1L6E
Solution structure of the docking and dimerization domain of protein kinase A II-alpha (RIIalpha D/D). Alternatively called the N-terminal dimerization domain of the regulatory subunit of protein kinase A.
Summary for 1L6E
| Entry DOI | 10.2210/pdb1l6e/pdb |
| Related | 1R2A |
| NMR Information | BMRB: 4473 |
| Descriptor | cAMP-dependent protein kinase Type II-alpha regulatory chain (1 entity in total) |
| Functional Keywords | four-helix bundle, helix-loop-helix, regulatory subunit, dimerization, docking, anchoring, transferase |
| Biological source | Mus musculus (house mouse) |
| Total number of polymer chains | 2 |
| Total formula weight | 10796.36 |
| Authors | Morikis, D.,Roy, M.,Newlon, M.G.,Scott, J.D.,Jennings, P.A. (deposition date: 2002-03-08, release date: 2002-04-03, Last modification date: 2024-05-22) |
| Primary citation | Morikis, D.,Roy, M.,Newlon, M.G.,Scott, J.D.,Jennings, P.A. Electrostatic properties of the structure of the docking and dimerization domain of protein kinase A IIalpha Eur.J.Biochem., 269:2040-2051, 2002 Cited by PubMed Abstract: The structure of the N-terminal docking and dimerization domain of the type IIalpha regulatory subunit (RIIalpha D/D) of protein kinase A (PKA) forms a noncovalent stand-alone X-type four-helix bundle structural motif, consisting of two helix-loop-helix monomers. RIIalpha D/D possesses a strong hydrophobic core and two distinct, exposed faces. A hydrophobic face with a groove is the site of protein-protein interactions necessary for subcellular localization. A highly charged face, opposite to the former, may be involved in regulation of protein-protein interactions as a result of changes in phosphorylation state of the regulatory subunit. Although recent studies have addressed the hydrophobic character of packing of RIIalpha D/D and revealed the function of the hydrophobic face as the binding site to A-kinase anchoring proteins (AKAPs), little attention has been paid to the charges involved in structure and function. To examine the electrostatic character of the structure of RIIalpha D/D we have predicted mean apparent pKa values, based on Poisson-Boltzmann electrostatic calculations, using an ensemble of calculated dimer structures. We propose that the helix promoting sequence Glu34-X-X-X-Arg38 stabilizes the second helix of each monomer, through the formation of a (i, i +4) side chain salt bridge. We show that a weak inter-helical hydrogen bond between Tyr35-Glu19 of each monomer contributes to tertiary packing and may be responsible for discriminating from alternative quaternary packing of the two monomers. We also show that an inter-monomer hydrogen bond between Asp30-Arg40 contributes to quaternary packing. We propose that the charged face comprising of Asp27-Asp30-Glu34-Arg38-Arg40-Glu41-Arg43-Arg44 may be necessary to provide flexibility or stability in the region between the C-terminus and the interdomain/autoinhibitory sequence of RIIalpha, depending on the activation state of PKA. We also discuss the structural requirements necessary for the formation of a stacked (rather than intertwined) dimer, which has consequences for the orientation of the functionally important and distinct faces. PubMed: 11985580DOI: 10.1046/j.1432-1033.2002.02852.x PDB entries with the same primary citation |
| Experimental method | SOLUTION NMR |
Structure validation
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