Your search keyword '"Bax BD"' showing total 27 results

1. How Do Gepotidacin and Zoliflodacin Stabilize DNA-Cleavage Complexes with Bacterial Type IIA Topoisomerases? 2. A Single Moving Metal Mechanism.

Author

Nicholls RA, Morgan H, Warren AJ, Ward SE, Long F, Murshudov GN, Sutormin D, and Bax BD

Subjects

DNA Topoisomerases, Type II metabolism, DNA Topoisomerases, Type II chemistry, Topoisomerase II Inhibitors pharmacology, Topoisomerase II Inhibitors chemistry, Acenaphthenes chemistry, Acenaphthenes metabolism, Models, Molecular, Fluoroquinolones pharmacology, Fluoroquinolones chemistry, Fluoroquinolones metabolism, DNA Gyrase metabolism, DNA Gyrase chemistry, Crystallography, X-Ray, Heterocyclic Compounds, 3-Ring, DNA Cleavage

Abstract

DNA gyrase is a bacterial type IIA topoisomerase that can create temporary double-stranded DNA breaks to regulate DNA topology and an archetypical target of antibiotics. The widely used quinolone class of drugs use a water-metal ion bridge in interacting with the GyrA subunit of DNA gyrase. Zoliflodacin sits in the same pocket as quinolones but interacts with the GyrB subunit and also stabilizes lethal double-stranded DNA breaks. Gepotidacin has been observed to sit on the twofold axis of the complex, midway between the two four-base-pair separated DNA-cleavage sites and has been observed to stabilize singe-stranded DNA breaks. Here, we use information from three crystal structures of complexes of Staphlococcus aureus DNA gyrase (one with a precursor of gepotidacin and one with the progenitor of zoliflodacin) to propose a simple single moving metal-ion-catalyzed DNA-cleavage mechanism. Our model explains why the catalytic tyrosine is in the tyrosinate (negatively charged) form for DNA cleavage. Movement of a single catalytic metal-ion (Mg 2+ or Mn 2+ ) guides water-mediated protonation and cleavage of the scissile phosphate, which is then accepted by the catalytic tyrosinate. Type IIA topoisomerases need to be able to rapidly cut the DNA when it becomes positively supercoiled (in front of replication forks and transcription bubbles) and we propose that the original purpose of the small Greek Key domain, common to all type IIA topoisomerases, was to allow access of the catalytic metal to the DNA-cleavage site. Although the proposed mechanism is consistent with published data, it is not proven and other mechanisms have been proposed. Finally, how such mechanisms can be experimentally distinguished is considered.

Published

2024

2. How Do Gepotidacin and Zoliflodacin Stabilize DNA Cleavage Complexes with Bacterial Type IIA Topoisomerases? 1. Experimental Definition of Metal Binding Sites.

Author

Morgan H, Nicholls RA, Warren AJ, Ward SE, Evans G, Long F, Murshudov GN, Duman R, and Bax BD

Subjects

Binding Sites, Crystallography, X-Ray, Oxazolidinones chemistry, Oxazolidinones metabolism, Staphylococcus aureus enzymology, Topoisomerase II Inhibitors chemistry, Acenaphthenes chemistry, Acenaphthenes metabolism, Models, Molecular, Manganese metabolism, Manganese chemistry, Heterocyclic Compounds, 3-Ring, DNA Topoisomerases, Type II metabolism, DNA Topoisomerases, Type II chemistry, DNA Cleavage

Abstract

One of the challenges for experimental structural biology in the 21st century is to see chemical reactions happen. Staphylococcus aureus ( S. aureus ) DNA gyrase is a type IIA topoisomerase that can create temporary double-stranded DNA breaks to regulate DNA topology. Drugs, such as gepotidacin, zoliflodacin and the quinolone moxifloxacin, can stabilize these normally transient DNA strand breaks and kill bacteria. Crystal structures of uncleaved DNA with a gepotidacin precursor (2.1 Å GSK2999423) or with doubly cleaved DNA and zoliflodacin (or with its progenitor QPT-1) have been solved in the same P6 1 space-group (a = b ≈ 93 Å, c ≈ 412 Å). This suggests that it may be possible to observe the two DNA cleavage steps (and two DNA-religation steps) in this P6 1 space-group. Here, a 2.58 Å anomalous manganese dataset in this crystal form is solved, and four previous crystal structures (1.98 Å, 2.1 Å, 2.5 Å and 2.65 Å) in this crystal form are re-refined to clarify crystal contacts. The structures clearly suggest a single moving metal mechanism-presented in an accompanying (second) paper. A previously published 2.98 Å structure of a yeast topoisomerase II, which has static disorder around a crystallographic twofold axis, was published as containing two metals at one active site. Re-refined coordinates of this 2.98 Å yeast structure are consistent with other type IIA topoisomerase structures in only having one metal ion at each of the two different active sites.

Published

2024

3. A 2.8 Å Structure of Zoliflodacin in a DNA Cleavage Complex with Staphylococcus aureus DNA Gyrase.

Author

Morgan H, Lipka-Lloyd M, Warren AJ, Hughes N, Holmes J, Burton NP, Mahenthiralingam E, and Bax BD

Subjects

Humans, DNA Gyrase metabolism, Staphylococcus aureus metabolism, DNA Topoisomerase IV genetics, DNA Cleavage, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents chemistry, Fluoroquinolones, Topoisomerase II Inhibitors pharmacology, Bacteria metabolism, Microbial Sensitivity Tests, DNA Topoisomerases, Type II metabolism, Quinolones pharmacology, Staphylococcal Infections

