Your search keyword '"Nyssa Drinkwater"' showing total 44 results

1. Chemoproteomics validates selective targeting of Plasmodium M1 alanyl aminopeptidase as an antimalarial strategy

Author

Carlo Giannangelo, Matthew P Challis, Ghizal Siddiqui, Rebecca Edgar, Tess R Malcolm, Chaille T Webb, Nyssa Drinkwater, Natalie Vinh, Christopher Macraild, Natalie Counihan, Sandra Duffy, Sergio Wittlin, Shane M Devine, Vicky M Avery, Tania De Koning-Ward, Peter Scammells, Sheena McGowan, and Darren J Creek

Subjects

chemoproteomics, malaria, metabolomics, aminopeptidase, drug target, mass spectrometry, Medicine, Science, Biology (General), QH301-705.5

Abstract

New antimalarial drug candidates that act via novel mechanisms are urgently needed to combat malaria drug resistance. Here, we describe the multi-omic chemical validation of Plasmodium M1 alanyl metalloaminopeptidase as an attractive drug target using the selective inhibitor, MIPS2673. MIPS2673 demonstrated potent inhibition of recombinant Plasmodium falciparum (PfA-M1) and Plasmodium vivax (PvA-M1) M1 metalloaminopeptidases, with selectivity over other Plasmodium and human aminopeptidases, and displayed excellent in vitro antimalarial activity with no significant host cytotoxicity. Orthogonal label-free chemoproteomic methods based on thermal stability and limited proteolysis of whole parasite lysates revealed that MIPS2673 solely targets PfA-M1 in parasites, with limited proteolysis also enabling estimation of the binding site on PfA-M1 to within ~5 Å of that determined by X-ray crystallography. Finally, functional investigation by untargeted metabolomics demonstrated that MIPS2673 inhibits the key role of PfA-M1 in haemoglobin digestion. Combined, our unbiased multi-omic target deconvolution methods confirmed the on-target activity of MIPS2673, and validated selective inhibition of M1 alanyl metalloaminopeptidase as a promising antimalarial strategy.

Published

2024

2. On-target, dual aminopeptidase inhibition provides cross-species antimalarial activity

Author

Rebecca C. S. Edgar, Tess R. Malcolm, Ghizal Siddiqui, Carlo Giannangelo, Natalie A. Counihan, Matthew Challis, Sandra Duffy, Mrittika Chowdhury, Jutta Marfurt, Madeline Dans, Grennady Wirjanata, Rintis Noviyanti, Kajal Daware, Chathura D. Suraweera, Ric N. Price, Sergio Wittlin, Vicky M. Avery, Nyssa Drinkwater, Susan A. Charman, Darren J. Creek, Tania F. de Koning-Ward, Peter J. Scammells, and Sheena McGowan

Subjects

malaria, drug resistance, aminopeptidase, Plasmodium falciparum, Plasmodium vivax, Microbiology, QR1-502

Abstract

ABSTRACT To combat the global burden of malaria, development of new drugs to replace or complement current therapies is urgently required. Here, we show that the compound MMV1557817 is a selective, nanomolar inhibitor of both Plasmodium falciparum and Plasmodium vivax aminopeptidases M1 and M17, leading to inhibition of end-stage hemoglobin digestion in asexual parasites. MMV1557817 can kill sexual-stage P. falciparum, is active against murine malaria, and does not show any shift in activity against a panel of parasites resistant to other antimalarials. MMV1557817-resistant P. falciparum exhibited a slow growth rate that was quickly outcompeted by wild-type parasites and were sensitized to the current clinical drug, artemisinin. Overall, these results confirm MMV1557817 as a lead compound for further drug development and highlights the potential of dual inhibition of M1 and M17 as an effective multi-species drug-targeting strategy.IMPORTANCEEach year, malaria infects approximately 240 million people and causes over 600,000 deaths, mostly in children under 5 years of age. For the past decade, artemisinin-based combination therapies have been recommended by the World Health Organization as the standard malaria treatment worldwide. Their widespread use has led to the development of artemisinin resistance in the form of delayed parasite clearance, alongside the rise of partner drug resistance. There is an urgent need to develop and deploy new antimalarial agents with novel targets and mechanisms of action. Here, we report a new and potent antimalarial compound, known as MMV1557817, and show that it targets multiple stages of the malaria parasite lifecycle, is active in a preliminary mouse malaria model, and has a novel mechanism of action. Excitingly, resistance to MMV15578117 appears to be self-limiting, suggesting that development of the compound may provide a new class of antimalarial.

