Literature DB >> 20512974

Dissecting the cAMP-inducible allosteric switch in protein kinase A RIalpha.

Timothy J Sjoberg1, Alexandr P Kornev, Susan S Taylor.   

Abstract

The regulatory subunits of cAMP-dependent protein kinase (PKA) are the major receptors of cAMP in most eukaryotic cells. As the cyclic nucleotide binding (CNB) domains release cAMP and bind to the catalytic subunit of PKA, they undergo a major conformational change. The change is mediated by the B/C helix in CNB-A, which extends into one long helix that now separates the two CNB domains and docks onto the surface of the catalytic subunit. We explore here the role of three key residues on the B/C helix that dock onto the catalytic subunit, Arg226, Leu233, and Met 234. By replacing each residue with Ala, we show that each contributes significantly to creating the R:C interface. By also deleting the second CNB domain (CNB-B), we show furthermore that CNB-B is a critical part of the cAMP-induced conformational switch that dislodges the B/C helix from the surface of the catalytic subunit. Without CNB-B the K(a) for activation by cAMP increases from 80 to 1000 nM. Replacing any of the key interface residues with Ala reduces the K(a) to 25-40 nM. Leu233 and M234 contribute to a hydrophobic latch that binds the B/C helix onto the large lobe of the C-subunit, while Arg226 is part of an electrostatic switch that couples the B/C helix to the phosphate binding cassette where the cAMP docks.

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Year:  2010        PMID: 20512974      PMCID: PMC2895245          DOI: 10.1002/pro.400

Source DB:  PubMed          Journal:  Protein Sci        ISSN: 0961-8368            Impact factor:   6.725


  31 in total

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3.  A simple electrostatic switch important in the activation of type I protein kinase A by cyclic AMP.

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4.  Structural basis for cAMP-mediated allosteric control of the catabolite activator protein.

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5.  Probing the multidomain structure of the type I regulatory subunit of cAMP-dependent protein kinase using mutational analysis: role and environment of endogenous tryptophans.

Authors:  D A Leon; J M Canaves; S S Taylor
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6.  Structure of the cyclic-AMP-responsive exchange factor Epac2 in its auto-inhibited state.

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8.  Novel isoform-specific interfaces revealed by PKA RIIbeta holoenzyme structures.

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9.  PKA type IIalpha holoenzyme reveals a combinatorial strategy for isoform diversity.

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  17 in total

1.  Molecular Simulations Reveal an Unresolved Conformation of the Type IA Protein Kinase A Regulatory Subunit and Suggest Its Role in the cAMP Regulatory Mechanism.

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2.  Identifying the hub gene and immune infiltration of osteoarthritis by bioinformatical methods.

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3.  cAMPr: A single-wavelength fluorescent sensor for cyclic AMP.

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4.  Electrostatic Interactions as Mediators in the Allosteric Activation of Protein Kinase A RIα.

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Review 6.  Towards Kinase Inhibitor Therapies for Fragile X Syndrome: Tweaking Twists in the Autism Spectrum Kinase Signaling Network.

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

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8.  Allostery through the computational microscope: cAMP activation of a canonical signalling domain.

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9.  Evolutionary paths of the cAMP-dependent protein kinase (PKA) catalytic subunits.

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Review 10.  Bridging scales through multiscale modeling: a case study on protein kinase A.

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