Abstract

Since 2000, some thirteen quinolones and fluoroquinolones have been developed and have come to market. The quinolones, one of the most successful classes of antibacterial drugs, stabilize DNA cleavage complexes with DNA gyrase and topoisomerase IV (topo IV), the two bacterial type IIA topoisomerases. The dual targeting of gyrase and topo IV helps decrease the likelihood of resistance developing. Here, we report on a 2.8 Å X-ray crystal structure, which shows that zoliflodacin, a spiropyrimidinetrione antibiotic, binds in the same DNA cleavage site(s) as quinolones, sterically blocking DNA religation. The structure shows that zoliflodacin interacts with highly conserved residues on GyrB (and does not use the quinolone water-metal ion bridge to GyrA), suggesting it may be more difficult for bacteria to develop target mediated resistance. We show that zoliflodacin has an MIC of 4 µg/mL against Acinetobacter baumannii ( A. baumannii ), an improvement of four-fold over its progenitor QPT-1. The current phase III clinical trial of zoliflodacin for gonorrhea is due to be read out in 2023. Zoliflodacin, together with the unrelated novel bacterial topoisomerase inhibitor gepotidacin, is likely to become the first entirely novel chemical entities approved against Gram-negative bacteria in the 21st century. Zoliflodacin may also become the progenitor of a new safer class of antibacterial drugs against other problematic Gram-negative bacteria.

Published

2023

4. Oligonucleotide-Recognizing Topoisomerase Inhibitors (OTIs): Precision Gene Editors for Neurodegenerative Diseases?

Author

Bax BD, Sutormin D, McDonald NQ, Burley GA, and Shelkovnikova T

Subjects

DNA metabolism, DNA Topoisomerases, Type I genetics, DNA Topoisomerases, Type I metabolism, DNA Topoisomerases, Type II metabolism, DNA, Superhelical, Humans, Imidazoles, Nylons, Pyrroles, Topoisomerase I Inhibitors pharmacology, Topoisomerase II Inhibitors, Topoisomerase Inhibitors pharmacology, Topoisomerase Inhibitors therapeutic use, Neurodegenerative Diseases drug therapy, Neurodegenerative Diseases genetics, Oligonucleotides chemistry

Abstract

Topoisomerases are essential enzymes that recognize and modify the topology of DNA to allow DNA replication and transcription to take place. Topoisomerases are divided into type I topoisomerases, that cleave one DNA strand to modify DNA topology, and type II, that cleave both DNA strands. Topoisomerases normally rapidly religate cleaved-DNA once the topology has been modified. Topoisomerases do not recognize specific DNA sequences, but actively cleave positively supercoiled DNA ahead of transcription bubbles or replication forks, and negative supercoils (or precatenanes) behind, thus allowing the unwinding of the DNA-helix to proceed (during both transcription and replication). Drugs that stabilize DNA-cleavage complexes with topoisomerases produce cytotoxic DNA damage and kill fast-dividing cells; they are widely used in cancer chemotherapy. Oligonucleotide-recognizing topoisomerase inhibitors (OTIs) have given drugs that stabilize DNA-cleavage complexes specificity by linking them to either: (i) DNA duplex recognizing triplex forming oligonucleotide (TFO-OTIs) or DNA duplex recognizing pyrrole-imidazole-polyamides (PIP-OTIs) (ii) or by conventional Watson-Crick base pairing (WC-OTIs). This converts compounds from indiscriminate DNA-damaging drugs to highly specific targeted DNA-cleaving OTIs. Herein we propose simple strategies to enable DNA-duplex strand invasion of WC-OTIs giving strand-invading SI-OTIs. This will make SI-OTIs similar to the guide RNAs of CRISPR/Cas9 nuclease bacterial immune systems. However, an important difference between OTIs and CRISPR/Cas9, is that OTIs do not require the introduction of foreign proteins into cells. Recent successful oligonucleotide therapeutics for neurodegenerative diseases suggest that OTIs can be developed to be highly specific gene editing agents for DNA lesions that cause neurodegenerative diseases.

Published

2022

5. Tyrosine 121 moves revealing a ligandable pocket that couples catalysis to ATP-binding in serine racemase.

Author

Koulouris CR, Gardiner SE, Harris TK, Elvers KT, Mark Roe S, Gillespie JA, Ward SE, Grubisha O, Nicholls RA, Atack JR, and Bax BD

Subjects

Adenosine Triphosphate chemistry, Animals, Catalysis, Serine, Racemases and Epimerases genetics, Tyrosine

Abstract

Human serine racemase (hSR) catalyses racemisation of L-serine to D-serine, the latter of which is a co-agonist of the NMDA subtype of glutamate receptors that are important in synaptic plasticity, learning and memory. In a 'closed' hSR structure containing the allosteric activator ATP, the inhibitor malonate is enclosed between the large and small domains while ATP is distal to the active site, residing at the dimer interface with the Tyr121 hydroxyl group contacting the α-phosphate of ATP. In contrast, in 'open' hSR structures, Tyr121 sits in the core of the small domain with its hydroxyl contacting the key catalytic residue Ser84. The ability to regulate SR activity by flipping Tyr121 from the core of the small domain to the dimer interface appears to have evolved in animals with a CNS. Multiple X-ray crystallographic enzyme-fragment structures show Tyr121 flipped out of its pocket in the core of the small domain. Data suggest that this ligandable pocket could be targeted by molecules that inhibit enzyme activity., (© 2022. The Author(s).)

Published

2022

6. Structures of the Human SPAK and OSR1 Conserved C-Terminal (CCT) Domains.

Author

Elvers KT, Lipka-Lloyd M, Trueman RC, Bax BD, and Mehellou Y

Subjects

Crystallography, X-Ray, Humans, Models, Molecular, Protein Domains, Protein Serine-Threonine Kinases metabolism, Protein Serine-Threonine Kinases chemistry

Abstract

STE20/SPS1-related proline/alanine-rich kinase (SPAK) and oxidative stress responsive 1 (OSR1) kinase are two serine/threonine protein kinases that regulate the function of ion co-transporters through phosphorylation. The highly conserved C-terminal (CCT) domains of SPAK and OSR1 bind to RFx[V/I] peptide sequences from their upstream 'With No Lysine Kinases (WNKs), facilitating their activation via phosphorylation. Thus, the inhibition of SPAK and OSR1 binding, via their CCT domains, to WNK kinases is a plausible strategy for inhibiting SPAK and OSR1 kinases. To facilitate structure-guided drug design of such inhibitors, we expressed and purified human SPAK and OSR1 CCT domains and solved their crystal structures. Interestingly, these crystal structures show a highly conserved primary pocket adjacent to a flexible secondary pocket. We also employed a biophysical strategy and determined the affinity of SPAK and OSR1 CCT domains to short peptides derived from WNK4 and NKCC1. Together, this work provides a platform that facilitates the design of CCT domain specific small molecule binders that inhibit SPAK- and OSR1-activation by WNK kinases, and these could be useful in treating hypertension and ischemic stroke., (© 2021 Wiley-VCH GmbH.)