Published

2024

3. Screening the Medicines for Malaria Venture 'Malaria Box' against the Plasmodium falciparum aminopeptidases, M1, M17 and M18.

Author

Alessandro Paiardini, Rebecca S Bamert, Komagal Kannan-Sivaraman, Nyssa Drinkwater, Shailesh N Mistry, Peter J Scammells, and Sheena McGowan

Subjects

Medicine, Science

Abstract

Malaria is a parasitic disease that remains a global health burden. The ability of the parasite to rapidly develop resistance to therapeutics drives an urgent need for the delivery of new drugs. The Medicines for Malaria Venture have compounds known for their antimalarial activity, but not necessarily the molecular targets. In this study, we assess the ability of the "MMV 400" compounds to inhibit the activity of three metalloaminopeptidases from Plasmodium falciparum, PfA-M1, PfA-M17 and PfM18 AAP. We have developed a multiplex assay system to allow rapid primary screening of compounds against all three metalloaminopeptidases, followed by detailed analysis of promising compounds. Our results show that there were no PfM18AAP inhibitors, whereas two moderate inhibitors of the neutral aminopeptidases PfA-M1 and PfA-M17 were identified. Further investigation through structure-activity relationship studies and molecular docking suggest that these compounds are competitive inhibitors with novel binding mechanisms, acting through either non-classical zinc coordination or independently of zinc binding altogether. Although it is unlikely that inhibition of PfA-M1 and/or PfA-M17 is the primary mechanism responsible for the antiplasmodial activity reported for these compounds, their detailed characterization, as presented in this work, pave the way for their further optimization as a novel class of dual PfA-M1/PfA-M17 inhibitors utilising non-classical zinc binding groups.

Published

2015

4. Identification and Validation of a Potent Dual Inhibitor of the P. falciparum M1 and M17 Aminopeptidases Using Virtual Screening.

Author

Chiara Ruggeri, Nyssa Drinkwater, Komagal Kannan Sivaraman, Rebecca S Bamert, Sheena McGowan, and Alessandro Paiardini

Subjects

Medicine, Science

Abstract

The Plasmodium falciparum PfA-M1 and PfA-M17 metalloaminopeptidases are validated drug targets for the discovery of antimalarial agents. In order to identify dual inhibitors of both proteins, we developed a hierarchical virtual screening approach, followed by in vitro evaluation of the highest scoring hits. Starting from the ZINC database of purchasable compounds, sequential 3D-pharmacophore and molecular docking steps were applied to filter the virtual 'hits'. At the end of virtual screening, 12 compounds were chosen and tested against the in vitro aminopeptidase activity of both PfA-M1 and PfA-M17. Two molecules showed significant inhibitory activity (low micromolar/nanomolar range) against both proteins. Finally, the crystal structure of the most potent compound in complex with both PfA-M1 and PfA-M17 was solved, revealing the binding mode and validating our computational approach.

Published

2015

5. Mapping the substrate specificity of the Plasmodium M1 and M17 aminopeptidases

Author

Tess R. Malcolm, Brooke K Hayes, Chaille T. Webb, Nyssa Drinkwater, Karolina Weronika Swiderska, Marcin Drag, and Sheena McGowan

Subjects

0301 basic medicine, Plasmodium, substrate specificity, Plasmodium berghei, leucine aminopeptidase, Plasmodium falciparum, Plasmodium vivax, Protozoan Proteins, Microbiology, metallo-aminopeptidase, Aminopeptidases, Biochemistry, Mice, 03 medical and health sciences, 0302 clinical medicine, Species Specificity, Leucine, parasitic diseases, Protein biosynthesis, Animals, Humans, Protease Inhibitors, Molecular Biology, Research Articles, chemistry.chemical_classification, alanyl-aminopeptidase, Molecular Interactions, biology, Chemistry, Substrate (chemistry), Cell Biology, biology.organism_classification, Recombinant Proteins, Malaria, Isoenzymes, Kinetics, 030104 developmental biology, Enzyme, 030220 oncology & carcinogenesis, Enzymology, Biocatalysis, Hemoglobin, Peptides

