an effort to find non-ATP competitive small-molecule regulators for type Ialpha cAMP-dependent Protein kinase (PKA-Ialpha), a protein complex that is implicated in disease. Our assay based on the LiReC principle utilizes a competitive fluorescent peptide probe to assess the integrity of the PKA-Ialpha complex upon introduction of an allosteric ligand. The developed fluorescence polarization method screens for small molecules that specifically protect (antagonists) or conversely activate (agonists) this protein complex. In high-throughput format, various cyclic nucleotide-derived agonists and antagonists are successfully detected with high precision. Furthermore, assay performance (Z'-factors above 0.7) far exceeds the minimum requirement for small-molecule screening. To identify compounds that operate through novel modes of action, our method shields the ATP-binding site and purposely excludes ATP-competitive ligands. These proof-of-principle experiments highlight the potential of the LiReC technique and suggest its application to other protein complexes, thereby providing a novel approach to identify and characterize modulators (small molecules, proteins, peptides, or nucleic acids) of protein-protein systems.

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Year:  2006        PMID: 17165815      PMCID: PMC3435108          DOI: 10.1021/ac061104g

Source DB:  PubMed          Journal:  Anal Chem        ISSN: 0003-2700            Impact factor:   6.986


  40 in total

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Authors: 
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Review 3.  Fluorescence polarization and anisotropy in high throughput screening: perspectives and primer.

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4.  RIalpha subunit of PKA: a cAMP-free structure reveals a hydrophobic capping mechanism for docking cAMP into site B.

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Journal:  Structure       Date:  2004-06       Impact factor: 5.006

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6.  Staurosporine, a protein kinase C inhibitor interferes with proliferation of arterial smooth muscle cells.

Authors:  H Matsumoto; Y Sasaki
Journal:  Biochem Biophys Res Commun       Date:  1989-01-16       Impact factor: 3.575

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8.  Mutations in the protein kinase A R1alpha regulatory subunit cause familial cardiac myxomas and Carney complex.

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9.  Synergistic binding of nucleotides and inhibitors to cAMP-dependent protein kinase examined by acrylodan fluorescence spectroscopy.

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  13 in total

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7.  Structure of a PKA RIα Recurrent Acrodysostosis Mutant Explains Defective cAMP-Dependent Activation.

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9.  Realizing the allosteric potential of the tetrameric protein kinase A RIα holoenzyme.

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10.  PKA RIα homodimer structure reveals an intermolecular interface with implications for cooperative cAMP binding and Carney complex disease.

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