Published

2022

7. Crystallization and structure of ebselen bound to Cys141 of human inositol monophosphatase.

Author

Fenn GD, Waller-Evans H, Atack JR, and Bax BD

Subjects

Cysteine chemistry, Humans, Isoindoles, Protein Binding, Protein Conformation, Protein Domains, Antioxidants metabolism, Azoles metabolism, Crystallography, X-Ray methods, Cysteine metabolism, Organoselenium Compounds metabolism, Ubiquitin-Protein Ligases chemistry, Ubiquitin-Protein Ligases metabolism

Abstract

Inositol monophosphatase (IMPase) is inhibited by lithium, which is the most efficacious treatment for bipolar disorder. Several therapies have been approved, or are going through clinical trials, aimed at the replacement of lithium in the treatment of bipolar disorder. One candidate small molecule is ebselen, a selenium-containing antioxidant, which has been demonstrated to produce lithium-like effects both in a murine model and in clinical trials. Here, the crystallization and the first structure of human IMPase covalently complexed with ebselen, a 1.47 Å resolution crystal structure (PDB entry 6zk0), are presented. In the complex with human IMPase, ebselen in a ring-opened conformation is covalently attached to Cys141, a residue located away from the active site. IMPase is a dimeric enzyme and in the crystal structure two adjacent dimers share four ebselen molecules, creating a tetramer with approximate 222 symmetry. In the crystal structure presented in this publication, the active site in the tetramer is still accessible, suggesting that ebselen may function as an allosteric inhibitor or may block the binding of partner proteins., (open access.)

Published

2020

8. Conformational flexibility within the small domain of human serine racemase.

Author

Koulouris CR, Bax BD, Atack JR, and Roe SM

Subjects

Amino Acid Sequence, Catalytic Domain, Crystallography, X-Ray, Humans, Models, Molecular, Protein Domains, Protein Conformation, Racemases and Epimerases chemistry, Serine chemistry

Abstract

Serine racemase (SR) is a pyridoxal 5'-phosphate (PLP)-containing enzyme that converts L-serine to D-serine, an endogenous co-agonist for the N-methyl-D-aspartate receptor (NMDAR) subtype of glutamate ion channels. SR regulates D-serine levels by the reversible racemization of L-serine to D-serine, as well as the catabolism of serine by α,β-elimination to produce pyruvate. The modulation of SR activity is therefore an attractive therapeutic approach to disorders associated with abnormal glutamatergic signalling since it allows an indirect modulation of NMDAR function. In the present study, a 1.89 Å resolution crystal structure of the human SR holoenzyme (including the PLP cofactor) with four subunits in the asymmetric unit is described. Comparison of this new structure with the crystal structure of human SR with malonate (PDB entry 3l6b) shows an interdomain cleft that is open in the holo structure but which disappears when the inhibitor malonate binds and is enclosed. This is owing to a shift of the small domain (residues 78-155) in human SR similar to that previously described for the rat enzyme. This domain movement is accompanied by changes within the twist of the central four-stranded β-sheet of the small domain, including changes in the φ-ψ angles of all three residues in the C-terminal β-strand (residues 149-151). In the malonate-bound structure, Ser84 (a catalytic residue) points its side chain at the malonate and is preceded by a six-residue β-strand (residues 78-83), but in the holoenzyme the β-strand is only four residues (78-81) and His82 has φ-ψ values in the α-helical region of the Ramachandran plot. These data therefore represent a crystallographic platform that enables the structure-guided design of small-molecule modulators for this important but to date undrugged target.

Published

2020

9. DNA Topoisomerase Inhibitors: Trapping a DNA-Cleaving Machine in Motion.

Author

Bax BD, Murshudov G, Maxwell A, and Germe T

Subjects

Catalytic Domain, DNA metabolism, DNA Gyrase chemistry, DNA Gyrase genetics, DNA Topoisomerases, Type I chemistry, DNA Topoisomerases, Type II chemistry, DNA Topoisomerases, Type II drug effects, Fluoroquinolones pharmacology, Metals, Models, Molecular, Protein Conformation, Quinolones, Staphylococcus aureus enzymology, Topoisomerase II Inhibitors pharmacology, Anti-Bacterial Agents pharmacology, DNA chemistry, DNA Cleavage drug effects, DNA Topoisomerases, Type I drug effects, Topoisomerase Inhibitors pharmacology

Abstract

Type II topoisomerases regulate DNA topology by making a double-stranded break in one DNA duplex, transporting another DNA segment through this break and then resealing it. Bacterial type IIA topoisomerase inhibitors, such as fluoroquinolones and novel bacterial topoisomerase inhibitors, can trap DNA cleavage complexes with double- or single-stranded cleaved DNA. To study the mode of action of such compounds, 21 crystal structures of a "gyrase CORE " fusion truncate of Staphyloccocus aureus DNA gyrase complexed with DNA and diverse inhibitors have been published, as well as 4 structures lacking inhibitors. These structures have the DNA in various cleavage states and appear to track trajectories along the catalytic paths of the DNA cleavage/religation steps. The various conformations sampled by these multiple "gyrase CORE " structures show rigid body movements of the catalytic GyrA WHD and GyrB TOPRIM domains across the dimer interface. Conformational changes common to all compound-bound structures suggest common mechanisms for DNA cleavage-stabilizing compounds. The structures suggest that S. aureus gyrase uses a single moving-metal ion for cleavage and that the central four base pairs need to be stretched between the two catalytic sites, in order for a scissile phosphate to attract a metal ion to the A-site to catalyze cleavage, after which it is "stored" in another coordination configuration (B-site) in the vicinity. We present a simplified model for the catalytic cycle in which capture of the transported DNA segment causes conformational changes in the ATPase domain that push the DNA gate open, resulting in stretching and cleaving the gate-DNA in two steps., (Copyright © 2019 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2019

