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Literature DB >> 23895500

Conformational freedom in tight binding enzymatic transition-state analogues.

Matthew W Motley¹, Vern L Schramm, Steven D Schwartz.

Abstract

Transition-state analogues of bacterial 5'-methylthioadenosine/S-adenosylhomocysteine nucleosidases (MTANs) disrupt quorum-sensing pathways in Escherichia coli and Vibrio cholerae, demonstrating the potential to limit pathogenicity without placing bacteria under intense selective pressure that leads to antibiotic resistance. Despite the similarity of the crystal structures of E. coli MTAN (EcMTAN) and V. cholerae MTAN (VcMTAN) bound to DADMe-Immucillin-A transition-state (TS) analogues, EcMTAN demonstrates femtomolar affinity for BuT-DADMe-Immucillin-A (BDIA) whereas VcMTAN possesses only picomolar affinity. Protein dynamic interactions are therefore implicated in this inhibitor affinity difference. We conducted molecular dynamics simulations of both EcMTAN and VcMTAN in complex with BDIA to explore differences in protein dynamic architecture. Simulations revealed that electrostatic and hydrophobic interactions with BDIA are similar for both enzymes and thus unlikely to account for the difference in inhibitor affinity. The EcMTAN-BDIA complex reveals a greater flexibility and conformational freedom of catalytically important atoms. We propose that conserved motions related to the EcMTAN transition state correlate with the increased affinity of BDIA for EcMTAN. Transition-state analogues permitting protein motion related to formation of the transition state are better mimics of the enzymatic transition state and can bind more tightly than those immobilizing catalytic site dynamics.

Entities: Chemical Disease Gene Species

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Year: 2013 PMID： 23895500 PMCID： PMC3786605 DOI： 10.1021/jp4030443

Source DB: PubMed Journal: J Phys Chem B ISSN： 1520-5207 Impact factor: 2.991

18 in total

Review 1. Protein crystallography for non-crystallographers, or how to get the best (but not more) from published macromolecular structures.

Authors: Alexander Wlodawer; Wladek Minor; Zbigniew Dauter; Mariusz Jaskolski
Journal: FEBS J Date: 2007-11-23 Impact factor: 5.542

Review 2. CHARMM: the biomolecular simulation program.

Authors: B R Brooks; C L Brooks; A D Mackerell; L Nilsson; R J Petrella; B Roux; Y Won; G Archontis; C Bartels; S Boresch; A Caflisch; L Caves; Q Cui; A R Dinner; M Feig; S Fischer; J Gao; M Hodoscek; W Im; K Kuczera; T Lazaridis; J Ma; V Ovchinnikov; E Paci; R W Pastor; C B Post; J Z Pu; M Schaefer; B Tidor; R M Venable; H L Woodcock; X Wu; W Yang; D M York; M Karplus
Journal: J Comput Chem Date: 2009-07-30 Impact factor: 3.376

3. Atomic detail of chemical transformation at the transition state of an enzymatic reaction.

Authors: Suwipa Saen-Oon; Sara Quaytman-Machleder; Vern L Schramm; Steven D Schwartz
Journal: Proc Natl Acad Sci U S A Date: 2008-10-22 Impact factor: 11.205

4. A 21st century revisionist's view at a turning point in enzymology.

Authors: Zachary D Nagel; Judith P Klinman
Journal: Nat Chem Biol Date: 2009-08 Impact factor: 15.040

5. Locally accessible conformations of proteins: multiple molecular dynamics simulations of crambin.

Authors: L S Caves; J D Evanseck; M Karplus
Journal: Protein Sci Date: 1998-03 Impact factor: 6.725

6. Transition state analogues for enzyme catalysis.

Authors: R Wolfenden
Journal: Nature Date: 1969-08-16 Impact factor: 49.962

7. A picomolar transition state analogue inhibitor of MTAN as a specific antibiotic for Helicobacter pylori.

Authors: Shanzhi Wang; Antti M Haapalainen; Funing Yan; Quan Du; Peter C Tyler; Gary B Evans; Agnes Rinaldo-Matthis; Rosemary L Brown; Gillian E Norris; Steven C Almo; Vern L Schramm
Journal: Biochemistry Date: 2012-08-22 Impact factor: 3.162

8. Conformational dynamics in human purine nucleoside phosphorylase with reactants and transition-state analogues.

Authors: Jennifer S Hirschi; Karunesh Arora; Charles L Brooks; Vern L Schramm
Journal: J Phys Chem B Date: 2010-10-11 Impact factor: 2.991

9. CHARMM general force field: A force field for drug-like molecules compatible with the CHARMM all-atom additive biological force fields.

Authors: K Vanommeslaeghe; E Hatcher; C Acharya; S Kundu; S Zhong; J Shim; E Darian; O Guvench; P Lopes; I Vorobyov; A D Mackerell
Journal: J Comput Chem Date: 2010-03 Impact factor: 3.376

10. Picomolar transition state analogue inhibitors of human 5'-methylthioadenosine phosphorylase and X-ray structure with MT-immucillin-A.

Authors: Vipender Singh; Wuxian Shi; Gary B Evans; Peter C Tyler; Richard H Furneaux; Steven C Almo; Vern L Schramm
Journal: Biochemistry Date: 2004-01-13 Impact factor: 3.162

8 in total

1. Transition States and transition state analogue interactions with enzymes.

Authors: Vern L Schramm
Journal: Acc Chem Res Date: 2015-04-07 Impact factor: 22.384

2. Neutron structures of the Helicobacter pylori 5'-methylthioadenosine nucleosidase highlight proton sharing and protonation states.

Authors: Michael T Banco; Vidhi Mishra; Andreas Ostermann; Tobias E Schrader; Gary B Evans; Andrey Kovalevsky; Donald R Ronning
Journal: Proc Natl Acad Sci U S A Date: 2016-11-16 Impact factor: 11.205

Conformational freedom in tight binding enzymatic transition-state analogues.

Review 1. Protein crystallography for non-crystallographers, or how to get the best (but not more) from published macromolecular structures.

Review 2. CHARMM: the biomolecular simulation program.

3. Atomic detail of chemical transformation at the transition state of an enzymatic reaction.

4. A 21st century revisionist's view at a turning point in enzymology.

5. Locally accessible conformations of proteins: multiple molecular dynamics simulations of crambin.

6. Transition state analogues for enzyme catalysis.

7. A picomolar transition state analogue inhibitor of MTAN as a specific antibiotic for Helicobacter pylori.

8. Conformational dynamics in human purine nucleoside phosphorylase with reactants and transition-state analogues.

9. CHARMM general force field: A force field for drug-like molecules compatible with the CHARMM all-atom additive biological force fields.

10. Picomolar transition state analogue inhibitors of human 5'-methylthioadenosine phosphorylase and X-ray structure with MT-immucillin-A.

1. Transition States and transition state analogue interactions with enzymes.

2. Neutron structures of the Helicobacter pylori 5'-methylthioadenosine nucleosidase highlight proton sharing and protonation states.

3. Evaluating hydrophobic galactonoamidines as transition state analogs for enzymatic β-galactoside hydrolysis.

4. Active site and remote contributions to catalysis in methylthioadenosine nucleosidases.

5. Enzyme homologues have distinct reaction paths through their transition states.

Review 6. Enzymatic Transition States and Drug Design.

7. Transition-State Analogues of Campylobacter jejuni 5'-Methylthioadenosine Nucleosidase.

8. 5-Fluorouracil blocks quorum-sensing of biofilm-embedded methicillin-resistant Staphylococcus aureus in mice.