Differentiating a Ligand's Chemical Requirements for Allosteric Interactions from Those for Protein Binding. Phenylalanine Inhibition of Pyruvate Kinase<sup>,</sup>

Williams, Rachel; Holyoak, Todd; Mcdonald, Gissel; Gui, Chunshan; Fenton, Aron W.

doi:10.1021/bi0524262

Cited by 73 publications

(186 citation statements)

References 26 publications

(39 reference statements)

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“…Interacting residues (Asn69 and His463) are situated near each other in the 3D structure of human muscle pyruvate kinase. Here we should state that both Asn69 and His463 (see Figure 4) form allosteric binding site for proline and alanine along with Arg42, Asn43, Arg105, Tyr465, Ile468, Phe469 and Pro470 [11,30]. As one can see in Figure 4 A and Figure 4 B, Docking Server included in the area for potential binding sites search the whole beta-bundle of pyruvate kinase and some parts of the protein situated around the beta-bundle.…”

Section: Docking Of Ethanol To Human and Rat Muscle Pyruvate Kinasesmentioning

confidence: 91%

“…As one can see in Figure 4 A and Figure 4 B, Docking Server included in the area for potential binding sites search the whole beta-bundle of pyruvate kinase and some parts of the protein situated around the beta-bundle. Putative site for ethanol binding is situated under the beta-bundle of pyruvate kinase, as well as the known allosteric site for proline and alanine binding [11,30].…”

Section: Docking Of Ethanol To Human and Rat Muscle Pyruvate Kinasesmentioning

confidence: 99%

“…It is likely that ethanol may inhibit activity of muscle pyruvate kinase by the way of binding to the allosteric site which is known to be involved in interaction with several relatively small molecules, such as alanine, proline and phenylalanine [11,30].…”

Section: Docking Of Ethanol To Human and Rat Muscle Pyruvate Kinasesmentioning

confidence: 99%

“…Asn69 and His463 participate in polar interactions with the allosteric inhibitor. So, Docking Server recognized five from nine residues of the described allosteric site [11,30]. Interestingly, alanine was placed to the substrate-binding site (upon the beta-bundle and not under it) at a frequency of 90% with higher estimated free energy of binding equal to -4.88 kcal/mol.…”

Section: Docking Of Alanine To Human and Rat Muscle Pyruvate Kinasesmentioning

confidence: 99%

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The Influence of Ethanol on Pyruvate Kinases Activity in Vivo, in Vitro, in Silico

Vladimirovich¹,

Khrustalev²,

Victorovich³

et al. 2013

AJMBR

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The influence of ethanol on enzymatic activities of muscle and liver pyruvate kinases has been studied in rats in series of in vivo and in vitro experiments accompanied by in silico study. Activity of muscle pyruvate kinase significantly decreased in experiments on acute alcohol intoxication (5.0g/kg of body weight), during chronic alcohol consumption (3.5g/kg of body weight 2 times a day for 14 and 28 days) and during the abstinence after the period of alcohol consumption (5.0g/kg of body weight 2 times a day for 5 days). Activity of liver pyruvate kinase was not decreased in rats after the period of alcohol consumption (5.0g/kg of body weight 2 times a day for 5 days) and during chronic alcohol consumption (3.5g/kg of body weight 2 times a day for 28 days). It even became significantly higher during the chronic alcohol consumption (3.5g/kg of body weight 2 times a day) lasting for 14 days. Inhibitory effect of alcohol bolus on activities of both pyruvate kinases should be linked with certain indirect mechanisms, since direct inhibitory effect was seen in vitro only after the addition of 500 mM ethanol to the rat muscle and liver supernatants. Since lactate dehydrogenase is used in a coupled assay for pyruvate kinase activity estimation we approved that 500mM ethanol did not inhibit lactate dehydrogenase activity in human plasma. Direct inhibition of pyruvate kinases activities should be due to the ability of ethanol to bind amino acid residues from the known allosteric site for alanine binding on muscle and liver pyruvate kinases shown by us with the help of molecular docking. Indirect activation of liver pyruvate kinase can be explained by the increase of glucose blood levels in rats during alcohol consumption promoting dephosphorylation of the enzyme as well as expression of the gene coding for it, and the decrease of alanine concentration in liver.