10. Structure-guided design of antibacterials that allosterically inhibit DNA gyrase.

Author

Thalji RK, Raha K, Andreotti D, Checchia A, Cui H, Meneghelli G, Profeta R, Tonelli F, Tommasi S, Bakshi T, Donovan BT, Howells A, Jain S, Nixon C, Quinque G, McCloskey L, Bax BD, Neu M, Chan PF, and Stavenger RA

Subjects

Animals, Anti-Bacterial Agents chemical synthesis, Anti-Bacterial Agents chemistry, Cell Line, Crystallography, X-Ray, Dose-Response Relationship, Drug, Humans, Mice, Mice, Knockout, Microbial Sensitivity Tests, Models, Molecular, Molecular Structure, Structure-Activity Relationship, Topoisomerase II Inhibitors chemical synthesis, Topoisomerase II Inhibitors chemistry, Acinetobacter baumannii drug effects, Anti-Bacterial Agents pharmacology, DNA Gyrase metabolism, Drug Design, Escherichia coli drug effects, Topoisomerase II Inhibitors pharmacology

Abstract

A series of DNA gyrase inhibitors were designed based on the X-ray structure of a parent thiophene scaffold with the objective to improve biochemical and whole-cell antibacterial activity, while reducing cardiac ion channel activity. The binding mode and overall design hypothesis of one series was confirmed with a co-crystal structure with DNA gyrase. Although some analogs retained both biochemical activity and whole-cell antibacterial activity, we were unable to significantly improve the activity of the series and analogs retained activity against the cardiac ion channels, therefore we stopped optimization efforts., (Copyright © 2019. Published by Elsevier Ltd.)

Published

2019

11. A new class of antibacterials, the imidazopyrazinones, reveal structural transitions involved in DNA gyrase poisoning and mechanisms of resistance.

Author

Germe T, Vörös J, Jeannot F, Taillier T, Stavenger RA, Bacqué E, Maxwell A, and Bax BD

Subjects

Adenosine Triphosphate metabolism, Anti-Bacterial Agents classification, Ciprofloxacin chemistry, DNA chemistry, DNA Cleavage, DNA Gyrase metabolism, Drug Resistance, Bacterial, Fluoroquinolones chemistry, Magnesium chemistry, Models, Molecular, Mutation, Anti-Bacterial Agents chemistry, DNA Gyrase chemistry, Pyrazines chemistry, Topoisomerase II Inhibitors chemistry

Abstract

Imidazopyrazinones (IPYs) are a new class of compounds that target bacterial topoisomerases as a basis for their antibacterial activity. We have characterized the mechanism of these compounds through structural/mechanistic studies showing they bind and stabilize a cleavage complex between DNA gyrase and DNA ('poisoning') in an analogous fashion to fluoroquinolones, but without the requirement for the water-metal-ion bridge. Biochemical experiments and structural studies of cleavage complexes of IPYs compared with an uncleaved gyrase-DNA complex, reveal conformational transitions coupled to DNA cleavage at the DNA gate. These involve movement at the GyrA interface and tilting of the TOPRIM domains toward the scissile phosphate coupled to capture of the catalytic metal ion. Our experiments show that these structural transitions are involved generally in poisoning of gyrase by therapeutic compounds and resemble those undergone by the enzyme during its adenosine triphosphate-coupled strand-passage cycle. In addition to resistance mutations affecting residues that directly interact with the compounds, we characterized a mutant (D82N) that inhibits formation of the cleavage complex by the unpoisoned enzyme. The D82N mutant appears to act by stabilizing the binary conformation of DNA gyrase with uncleaved DNA without direct interaction with the compounds. This provides general insight into the resistance mechanisms to antibiotics targeting bacterial type II topoisomerases.

Published

2018

12. A new class of antibacterials, the imidazopyrazinones, reveal structural transitions involved in DNA gyrase poisoning and mechanisms of resistance.

Author

Germe T, Vörös J, Jeannot F, Taillier T, Stavenger RA, Bacqué E, Maxwell A, and Bax BD

Published

2018

13. From PIM1 to PI3Kδ via GSK3β: Target Hopping through the Kinome.

Author

Henley ZA, Bax BD, Inglesby LM, Champigny A, Gaines S, Faulder P, Le J, Thomas DA, Washio Y, and Baldwin IR

Abstract

Selective inhibitors of phosphoinositide 3-kinase delta are of interest for the treatment of inflammatory diseases. Initial optimization of a 3-substituted indazole hit compound targeting the kinase PIM1 focused on improving selectivity over GSK3β through consideration of differences in the ATP binding pockets. Continued kinase cross-screening showed PI3Kδ activity in a series of 4,6-disubstituted indazole compounds, and subsequent structure-activity relationship exploration led to the discovery of an indole-containing lead compound as a potent PI3Kδ inhibitor with selectivity over the other PI3K isoforms.

