1q21

From Proteopedia

Revision as of 02:46, 3 May 2008

spinqualitylabelsall models PDB ID 1q21 Show:Asymmetric Unit Biological Assembly Drag the structure with the mouse to rotate   Export Animated Image
1q21, resolution 2.20Å ()
Ligands:	,
Structural annotation: Resources: CATH : 1Q21000 InterPro : Ipr003577, Ipr005225, Ipr001806, Ipr015592, Ipr013753 Pfam : PF00071 SCOP : d1q21__ UniProt : P01112
Functional annotation: Cellular component: Golgi apparatus intracellular cytoplasm membrane plasma membrane Biological process: small GTPase mediated signal transduction cell surface receptor linked signal transduction signal transduction chemotaxis organ morphogenesis Molecular function: protein C-terminus binding GTP binding protein binding nucleotide binding
Evolutionary conservation: Toggle Conservation Colors: Rows = identical sequences: Further Information: Caveats, Explanation, Complete Results at ConSurfDB
Resources:	FirstGlance, OCA, RCSB, PDBsum
Coordinates:	save as pdb, mmCIF, xml

CRYSTAL STRUCTURES AT 2.2 ANGSTROMS RESOLUTION OF THE CATALYTIC DOMAINS OF NORMAL RAS PROTEIN AND AN ONCOGENIC MUTANT COMPLEXED WITH GSP

Overview

The biological functions of ras proteins are controlled by the bound guanine nucleotide GDP or GTP. The GTP-bound conformation is biologically active, and is rapidly deactivated to the GDP-bound conformation through interaction with GAP (GTPase Activating Protein). Most transforming mutants of ras proteins have drastically reduced GTP hydrolysis rates even in the presence of GAP. The crystal structures of the GDP complexes of ras proteins at 2.2 A resolution reveal the detailed interaction between the ras proteins and the GDP molecule. All the currently known transforming mutation positions are clustered around the bound guanine nucleotide molecule. The presumed "effector" region and the GAP recognition region are both highly exposed. No significant structural differences were found between the GDP complexes of normal ras protein and the oncogenic mutant with valine at position 12, except the side-chain of the valine residue. However, comparison with GTP-analog complexes of ras proteins suggests that the valine side-chain may inhibit GTP hydrolysis in two possible ways: (1) interacting directly with the gamma-phosphate and altering its orientation or the conformation of protein residues around the phosphates; and/or (2) preventing either the departure of gamma-phosphate on GTP hydrolysis or the entrance of a nucleophilic group to attack the gamma-phosphate. The structural similarity between ras protein and the bacterial elongation factor Tu suggests that their common structural motif might be conserved for other guanine nucleotide binding proteins.

About this Structure

1Q21 is a Single protein structure of sequence from Homo sapiens. This structure supersedes the now removed PDB entry 2p21. Full crystallographic information is available from OCA.

Reference

Crystal structures at 2.2 A resolution of the catalytic domains of normal ras protein and an oncogenic mutant complexed with GDP., Tong LA, de Vos AM, Milburn MV, Kim SH, J Mol Biol. 1991 Feb 5;217(3):503-16. PMID:1899707 Page seeded by OCA on Sat May 3 05:46:12 2008