Abstract

During malarial infection, Plasmodium parasites digest human hemoglobin to obtain free amino acids for protein production and maintenance of osmotic pressure. The Plasmodium M1 and M17 aminopeptidases are both postulated to have an essential role in the terminal stages of the hemoglobin digestion process and are validated drug targets for the design of new dual-target anti-malarial compounds. In this study, we profiled the substrate specificity fingerprints and kinetic behaviors of M1 and M17 aminopeptidases from Plasmodium falciparum and Plasmodium vivax, and the mouse model species, Plasmodium berghei. We found that although the Plasmodium M1 aminopeptidases share a largely similar, broad specificity at the P1 position, the P. falciparum M1 displays the greatest diversity in specificity and P. berghei M1 showing a preference for charged P1 residues. In contrast, the Plasmodium M17 aminopeptidases share a highly conserved preference for hydrophobic residues at the P1 position. The aminopeptidases also demonstrated intra-peptide sequence specificity, particularly the M1 aminopeptidases, which showed a definitive preference for peptides with fewer negatively charged intrapeptide residues. Overall, the P. vivax and P. berghei enzymes had a faster substrate turnover rate than the P. falciparum enzymes, which we postulate is due to subtle differences in structural dynamicity. Together, these results build a kinetic profile that allows us to better understand the catalytic nuances of the M1 and M17 aminopeptidases from different Plasmodium species.

Published

2021

6. High avidity drives the interaction between the streptococcal C1 phage endolysin, PlyC, with the cell surface carbohydrates of Group A Streptococcus

Author

James Fodor, Blake T. Riley, Kirill Tsyganov, Anne Geert Volbeda, Daniel C. Nelson, Kylie A Farrow, Brooke K. Hayes, Colin J. Jackson, Sheena McGowan, Sebastian S. Broendum, Ben E. Clifton, Ryan D. Heselpoth, Jeroen D. C. Codée, Felix Kraus, Daniel E. Williams, Nyssa Drinkwater, and Ashley M. Buckle

Subjects

Streptococcus pyogenes, Lysin, Peptidoglycan, Biology, Rhamnose, Microbiology, Group A, Bacteriophage, 03 medical and health sciences, chemistry.chemical_compound, Cell Wall, Endopeptidases, Bacteriophages, Avidity, Binding site, Molecular Biology, 030304 developmental biology, 0303 health sciences, Binding Sites, 030306 microbiology, Cell Membrane, Rhamnose binding, biology.organism_classification, Molecular Docking Simulation, chemistry, Lytic cycle, Protein Binding

Abstract

Endolysin enzymes from bacteriophage cause bacterial lysis by degrading the peptidoglycan cell wall. The streptococcal C1 phage endolysin PlyC, is the most potent endolysin described to date and can rapidly lyse group A, C, and E streptococci. PlyC is known to bind the Group A streptococcal cell wall, but the specific molecular target or the binding site within PlyC remain uncharacterized. Here we report for the first time, that the polyrhamnose backbone of the Group A streptococcal cell wall is the binding target of PlyC. We have also characterized the putative rhamnose binding groove of PlyC and found four key residues that were critical to either the folding or the cell wall binding action of PlyC. Based on our results, we suggest that the interaction between PlyC and the cell wall may not be a high-affinity interaction as previously proposed, but rather a high avidity one, allowing for PlyC's remarkable lytic activity. Resistance to our current antibiotics is reaching crisis levels and there is an urgent need to develop the antibacterial agents with new modes of action. A detailed understanding of this potent endolysin may facilitate future developments of PlyC as a tool against the rise of antibiotic resistance.

Published

2021

7. X-ray crystal structure and specificity of the Toxoplasma gondii ME49 TgAPN2

Author

Emilia M. Marijanovic, Nyssa Drinkwater, Jasmin C Aschenbrenner, James Andersen, Chaille T. Webb, Sheena McGowan, Marcin Drag, and Karolina Weronika Swiderska

Subjects

M1 aminopeptidase, Protozoan Proteins, Toxoplasma gondii, Crystallography, X-Ray, Aminopeptidases, Biochemistry, Aminopeptidase, Structural Biology, medicine, Parasite hosting, metalloproteases, Molecular Biology, Research Articles, chemistry.chemical_classification, Metalloproteinase, biology, Cell Biology, aminopeptidase N, medicine.disease, biology.organism_classification, Virology, Toxoplasmosis, Structure and function, Enzyme, chemistry, Parasitic disease, Enzymology, Parasitology, PfA-M1, Toxoplasma

Abstract

Toxoplasmosis is a parasitic disease caused by infection with Toxoplasma gondii that currently has few therapeutic options. The M1 aminopeptidase enzymes have been shown to be attractive targets for anti-parasitic agents and/or vaccine candidates, suggesting potential to re-purpose inhibitors between parasite M1 aminopeptidase targets. The M1 aminopeptidase TgAPN2 has been suggested to be a potential new drug target for toxoplasmosis. Here we investigate the structure and function of TgAPN2, a homologue of the antimalarial drug target PfA-M1, and evaluate the capacity to use inhibitors that target PfA-M1 against TgAPN2. The results show that despite a similar overall fold, the TgAPN2 has a unique substrate specificity and inhibition profile. Sequence and structure differences are investigated and show how comparative structure-activity relationships may provide a route to obtaining potent inhibitors of TgAPN2.