Published

2017

14. Thiophene antibacterials that allosterically stabilize DNA-cleavage complexes with DNA gyrase.

Author

Chan PF, Germe T, Bax BD, Huang J, Thalji RK, Bacqué E, Checchia A, Chen D, Cui H, Ding X, Ingraham K, McCloskey L, Raha K, Srikannathasan V, Maxwell A, and Stavenger RA

Subjects

Crystallography, X-Ray, Drug Discovery, Models, Molecular, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents metabolism, DNA Cleavage, DNA Gyrase chemistry, DNA Gyrase metabolism, Thiophenes chemistry, Thiophenes metabolism

Abstract

A paucity of novel acting antibacterials is in development to treat the rising threat of antimicrobial resistance, particularly in Gram-negative hospital pathogens, which has led to renewed efforts in antibiotic drug discovery. Fluoroquinolones are broad-spectrum antibacterials that target DNA gyrase by stabilizing DNA-cleavage complexes, but their clinical utility has been compromised by resistance. We have identified a class of antibacterial thiophenes that target DNA gyrase with a unique mechanism of action and have activity against a range of bacterial pathogens, including strains resistant to fluoroquinolones. Although fluoroquinolones stabilize double-stranded DNA breaks, the antibacterial thiophenes stabilize gyrase-mediated DNA-cleavage complexes in either one DNA strand or both DNA strands. X-ray crystallography of DNA gyrase-DNA complexes shows the compounds binding to a protein pocket between the winged helix domain and topoisomerase-primase domain, remote from the DNA. Mutations of conserved residues around this pocket affect activity of the thiophene inhibitors, consistent with allosteric inhibition of DNA gyrase. This druggable pocket provides potentially complementary opportunities for targeting bacterial topoisomerases for antibiotic development., Competing Interests: The authors declare no conflict of interest.

Published

2017

15. Structural basis of DNA gyrase inhibition by antibacterial QPT-1, anticancer drug etoposide and moxifloxacin.

Author

Chan PF, Srikannathasan V, Huang J, Cui H, Fosberry AP, Gu M, Hann MM, Hibbs M, Homes P, Ingraham K, Pizzollo J, Shen C, Shillings AJ, Spitzfaden CE, Tanner R, Theobald AJ, Stavenger RA, Bax BD, and Gwynn MN

Subjects

Anti-Bacterial Agents pharmacology, Antineoplastic Agents pharmacology, DNA Gyrase genetics, DNA Gyrase metabolism, DNA, Bacterial chemistry, DNA, Bacterial genetics, DNA, Bacterial metabolism, Drug Resistance, Bacterial, Etoposide pharmacology, Fluoroquinolones pharmacology, Models, Molecular, Molecular Structure, Moxifloxacin, Staphylococcus aureus chemistry, Staphylococcus aureus drug effects, Topoisomerase II Inhibitors pharmacology, Anti-Bacterial Agents chemistry, Antineoplastic Agents chemistry, DNA Gyrase chemistry, Etoposide chemistry, Fluoroquinolones chemistry, Staphylococcus aureus enzymology, Topoisomerase II Inhibitors chemistry

Abstract

New antibacterials are needed to tackle antibiotic-resistant bacteria. Type IIA topoisomerases (topo2As), the targets of fluoroquinolones, regulate DNA topology by creating transient double-strand DNA breaks. Here we report the first co-crystal structures of the antibacterial QPT-1 and the anticancer drug etoposide with Staphylococcus aureus DNA gyrase, showing binding at the same sites in the cleaved DNA as the fluoroquinolone moxifloxacin. Unlike moxifloxacin, QPT-1 and etoposide interact with conserved GyrB TOPRIM residues rationalizing why QPT-1 can overcome fluoroquinolone resistance. Our data show etoposide's antibacterial activity is due to DNA gyrase inhibition and suggests other anticancer agents act similarly. Analysis of multiple DNA gyrase co-crystal structures, including asymmetric cleavage complexes, led to a 'pair of swing-doors' hypothesis in which the movement of one DNA segment regulates cleavage and religation of the second DNA duplex. This mechanism can explain QPT-1's bacterial specificity. Structure-based strategies for developing topo2A antibacterials are suggested.

Published

2015

16. Crystallization and initial crystallographic analysis of covalent DNA-cleavage complexes of Staphyloccocus aureus DNA gyrase with QPT-1, moxifloxacin and etoposide.

Author

Srikannathasan V, Wohlkonig A, Shillings A, Singh O, Chan PF, Huang J, Gwynn MN, Fosberry AP, Homes P, Hibbs M, Theobald AJ, Spitzfaden C, and Bax BD

Subjects

Base Sequence, Crystallization, Crystallography, X-Ray, Molecular Sequence Data, Moxifloxacin, DNA Cleavage, DNA Gyrase chemistry, Etoposide chemistry, Fluoroquinolones chemistry, Heterocyclic Compounds, 4 or More Rings chemistry, Spiro Compounds chemistry, Staphylococcus aureus enzymology

Abstract

Fluoroquinolone drugs such as moxifloxacin kill bacteria by stabilizing the normally transient double-stranded DNA breaks created by bacterial type IIA topoisomerases. Previous crystal structures of Staphylococcus aureus DNA gyrase with asymmetric DNAs have had static disorder (with the DNA duplex observed in two orientations related by the pseudo-twofold axis of the complex). Here, 20-base-pair DNA homoduplexes were used to obtain crystals of covalent DNA-cleavage complexes of S. aureus DNA gyrase. Crystals with QPT-1, moxifloxacin or etoposide diffracted to between 2.45 and 3.15 Å resolution. A G/T mismatch introduced at the ends of the DNA duplexes facilitated the crystallization of slightly asymmetric complexes of the inherently flexible DNA-cleavage complexes.

