2gnl

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Revision as of 15:33, 21 February 2008

PKA threefold mutant model of Rho-kinase with inhibitor H-1152P

Overview

Controlling aberrant kinase-mediated cellular signaling is a major strategy in cancer therapy; successful protein kinase inhibitors such as Tarceva and Gleevec verify this approach. Specificity of inhibitors for the targeted kinase(s), however, is a crucial factor for therapeutic success. Based on homology modeling, we previously identified four amino acids in the active site of Rho-kinase that likely determine inhibitor specificities observed for Rho-kinase relative to protein kinase A (PKA) (in PKA numbering: T183A, L49I, V123M, and E127D), and a fifth (Q181K) that played a surprising role in PKA-PKB hybrid proteins. We have systematically mutated these residues in PKA to their counterparts in Rho-kinase, individually and in combination. Using four Rho-kinase-specific, one PKA-specific, and one pan-kinase-specific inhibitor, we measured the inhibitor-binding properties of the mutated proteins and identify the roles of individual residues as specificity determinants. Two combined mutant proteins, containing the combination of mutations T183A and L49I, closely mimic Rho-kinase. Kinetic results corroborate the hypothesis that side-chain identities form the major determinants of selectivity. An unexpected result of the analysis is the consistent contribution of the individual mutations by simple factors. Crystal structures of the surrogate kinase inhibitor complexes provide a detailed basis for an understanding of these selectivity determinant residues. The ability to obtain kinetic and structural data from these PKA mutants, combined with their Rho-kinase-like selectivity profiles, make them valuable for use as surrogate kinases for structure-based inhibitor design.

About this Structure

2GNL is a Protein complex structure of sequences from Bos taurus with as ligand. Active as cAMP-dependent protein kinase, with EC number 2.7.11.11 Full crystallographic information is available from OCA.

Reference

Structural analysis of protein kinase A mutants with Rho-kinase inhibitor specificity., Bonn S, Herrero S, Breitenlechner CB, Erlbruch A, Lehmann W, Engh RA, Gassel M, Bossemeyer D, J Biol Chem. 2006 Aug 25;281(34):24818-30. Epub 2006 May 12. PMID:16699172

