Sandbox Reserved 1127

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==Allosteric regulation==
==Allosteric regulation==
==Positive regulation==
==Positive regulation==
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PDE5 contains several cGMP binding sites that do not have the same effect on its activity. These allosteric domains are GAF A and GAF B play a rôle in PDE5 activity. Especially GAF A(see the picture below) binds cGMP, by establishing hydrogens bonds between cGMP and the residues T,I, colored in the picture below. CGMP binding to GAF A trigegr an allosteric modification that lead to the seperation of the dimeric catalytic site of the enzyme, so that it opens cGMP access to the catalytic site.
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PDE5 contains several cGMP binding sites that do not have the same effect on its activity. These allosteric domains are GAF A and GAF B play a rôle in PDE5 activity. Especially GAF A(see the picture below) binds cGMP, by establishing hydrogens bonds between cGMP and the residues T,I, colored in the picture below.
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[[Image:Image:Free_GAF_A_domain_residues_that_binds_cGMP.png]]
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CGMP binding to GAF A trigegr an allosteric modification that lead to the seperation of the dimeric catalytic site of the enzyme, so that it opens cGMP access to the catalytic site.
This cGMP binding to allosteric sites increases the enzyme affinity to cGMP.
This cGMP binding to allosteric sites increases the enzyme affinity to cGMP.
Plus,the phosphorylation the Ser92 lead to increase the catalytic activity of the enzyme.
Plus,the phosphorylation the Ser92 lead to increase the catalytic activity of the enzyme.

Revision as of 18:57, 30 January 2016

This Sandbox is Reserved from 15/12/2015, through 15/06/2016 for use in the course "Structural Biology" taught by Bruno Kieffer at the University of Strasbourg, ESBS. This reservation includes Sandbox Reserved 1120 through Sandbox Reserved 1159.
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Human PDE5

PDE5 and its inhibitor Sildenafil

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