Published

2015

17. Protein arginine deiminase 2 binds calcium in an ordered fashion: implications for inhibitor design.

Author

Slade DJ, Fang P, Dreyton CJ, Zhang Y, Fuhrmann J, Rempel D, Bax BD, Coonrod SA, Lewis HD, Guo M, Gross ML, and Thompson PR

Subjects

Amino Acid Sequence, Benzimidazoles chemistry, Benzimidazoles pharmacology, Catalytic Domain, Crystallography, X-Ray, Cysteine chemistry, Cysteine metabolism, Deuterium Exchange Measurement, Enzyme Activation, Enzyme Inhibitors chemistry, Humans, Hydrolases antagonists & inhibitors, Molecular Docking Simulation, Molecular Sequence Data, Protein Conformation, Protein-Arginine Deiminase Type 2, Protein-Arginine Deiminases, Calcium metabolism, Hydrolases chemistry, Hydrolases metabolism

Abstract

Protein arginine deiminases (PADs) are calcium-dependent histone-modifying enzymes whose activity is dysregulated in inflammatory diseases and cancer. PAD2 functions as an Estrogen Receptor (ER) coactivator in breast cancer cells via the citrullination of histone tail arginine residues at ER binding sites. Although an attractive therapeutic target, the mechanisms that regulate PAD2 activity are largely unknown, especially the detailed role of how calcium facilitates enzyme activation. To gain insights into these regulatory processes, we determined the first structures of PAD2 (27 in total), and through calcium-titrations by X-ray crystallography, determined the order of binding and affinity for the six calcium ions that bind and activate this enzyme. These structures also identified several PAD2 regulatory elements, including a calcium switch that controls proper positioning of the catalytic cysteine residue, and a novel active site shielding mechanism. Additional biochemical and mass-spectrometry-based hydrogen/deuterium exchange studies support these structural findings. The identification of multiple intermediate calcium-bound structures along the PAD2 activation pathway provides critical insights that will aid the development of allosteric inhibitors targeting the PADs.

Published

2015

18. Inhibition of PAD4 activity is sufficient to disrupt mouse and human NET formation.

Author

Lewis HD, Liddle J, Coote JE, Atkinson SJ, Barker MD, Bax BD, Bicker KL, Bingham RP, Campbell M, Chen YH, Chung CW, Craggs PD, Davis RP, Eberhard D, Joberty G, Lind KE, Locke K, Maller C, Martinod K, Patten C, Polyakova O, Rise CE, Rüdiger M, Sheppard RJ, Slade DJ, Thomas P, Thorpe J, Yao G, Drewes G, Wagner DD, Thompson PR, Prinjha RK, and Wilson DM

Subjects

Animals, Benzimidazoles chemical synthesis, Binding, Competitive, Calcium metabolism, Citrulline metabolism, Enzyme Inhibitors chemical synthesis, HEK293 Cells, Histones metabolism, Humans, In Vitro Techniques, Mice, Models, Molecular, Protein-Arginine Deiminase Type 4, Protein-Arginine Deiminases, Small Molecule Libraries, Substrate Specificity, Benzimidazoles pharmacology, Enzyme Inhibitors pharmacology, Hydrolases antagonists & inhibitors, Neutrophils drug effects

Abstract

PAD4 has been strongly implicated in the pathogenesis of autoimmune, cardiovascular and oncological diseases through clinical genetics and gene disruption in mice. New selective PAD4 inhibitors binding a calcium-deficient form of the PAD4 enzyme have validated the critical enzymatic role of human and mouse PAD4 in both histone citrullination and neutrophil extracellular trap formation for, to our knowledge, the first time. The therapeutic potential of PAD4 inhibitors can now be explored.

Published

2015

19. Crystallizing Membrane Proteins in the Lipidic Mesophase. Experience with Human Prostaglandin E2 Synthase 1 and an Evolving Strategy.

Author

Li D, Howe N, Dukkipati A, Shah ST, Bax BD, Edge C, Bridges A, Hardwicke P, Singh OM, Giblin G, Pautsch A, Pfau R, Schnapp G, Wang M, Olieric V, and Caffrey M

Abstract

The lipidic mesophase or in meso method for crystallizing membrane proteins has several high profile targets to its credit and is growing in popularity. Despite its success, the method is in its infancy as far as rational crystallogenesis is concerned. Consequently, significant time, effort, and resources are still required to generate structure-grade crystals, especially with a new target type. Therefore, a need exists for crystallogenesis protocols that are effective with a broad range of membrane protein types. Recently, a strategy for crystallizing a prokaryotic α-helical membrane protein, diacylglycerol kinase (DgkA), by the in meso method was reported (Cryst. Growth. Des.2013, 14, 2846-2857). Here, we describe its application to the human α-helical microsomal prostaglandin E2 synthase 1 (mPGES1). While the DgkA strategy proved useful, significant modifications were needed to generate structure-quality crystals of this important therapeutic target. These included protein engineering, using an additive phospholipid in the hosting mesophase, performing multiple rounds of salt screening, and carrying out trials at 4 °C in the presence of a tight binding ligand. The crystallization strategy detailed here should prove useful for generating structures of other integral membrane proteins by the in meso method.

Published

2014

20. Purification, crystallization and preliminary X-ray crystallographic studies of the Mycobacterium tuberculosis DNA gyrase ATPase domain.

Author

Roué M, Agrawal A, Volker C, Mossakowska D, Mayer C, and Bax BD

Subjects

Adenosine Triphosphatases isolation & purification, Bacterial Proteins isolation & purification, Crystallization, Crystallography, X-Ray, DNA Gyrase isolation & purification, Adenosine Triphosphatases chemistry, Bacterial Proteins chemistry, DNA Gyrase chemistry, Mycobacterium tuberculosis enzymology

Abstract

Mycobacterium tuberculosis DNA gyrase, a nanomachine involved in the regulation of DNA topology, is the only type II topoisomerase present in this organism and hence is the sole target of fluoroquinolones in the treatment of tuberculosis. The ATPase domain provides the energy required for catalysis by ATP hydrolysis. Two constructs corresponding to this 43 kDa domain, Mtb-GyrB47(C1) and Mtb-GyrB47(C2), have been overproduced, purified and crystallized. Diffraction data were collected from three crystal forms. The crystals belonged to space groups P1 and P21 and diffracted to resolutions of 2.9 and 3.3 Å, respectively.

Published

2013

21. Integration of lead optimization with crystallography for a membrane-bound ion channel target: discovery of a new class of AMPA receptor positive allosteric modulators.

