Pyruvate phosphate dikinase: Difference between revisions

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You may also [https://carb.umbi.umd.edu/files/ppdk_release.mpg download] the full High Resolution video.
You may also [https://carb.umbi.umd.edu/files/ppdk_release.mpg download] the full High Resolution video.
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Two PEP-utilizing enzymes function in vastly different biological contexts, yet both catalyze phosphoryl group transfer by shuttling a phosphohistidine residue between remote active centers. These enzymes utilize a swivel domain mechanism to deliver the phosphoryl group to the appropriate substrate.
Pyruvate phosphate dikinase (PPDK) catalyzes the inter-conversion of adenosine triphosphate (ATP), PO4-3, and pyruvate with adenine monophosphate (AMP), pyrophosphate (P2O7-4), and phosphoenolpyruvate (PEP) in the presence of Mg2+ and K+/Na+. The three-step reversible reaction proceeds via phosphoenzyme and pyrophosphoenzyme intermediates with a histidine residue serving as the phosphocarrier:
         
== (1) PPDK-His + PEP ⇄ PPDK-His~PO3 + pyruvate ==
== (2) PPDK-His~PO3 + P2O7  ⇄ PPDK-His~P2O7 + PO3 ==
== (3) PPDK-His~P2O7 + AMP ⇄ PPDK-His + ATP ==
 
The enzyme contains two remotely located reaction centers(~45 Å apart; the PEP/pyruvate partial reaction (step 1) takes place at the C-terminal domain (adopting an α/β barrel fold) and the nucleotide and inorganic phosphate partial reactions (steps 2 and 3) take place at the N-terminal domain (adopting the ATP grasp fold with two sub domains). A central domain, tethered to the N- and C-terminal domains by two closely-associated linkers, contains a phosphorylatable histidine residue (His455). To shuttle the phosphoryl group between the two reaction centers, the His-domain undergoes a ~110° swivel motion around the two linkers. In addition, upon detachment from the His-domain, the two nucleotide-binding sub domains undergo a ~40° hinge motion that opens the active site cleft.
 
The movie depicts the catalytic reaction involving three in-line phosphotransfers and the accompanied protein conformational transitions. This is a model based on crystal structures of PPDK in the two extreme conformational states and of complexes bound to substrate analogs, phosphonopyruvate and 5'-adenylyl-β,γ -imidodiphosphate (AMPPNP). The nucleotide binding subdomains are colored green and blue. The PEP binding domain is colored cyan. The His-domain is colored yellow, and the linker segments that connect the His-domain to the partner domains are colored red. Ligands and the catalytic histidine are depicted in stick models with the atomic color scheme: Carbon – gray, Nitrogen – blue, Oxygen – red, Phosphorous – green, Magnesium – magenta.
   
References:
 
1. Herzberg, O., Chen, C. C. H., Kapadia, G., McGuire, M., Carroll, L. J., Noh, S. J., Dunaway-Mariano, D. (1996) Swiveling-domain mechanism for enzymatic phosphotransfer between remote reaction sites, Proc Natl Acad Sci 93, 2652-2657.
 
2. Herzberg, O., Chen, C. C. H., Liu, S., Tempczyk, A., Howard, A., Wei, M., Ye, D., Dunaway-Mariano, D. (2002) Pyruvate site of pyruvate phosphate dikinase: crystal structure of the enzyme-phosphonopyruvate complex, and mutant analysis, Biochemistry 41, 780-787.
 
3. Lim, K., Read, R. J., Chen, C. C., Tempczyk, A., Wei, M., Ye, D., Wu, C., Dunaway-Mariano, D., and Herzberg, O. (2007) Swiveling domain mechanism in pyruvate phosphate dikinase, Biochemistry 46, 14845-14853.