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@@ Line 1: / Line 1: @@
-[[Image:2gnl.gif|left|200px]]<br /><applet load="2gnl" size="450" color="white" frame="true" align="right" spinBox="true"
+[[Image:2gnl.gif|left|200px]]<br /><applet load="2gnl" size="350" color="white" frame="true" align="right" spinBox="true"
 caption="2gnl, resolution 2.60&Aring;" />
 '''PKA threefold mutant model of Rho-kinase with inhibitor H-1152P'''<br />
 ==Overview==
-Controlling aberrant kinase-mediated cellular signaling is a major, strategy in cancer therapy; successful protein kinase inhibitors such as, Tarceva and Gleevec verify this approach. Specificity of inhibitors for, the targeted kinase(s), however, is a crucial factor for therapeutic, success. Based on homology modeling, we previously identified four amino, acids in the active site of Rho-kinase that likely determine inhibitor, specificities observed for Rho-kinase relative to protein kinase A (PKA), (in PKA numbering: T183A, L49I, V123M, and E127D), and a fifth (Q181K), that played a surprising role in PKA-PKB hybrid proteins. We have, systematically mutated these residues in PKA to their counterparts in, Rho-kinase, individually and in combination. Using four, Rho-kinase-specific, one PKA-specific, and one pan-kinase-specific, inhibitor, we measured the inhibitor-binding properties of the mutated, proteins and identify the roles of individual residues as specificity, determinants. Two combined mutant proteins, containing the combination of, mutations T183A and L49I, closely mimic Rho-kinase. Kinetic results, corroborate the hypothesis that side-chain identities form the major, determinants of selectivity. An unexpected result of the analysis is the, consistent contribution of the individual mutations by simple factors., Crystal structures of the surrogate kinase inhibitor complexes provide a, detailed basis for an understanding of these selectivity determinant, residues. The ability to obtain kinetic and structural data from these PKA, mutants, combined with their Rho-kinase-like selectivity profiles, make, them valuable for use as surrogate kinases for structure-based inhibitor, design.
+Controlling aberrant kinase-mediated cellular signaling is a major strategy in cancer therapy; successful protein kinase inhibitors such as Tarceva and Gleevec verify this approach. Specificity of inhibitors for the targeted kinase(s), however, is a crucial factor for therapeutic success. Based on homology modeling, we previously identified four amino acids in the active site of Rho-kinase that likely determine inhibitor specificities observed for Rho-kinase relative to protein kinase A (PKA) (in PKA numbering: T183A, L49I, V123M, and E127D), and a fifth (Q181K) that played a surprising role in PKA-PKB hybrid proteins. We have systematically mutated these residues in PKA to their counterparts in Rho-kinase, individually and in combination. Using four Rho-kinase-specific, one PKA-specific, and one pan-kinase-specific inhibitor, we measured the inhibitor-binding properties of the mutated proteins and identify the roles of individual residues as specificity determinants. Two combined mutant proteins, containing the combination of mutations T183A and L49I, closely mimic Rho-kinase. Kinetic results corroborate the hypothesis that side-chain identities form the major determinants of selectivity. An unexpected result of the analysis is the consistent contribution of the individual mutations by simple factors. Crystal structures of the surrogate kinase inhibitor complexes provide a detailed basis for an understanding of these selectivity determinant residues. The ability to obtain kinetic and structural data from these PKA mutants, combined with their Rho-kinase-like selectivity profiles, make them valuable for use as surrogate kinases for structure-based inhibitor design.
 ==About this Structure==
-GNL is a [http://en.wikipedia.org/wiki/Protein_complex Protein complex] structure of sequences from [http://en.wikipedia.org/wiki/Bos_taurus Bos taurus] with H52 as [http://en.wikipedia.org/wiki/ligand ligand]. Active as [http://en.wikipedia.org/wiki/cAMP-dependent_protein_kinase cAMP-dependent protein kinase], with EC number [http://www.brenda-enzymes.info/php/result_flat.php4?ecno=2.7.11.11 2.7.11.11] Full crystallographic information is available from [http://ispc.weizmann.ac.il/oca-bin/ocashort?id=2GNL OCA].
+GNL is a [http://en.wikipedia.org/wiki/Protein_complex Protein complex] structure of sequences from [http://en.wikipedia.org/wiki/Bos_taurus Bos taurus] with <scene name='pdbligand=H52:'>H52</scene> as [http://en.wikipedia.org/wiki/ligand ligand]. Active as [http://en.wikipedia.org/wiki/cAMP-dependent_protein_kinase cAMP-dependent protein kinase], with EC number [http://www.brenda-enzymes.info/php/result_flat.php4?ecno=2.7.11.11 2.7.11.11] Full crystallographic information is available from [http://oca.weizmann.ac.il/oca-bin/ocashort?id=2GNL OCA].
 ==Reference==
@@ Line 16: / Line 16: @@
 [[Category: Bonn, S.]]
 [[Category: Bossemeyer, D.]]
-[[Category: Breitenlechner, C.B.]]
+[[Category: Breitenlechner, C B.]]
-[[Category: Engh, R.A.]]
+[[Category: Engh, R A.]]
 [[Category: Gassel, M.]]
 [[Category: Herrero, S.]]
@@ Line 28: / Line 28: @@
 [[Category: surrogate]]
-''Page seeded by [http://ispc.weizmann.ac.il/oca OCA ] on Wed Nov 21 11:17:55 2007''
+''Page seeded by [http://oca.weizmann.ac.il/oca OCA ] on Thu Feb 21 17:33:30 2008''

2gnl

From Proteopedia

Revision as of 15:33, 21 February 2008

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About this Structure

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