Published

2020

8. A metal ion-dependent conformational switch modulates activity of the Plasmodium M17 aminopeptidase

Author

Chaille T. Webb, Wei Yang, Blake T. Riley, Brooke K. Hayes, Komagal Kannan Sivaraman, Tess R. Malcolm, Stephen Harrop, Sarah C. Atkinson, Itamar Kass, Ashley M. Buckle, Nyssa Drinkwater, and Sheena McGowan

Subjects

Metals, Catalytic Domain, Plasmodium falciparum, Cell Biology, Molecular Biology, Biochemistry, Aminopeptidases

Abstract

The metal-dependent M17 aminopeptidases are conserved throughout all kingdoms of life. This large enzyme family is characterized by a conserved binuclear metal center and a distinctive homohexameric arrangement. Recently, we showed that hexamer formation in Plasmodium M17 aminopeptidases was controlled by the metal ion environment, although the functional necessity for hexamer formation is still unclear. To further understand the mechanistic role of the hexameric assembly, here we undertook an investigation of the structure and dynamics of the M17 aminopeptidase from Plasmodium falciparum, PfA-M17. We describe a novel structure of PfA-M17, which shows that the active sites of each trimer are linked by a dynamic loop, and loop movement is coupled with a drastic rearrangement of the binuclear metal center and substrate-binding pocket, rendering the protein inactive. Molecular dynamics simulations and biochemical analyses of PfA-M17 variants demonstrated that this rearrangement is inherent to PfA-M17, and that the transition between the active and inactive states is metal dependent and part of a dynamic regulatory mechanism. Key to the mechanism is a remodeling of the binuclear metal center, which occurs in response to a signal from the neighboring active site and serves to moderate the rate of proteolysis under different environmental conditions. In conclusion, this work identifies a precise mechanism by which oligomerization contributes to PfA-M17 function. Furthermore, it describes a novel role for metal cofactors in the regulation of enzymes, with implications for the wide range of metalloenzymes that operate via a two-metal ion catalytic center, including DNA processing enzymes and metalloproteases.

Published

2022

9. Structure-based development of potent Plasmodium falciparum M1 and M17 aminopeptidase selective and dual inhibitors via S1′-region optimisation

Author

Petar P.S. Calic, Natalie B. Vinh, Chaille T. Webb, Tess R. Malcolm, Anna Ngo, Kym Lowes, Nyssa Drinkwater, Sheena McGowan, and Peter J. Scammells

Subjects

Pharmacology, Organic Chemistry, Drug Discovery, General Medicine

Published

2023

10. M17 aminopeptidases diversify function by moderating their macromolecular assemblies and active site environment

Author

Tess R. Malcolm, Nyssa Drinkwater, and Sheena McGowan

Subjects

Models, Molecular, 0301 basic medicine, Proteolysis, Computational biology, Biochemistry, Substrate Specificity, Leucyl Aminopeptidase, 03 medical and health sciences, Catalytic Domain, medicine, Animals, Humans, chemistry.chemical_classification, Bacteria, 030102 biochemistry & molecular biology, biology, medicine.diagnostic_test, Eukaryota, Active site, General Medicine, Amino acid, Macromolecular assembly, 030104 developmental biology, Enzyme, Order (biology), chemistry, Metals, biology.protein, Function (biology), Macromolecule

Abstract

The family of M17 aminopeptidases (alias ‘leucine aminopeptidases’, M17-LAPs) utilize a highly conserved hexameric structure and a binuclear metal center to selectively remove N-terminal amino acids from short peptides. However, M17-LAPs are responsible for a wide variety of functions that are seemingly unrelated to proteolysis. Herein, we aimed to investigate the myriad of functions attributed to M17. Further, we attempted to differentiate between the different molecular mechanisms that allow the conserved hexameric structure of an M17-LAP to mediate such diverse functions. We have provided an overview of research that identifies precise physiological roles of M17-LAPs, and the distinct mechanisms by which the enzymes moderate those roles. The review shows that the conserved hexameric structure of the M17-LAPs has an extraordinary capability to moderate different molecular mechanisms. We have broadly categorized these mechanisms as ‘aminopeptidase-based’, which include the characteristic proteolysis reactions, and ‘association-driven’, which involves moderation of the molecule's macromolecular assembly and higher order complexation events. The different molecular mechanisms are capable of eliciting very different cellular outcomes, and must be regarded as distinct when the physiological roles of this large and important family are considered.

