User:Adrian Aldrich/Prokaryotic Glutamine Synthetase Pfam Domains Outline

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The beta grasp domain is the N-terminal domain, extending from residues 13-94. This domain is responsible for binding ATP, Glutamate, and Ammonia. ATP binds first, activating the site for binding glutamate.
The beta grasp domain is the N-terminal domain, extending from residues 13-94. This domain is responsible for binding ATP, Glutamate, and Ammonia. ATP binds first, activating the site for binding glutamate.
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<applet load='Betagrasp' size='300' frame='true' align='right' caption='The Prokaryotic Glutamine Synthetase Beta-Grasp Domain' />
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<scene name='User:Adrian_Aldrich/Prokaryotic_Glutamine_Synthetase_Pfam_Domains_Outline/Betagrasp/1'>Prokaryotic Glutamine Synthetase Beta-Grasp Domain</scene>

Revision as of 23:37, 16 December 2008

Prokaryotic Glutamine Synthetase Tertiary Structure: PFam domains

Prokaryotic Glutamine Synthetase is a dodecamer, comprised of 12 identical polypeptide chains, organized as a dimer of two disk like hexamers. Each protomer contains 2 Pfam domains, the Beta Grasp domain and the catalytic domain, preceded by meanders of a few resides in length which link the protomers together in the dodecamers core.

Beta Grasp domain

The beta grasp domain is the N-terminal domain, extending from residues 13-94. This domain is responsible for binding ATP, Glutamate, and Ammonia. ATP binds first, activating the site for binding glutamate.


Catalytic domain

The catalytic domain is the C-terminal domain, extending from residues 101-382.

The Prokaryotic Glutamine Synthetase Catalytic Domain

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Active site

The dodecamer contains 12 active sites total, each formed from the Beta grasp domain of one protomer and the Catalytic domain of the neighboring protomer.

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PDB ID 1lgr

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1lgr, resolution 2.79Å ()
Ligands: ,
Activity: Glutamate--ammonia ligase, with EC number 6.3.1.2
Resources: FirstGlance, OCA, PDBsum, RCSB
Coordinates: save as pdb, mmCIF, xml


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Adrian Aldrich

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