Pyruvate phosphate dikinase (PPDK), catalyzes the interconversion of PEP, AMP and PPi to pyruvate, ATP and Pi. The PEP/pyruvate bind in a site remotely located from the nucleotide and phosphate binding site. Enzyme I of the bacterial PEP:sugar phosphotransferase system (PTS), transfers the phosphoryl group of PEP to the next PTS protein, HPr. HPr~P then proceeds to phosphorylate a sugar specific permease responsible for the uptake of the incoming sugar. Again, PEP and HPR bind remotely from one another.
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Revision as of 00:55, 19 August 2008

Pyruvate phosphate dikinase, A Molecular MachinePyruvate phosphate dikinase, A Molecular Machine

(this is a very preliminar page for Dr Osnat Herzberg)

<swf width="300" height="300">https://carb.umbi.umd.edu/system/files/ppdk_release.swf</swf>

You may also download the full High Resolution video.

Pyruvate phosphate dikinase (PPDK) catalyzes the inter-conversion of adenosine triphosphate (ATP), PO4-3, and pyruvate with adenine monophosphate (AMP), pyrophosphate (P2O7-4), and phosphoenolpyruvate (PEP) in the presence of Mg2+ and K+/Na+. The three-step reversible reaction proceeds via phosphoenzyme and pyrophosphoenzyme intermediates with a histidine residue serving as the phosphocarrier:

(1) PPDK-His + PEP ⇄ PPDK-His~PO3 + pyruvate(1) PPDK-His + PEP ⇄ PPDK-His~PO3 + pyruvate

(2) PPDK-His~PO3 + P2O7 ⇄ PPDK-His~P2O7 + PO3(2) PPDK-His~PO3 + P2O7 ⇄ PPDK-His~P2O7 + PO3

(3) PPDK-His~P2O7 + AMP ⇄ PPDK-His + ATP(3) PPDK-His~P2O7 + AMP ⇄ PPDK-His + ATP

The enzyme contains two remotely located reaction centers(~45 Å apart; the PEP/pyruvate partial reaction (step 1) takes place at the C-terminal domain (adopting an α/β barrel fold) and the nucleotide and inorganic phosphate partial reactions (steps 2 and 3) take place at the N-terminal domain (adopting the ATP grasp fold with two sub domains). A central domain, tethered to the N- and C-terminal domains by two closely-associated linkers, contains a phosphorylatable histidine residue (His455). To shuttle the phosphoryl group between the two reaction centers, the His-domain undergoes a ~110° swivel motion around the two linkers. In addition, upon detachment from the His-domain, the two nucleotide-binding sub domains undergo a ~40° hinge motion that opens the active site cleft.

The movie depicts the catalytic reaction involving three in-line phosphotransfers and the accompanied protein conformational transitions. This is a model based on crystal structures of PPDK in the two extreme conformational states and of complexes bound to substrate analogs, phosphonopyruvate and 5'-adenylyl-β,γ -imidodiphosphate (AMPPNP). The nucleotide binding subdomains are colored green and blue. The PEP binding domain is colored cyan. The His-domain is colored yellow, and the linker segments that connect the His-domain to the partner domains are colored red. Ligands and the catalytic histidine are depicted in stick models with the atomic color scheme: Carbon – gray, Nitrogen – blue, Oxygen – red, Phosphorous – green, Magnesium – magenta.

References:

1. Herzberg, O., Chen, C. C. H., Kapadia, G., McGuire, M., Carroll, L. J., Noh, S. J., Dunaway-Mariano, D. (1996) Swiveling-domain mechanism for enzymatic phosphotransfer between remote reaction sites, Proc Natl Acad Sci 93, 2652-2657.

2. Herzberg, O., Chen, C. C. H., Liu, S., Tempczyk, A., Howard, A., Wei, M., Ye, D., Dunaway-Mariano, D. (2002) Pyruvate site of pyruvate phosphate dikinase: crystal structure of the enzyme-phosphonopyruvate complex, and mutant analysis, Biochemistry 41, 780-787.

3. Lim, K., Read, R. J., Chen, C. C., Tempczyk, A., Wei, M., Ye, D., Wu, C., Dunaway-Mariano, D., and Herzberg, O. (2007) Swiveling domain mechanism in pyruvate phosphate dikinase, Biochemistry 46, 14845-14853.

Proteopedia Page Contributors and Editors (what is this?)Proteopedia Page Contributors and Editors (what is this?)

Jaime Prilusky, Osnat Herzberg, Eran Hodis, Dan Bolser, David Canner, Michal Harel, Alexander Berchansky, Karl Oberholser, Joel L. Sussman
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