Title : Structural and mutational studies of organophosphorus hydrolase reveal a cryptic and functional allosteric-binding site - Grimsley_2005_Arch.Biochem.Biophys_442_169 |
Author(s) : Grimsley JK , Calamini B , Wild JR , Mesecar AD |
Ref : Archives of Biochemistry & Biophysics , 442 :169 , 2005 |
Abstract :
Organophosphorus hydrolase detoxifies a broad range of organophosphate pesticides and the chemical warfare agents (CWAs) sarin and VX. Previously, rational genetic engineering produced OPH variants with 30-fold enhancements in the hydrolysis of CWA and their analogs. One interesting variant (H254R) in which the histidine at position 254 was changed to an arginine showed a 4-fold increase in the hydrolysis of demetonS (VX analog), a 14-fold decrease with paraoxon (an insecticide), and a 183-fold decrease with DFP (sarin analog). The three-dimensional structure of this enzyme at 1.9A resolution with the inhibitor, diethyl 4-methylbenzylphosphonate (EBP), revealed that the inhibitor did not bind at the active site, but bound exclusively into a well-defined surface pocket 12 A away from the active site. This structural feature was accompanied by non-competitive inhibition of paraoxon hydrolysis by EBP with H254R, in contrast to the native enzyme, which showed competitive inhibition. These parallel structure-function characteristics identify a functional, allosteric site on the surface of this enzyme. |
PubMedSearch : Grimsley_2005_Arch.Biochem.Biophys_442_169 |
PubMedID: 16188223 |
Inhibitor | SCHEMBL3294100 |
Grimsley JK, Calamini B, Wild JR, Mesecar AD (2005)
Structural and mutational studies of organophosphorus hydrolase reveal a cryptic and functional allosteric-binding site
Archives of Biochemistry & Biophysics
442 :169
Grimsley JK, Calamini B, Wild JR, Mesecar AD (2005)
Archives of Biochemistry & Biophysics
442 :169