Author

Ward SE, Harries M, Aldegheri L, Austin NE, Ballantine S, Ballini E, Bradley DM, Bax BD, Clarke BP, Harris AJ, Harrison SA, Melarange RA, Mookherjee C, Mosley J, Dal Negro G, Oliosi B, Smith KJ, Thewlis KM, Woollard PM, and Yusaf SP

Subjects

Allosteric Regulation, Animals, Calcium metabolism, Crystallography, X-Ray, Dogs, High-Throughput Screening Assays, Humans, In Vitro Techniques, Indazoles pharmacokinetics, Indazoles pharmacology, Ligands, Macaca fascicularis, Male, Microsomes, Liver metabolism, Models, Molecular, Molecular Conformation, Patch-Clamp Techniques, Protein Multimerization, Rats, Rats, Sprague-Dawley, Receptors, AMPA chemistry, Recombinant Proteins chemistry, Solubility, Structure-Activity Relationship, Swine, Swine, Miniature, Indazoles chemical synthesis, Receptors, AMPA physiology

Abstract

A novel series of AMPAR positive modulators is described that were identified by high throughput screening. The molecules of the series have been optimized from a high quality starting point hit to afford excellent developability, tolerability, and efficacy profiles, leading to identification of a clinical candidate. Unusually for an ion channel target, this optimization was integrated with regular generation of ligand-bound crystal structures and uncovered a novel chemotype with a unique and highly conserved mode of interaction via a trifluoromethyl group.

Published

2011

22. Structural basis of quinolone inhibition of type IIA topoisomerases and target-mediated resistance.

Author

Wohlkonig A, Chan PF, Fosberry AP, Homes P, Huang J, Kranz M, Leydon VR, Miles TJ, Pearson ND, Perera RL, Shillings AJ, Gwynn MN, and Bax BD

Subjects

DNA Topoisomerase IV pharmacology, Enzyme Inhibitors pharmacology, Models, Molecular, Protein Structure, Quaternary, Protein Structure, Tertiary, Quinolones pharmacology, Acinetobacter baumannii enzymology, DNA Topoisomerase IV chemistry, Enzyme Inhibitors chemistry, Quinolones chemistry

Abstract

Quinolone antibacterials have been used to treat bacterial infections for over 40 years. A crystal structure of moxifloxacin in complex with Acinetobacter baumannii topoisomerase IV now shows the wedge-shaped quinolone stacking between base pairs at the DNA cleavage site and binding conserved residues in the DNA cleavage domain through chelation of a noncatalytic magnesium ion. This provides a molecular basis for the quinolone inhibition mechanism, resistance mutations and invariant quinolone antibacterial structural features.

Published

2010

23. Type IIA topoisomerase inhibition by a new class of antibacterial agents.

Author

Bax BD, Chan PF, Eggleston DS, Fosberry A, Gentry DR, Gorrec F, Giordano I, Hann MM, Hennessy A, Hibbs M, Huang J, Jones E, Jones J, Brown KK, Lewis CJ, May EW, Saunders MR, Singh O, Spitzfaden CE, Shen C, Shillings A, Theobald AJ, Wohlkonig A, Pearson ND, and Gwynn MN

Subjects

Anti-Bacterial Agents metabolism, Apoenzymes chemistry, Apoenzymes metabolism, Arginine metabolism, Aspartic Acid metabolism, Binding Sites, Catalytic Domain, Ciprofloxacin chemistry, Ciprofloxacin metabolism, Crystallography, X-Ray, DNA chemistry, DNA metabolism, DNA Cleavage, DNA Gyrase metabolism, DNA, Superhelical chemistry, DNA, Superhelical metabolism, Drug Design, Drug Resistance, Escherichia coli enzymology, Manganese metabolism, Models, Molecular, Protein Conformation, Quinolines metabolism, Quinolones chemistry, Quinolones metabolism, Structure-Activity Relationship, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents pharmacology, DNA Gyrase chemistry, Quinolines chemistry, Quinolines pharmacology, Staphylococcus aureus enzymology, Topoisomerase II Inhibitors

Abstract

Despite the success of genomics in identifying new essential bacterial genes, there is a lack of sustainable leads in antibacterial drug discovery to address increasing multidrug resistance. Type IIA topoisomerases cleave and religate DNA to regulate DNA topology and are a major class of antibacterial and anticancer drug targets, yet there is no well developed structural basis for understanding drug action. Here we report the 2.1 A crystal structure of a potent, new class, broad-spectrum antibacterial agent in complex with Staphylococcus aureus DNA gyrase and DNA, showing a new mode of inhibition that circumvents fluoroquinolone resistance in this clinically important drug target. The inhibitor 'bridges' the DNA and a transient non-catalytic pocket on the two-fold axis at the GyrA dimer interface, and is close to the active sites and fluoroquinolone binding sites. In the inhibitor complex the active site seems poised to cleave the DNA, with a single metal ion observed between the TOPRIM (topoisomerase/primase) domain and the scissile phosphate. This work provides new insights into the mechanism of topoisomerase action and a platform for structure-based drug design of a new class of antibacterial agents against a clinically proven, but conformationally flexible, enzyme class.

Published

2010

24. Discovery of N-[(2S)-5-(6-fluoro-3-pyridinyl)-2,3-dihydro-1H-inden-2-yl]-2-propanesulfonamide, a novel clinical AMPA receptor positive modulator.