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Section: Docking Of Ethanol To Human and Rat Muscle Pyruvate Kinasesmentioning

confidence: 91%

Section: Docking Of Ethanol To Human and Rat Muscle Pyruvate Kinasesmentioning

confidence: 99%

Section: Docking Of Ethanol To Human and Rat Muscle Pyruvate Kinasesmentioning

confidence: 99%

Section: Docking Of Alanine To Human and Rat Muscle Pyruvate Kinasesmentioning

confidence: 99%

See 2 more Smart Citations

The Influence of Ethanol on Pyruvate Kinases Activity in Vivo, in Vitro, in Silico

Vladimirovich¹,

Khrustalev²,

Victorovich³

et al. 2013

AJMBR

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“…2 Among them there are ACE-NEP, 3 urokinase 4 and pyruvate kinase inhibitors. 5 Modifications of phenylalanine are active against the infections caused by Gram-positive bacteria (e.g. vancomycin 6 ).…”

Section: Introductionmentioning

confidence: 99%

Chemo- and regioselective modification of D,L-phenylalanine with α-cyanoacetylenic alcohols in water

Малькина¹,

Borisova²,

Nosyreva³

et al. 2011

Arkivoc

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D,L-Phenylalanine reacts with -cyanoacetylenic alcohols under biomimetic conditions (room temperature, water) to give a novel family of unnatural amino acids, containing 2,5-dihydro-5-iminofuranyl substituents in the amino group, in almost quantitative yields (92-95%). This "green" one-pot version of the tandem assembly of nontraditional amino acids opens an unexplored avenue to the new types of drugs and their precursors.

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Cancer‐associated mutations in human pyruvate kinase M2 impair enzyme activity

et al. 2019

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Mammalian pyruvate kinase catalyzes the final step of glycolysis, and its M2 isoform (PKM2) is widely expressed in proliferative tissues. Mutations in PKM2 are found in some human cancers; however, the effects of these mutations on enzyme activity and regulation are unknown. Here, we characterized five cancer‐associated PKM2 mutations, occurring at various locations on the enzyme, with respect to substrate kinetics and activation by the allosteric activator fructose‐1,6‐bisphosphate (FBP). The mutants exhibit reduced maximal velocity, reduced substrate affinity, and/or altered activation by FBP. The kinetic parameters of five additional PKM2 mutants that have been used to study enzyme function or regulation also demonstrate the deleterious effects of mutations on PKM2 function. Our findings indicate that PKM2 is sensitive to many amino acid changes and support the hypothesis that decreased PKM2 activity is selected for in rapidly proliferating cells.

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Differentiating a Ligand's Chemical Requirements for Allosteric Interactions from Those for Protein Binding. Phenylalanine Inhibition of Pyruvate Kinase^,

Cited by 73 publications

References 26 publications

The Influence of Ethanol on Pyruvate Kinases Activity in Vivo, in Vitro, in Silico

The Influence of Ethanol on Pyruvate Kinases Activity in Vivo, in Vitro, in Silico

Chemo- and regioselective modification of D,L-phenylalanine with α-cyanoacetylenic alcohols in water

Cancer‐associated mutations in human pyruvate kinase M2 impair enzyme activity

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Differentiating a Ligand's Chemical Requirements for Allosteric Interactions from Those for Protein Binding. Phenylalanine Inhibition of Pyruvate Kinase,

Cited by 73 publications

References 26 publications

The Influence of Ethanol on Pyruvate Kinases Activity in Vivo, in Vitro, in Silico

The Influence of Ethanol on Pyruvate Kinases Activity in Vivo, in Vitro, in Silico

Chemo- and regioselective modification of D,L-phenylalanine with α-cyanoacetylenic alcohols in water

Cancer‐associated mutations in human pyruvate kinase M2 impair enzyme activity

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Product

Resources

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Differentiating a Ligand's Chemical Requirements for Allosteric Interactions from Those for Protein Binding. Phenylalanine Inhibition of Pyruvate Kinase^,