Author

Ward SE, Harries M, Aldegheri L, Andreotti D, Ballantine S, Bax BD, Harris AJ, Harker AJ, Lund J, Melarange R, Mingardi A, Mookherjee C, Mosley J, Neve M, Oliosi B, Profeta R, Smith KJ, Smith PW, Spada S, Thewlis KM, and Yusaf SP

Subjects

Administration, Oral, Allosteric Regulation, Animals, Biological Availability, Blood Proteins metabolism, Blood-Brain Barrier metabolism, Callithrix, Cell Line, Crystallography, X-Ray, Dogs, Humans, Indenes pharmacokinetics, Indenes pharmacology, Macaca fascicularis, Male, Microsomes, Liver metabolism, Models, Molecular, Protein Binding, Protein Structure, Tertiary, Pyridines pharmacokinetics, Pyridines pharmacology, Rats, Rats, Sprague-Dawley, Species Specificity, Stereoisomerism, Structure-Activity Relationship, Sulfonamides pharmacokinetics, Sulfonamides pharmacology, Indenes chemical synthesis, Pyridines chemical synthesis, Receptors, AMPA physiology, Sulfonamides chemical synthesis

Abstract

A series of AMPA receptor positive allosteric modulators has been optimized from poorly penetrant leads to identify molecules with excellent preclinical pharmacokinetics and CNS penetration. These discoveries led to 17i, a potent, efficacious CNS penetrant molecule with an excellent pharmacokinetic profile across preclinical species, which is well tolerated and is also orally bioavailable in humans.

Published

2010

25. Challenges for and current status of research into positive modulators of AMPA receptors.

Author

Ward SE, Bax BD, and Harries M

Subjects

Allosteric Regulation, Animals, Crystallography, X-Ray methods, High-Throughput Screening Assays, Humans, Protein Subunits, Receptors, AMPA metabolism, Structure-Activity Relationship, Drug Delivery Systems, Drug Design, Receptors, AMPA drug effects

Abstract

AMPA receptors consist of a family of hetero-oligomeric (tetrameric) receptors arising from four genes, each of which encodes a distinct receptor subunit (GluA1-4). Recombinant homo-tetrameric AMPA receptors, comprising four identical subunits, are functionally active and have been used in in vitro assays. However, the many different subunit permutations make possible the functional and anatomical diversity of AMPA receptors throughout the CNS. Furthermore, AMPA receptor subunit stoichiometry influences the biophysical and functional properties of the receptor. A number of chemically diverse positive modulators of AMPA receptor have been identified which potentiate AMPA receptor-mediated activity in vitro as well as improving cognitive performance in rodents and non-human primates with several being taken further in the clinic. This review article summarizes the current status in the research on positive allosteric modulation of AMPA receptors and outlines the challenges involved in identifying a chemically distinct series of AMPA receptor positive modulators, addressing the challenges created by the heterogeneity of the AMPA receptor populations and the development of structure-activity relationships driven by homomeric, recombinant systems on high-throughput platforms. We also review the role of X-ray crystallography in the selection and prioritization of targets for lead optimization for AMPA receptor positive modulators.

Published

2010

26. 1-Aryl-3,4-dihydroisoquinoline inhibitors of JNK3.

Author

Christopher JA, Atkinson FL, Bax BD, Brown MJ, Champigny AC, Chuang TT, Jones EJ, Mosley JE, and Musgrave JR

Subjects

Binding Sites physiology, Fluorescence Polarization methods, Humans, Isoquinolines metabolism, Isoquinolines pharmacology, Mitogen-Activated Protein Kinase 10 metabolism, Mitogen-Activated Protein Kinase 14 antagonists & inhibitors, Mitogen-Activated Protein Kinase 14 metabolism, Mitogen-Activated Protein Kinase 8 antagonists & inhibitors, Mitogen-Activated Protein Kinase 8 metabolism, Protein Kinase Inhibitors metabolism, Protein Kinase Inhibitors pharmacology, Isoquinolines chemical synthesis, Mitogen-Activated Protein Kinase 10 antagonists & inhibitors, Protein Kinase Inhibitors chemical synthesis

Abstract

A series of 1-aryl-3,4-dihydroisoquinoline inhibitors of JNK3 are described. Compounds 20 and 24 are the most potent inhibitors (pIC50 7.3 and 6.9, respectively in a radiometric filter binding assay), with 10- and 1000-fold selectivity over JNK2 and JNK1, respectively, and selectivity within the wider mitogen-activated protein kinase (MAPK) family against p38alpha and ERK2. X-ray crystallography of 16 reveals a highly unusual binding mode where an H-bond acceptor interaction with the hinge region is made by a chloro substituent.

Published

2009

27. Nerve growth factor alpha subunit: effect of site-directed mutations on catalytic activity and 7S NGF complex formation.

Author

Yarski MA, Bax BD, Hogue-Angeletti RA, and Bradshaw RA

Subjects

Amino Acid Sequence, Animals, Catalysis, Cell Line, Chromatography, Gel, Enzyme Precursors chemistry, Humans, Mass Spectrometry, Mice, Models, Molecular, Molecular Sequence Data, Mutagenesis, Site-Directed, Mutation, Nerve Growth Factor biosynthesis, Nerve Growth Factor genetics, Nerve Growth Factors chemistry, Plasmids, Protein Conformation, Recombinant Proteins chemistry, Submandibular Gland enzymology, Endopeptidases chemistry, Nerve Growth Factor chemistry

Abstract

Mouse alpha- and gamma-nerve growth factor (NGF) are glandular kallikreins that form a non-covalent complex (7S NGF) with beta-NGF. gamma-NGF is an active arginine-specific esteropeptidase; the alpha-subunit is catalytically inactive and has a zymogen-like conformation. Site-directed mutagenesis of alpha-NGF to alter the N-terminus and three residues in loop 7, a region that contributes to the catalytic center, restored substantial catalytic activity against N-benzoyl arginine-p-nitroanilide as substrate in two derivatives although they were not as active as recombinant gamma-NGF. Seven of the 15 derivatives that remained more alpha-like were able to substitute for native alpha-NGF in reforming 7S complexes; the other eight derivatives that were more gamma-like showed greatly reduced ability to do so. However, the most gamma-like alpha-NGF derivative could not substitute for native gamma-NGF in 7S complex formation. These findings suggest that the alpha-NGF backbone can be corrected to a functional enzyme by the addition of a normal N-terminal structure and two catalytic site substitutions and that the 7S complex requires one kallikrein subunit in the zymogen form and one in an active conformation.

Published

2000