Published

2019

11. Cephamycins inhibit pathogen sporulation and effectively treat recurrent Clostridioides difficile infection

Author

Bliss Cunningham, Dena Lyras, Sophie L. Day, Melanie L. Hutton, Milena M. Awad, Yogitha N. Srikhanta, Nyssa Drinkwater, Sheena McGowan, and Julie Singleton

Subjects

Microbiology (medical), 0303 health sciences, biology, 030306 microbiology, medicine.drug_class, fungi, Immunology, Antibiotics, Bacillus cereus, Cell Biology, Clostridium difficile, biology.organism_classification, Applied Microbiology and Biotechnology, Microbiology, Bacillus anthracis, 03 medical and health sciences, Genetics, medicine, Vancomycin, Cephamycins, Cephamycin, Pathogen, 030304 developmental biology, medicine.drug

Abstract

Spore-forming bacteria encompass a diverse range of genera and species, including important human and animal pathogens, and food contaminants. Clostridioides difficile is one such bacterium and is a global health threat because it is the leading cause of antibiotic-associated diarrhoea in hospitals. A crucial mediator of C. difficile disease initiation, dissemination and re-infection is the formation of spores that are resistant to current therapeutics, which do not target sporulation. Here, we show that cephamycin antibiotics inhibit C. difficile sporulation by targeting spore-specific penicillin-binding proteins. Using a mouse disease model, we show that combined treatment with the current standard-of-care antibiotic, vancomycin, and a cephamycin prevents disease recurrence. Cephamycins were found to have broad applicability as an anti-sporulation strategy, as they inhibited sporulation in other spore-forming pathogens, including the food contaminant Bacillus cereus. This study could directly and immediately affect treatment of C. difficile infection and advance drug development to control other important spore-forming bacteria that are problematic in the food industry (B. cereus), are potential bioterrorism agents (Bacillus anthracis) and cause other animal and human infections.

Published

2019

12. Novel Human Aminopeptidase N Inhibitors: Discovery and Optimization of Subsite Binding Interactions

Author

Luke S. Schembri, Susan A. Charman, Sheena McGowan, Georgina S. Butler, Christopher M. Overall, Jisook Lee, Wei Yang, Nyssa Drinkwater, Peter M. Grin, Peter J. Scammells, Natalie B. Vinh, Komagal Kannan Sivaraman, and Michelle Gazdik

Subjects

Male, Angiogenesis, CD13 Antigens, 01 natural sciences, Aminopeptidase, Mice, 03 medical and health sciences, chemistry.chemical_compound, Drug Discovery, Animals, Humans, Enzyme Inhibitors, Cytotoxicity, Benzamide, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Binding Sites, Hydroxamic acid, biology, Plasmodium falciparum, biology.organism_classification, In vitro, Protein Structure, Tertiary, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Enzyme, chemistry, Biochemistry, Molecular Medicine, hormones, hormone substitutes, and hormone antagonists, Protein Binding

Abstract

Aminopeptidase N (APN/CD13) is a zinc-dependent M1 aminopeptidase that contributes to cancer progression by promoting angiogenesis, metastasis, and tumor invasion. We have previously identified hydroxamic acid-containing analogues that are potent inhibitors of the APN homologue from the malarial parasite Plasmodium falciparum M1 aminopeptidase (PfA-M1). Herein, we describe the rationale that underpins the repurposing of PfA-M1 inhibitors as novel APN inhibitors. A series of novel hydroxamic acid analogues were developed using a structure-based design approach and evaluated their inhibition activities against APN. N-(2-(Hydroxyamino)-2-oxo-1-(3',4',5'-trifluoro-[1,1'-biphenyl]-4-yl)ethyl)-4-(methylsulfonamido)benzamide (6ad) proved to be an extremely potent inhibitor of APN activity in vitro, selective against other zinc-dependent enzymes such as matrix metalloproteases, and possessed limited cytotoxicity against Ad293 cells and favorable physicochemical and metabolic stability properties. The combined results indicate that compound 6ad may be a useful lead for the development of anticancer agents.

Published

2019

13. Mapping the substrate sequence and length of the Plasmodium M1 and M17 aminopeptidases

Author

Tess R. Malcolm, Karolina Weronika Swiderska, Marcin Drag, Brooke K. Hayes, Nyssa Drinkwater, and Sheena McGowan

Subjects

chemistry.chemical_classification, biology, Plasmodium vivax, Cooperativity, Peptide, Plasmodium falciparum, biology.organism_classification, Plasmodium, Aminopeptidase, Enzyme, Biochemistry, chemistry, parasitic diseases, Plasmodium berghei

Abstract

During malarial infection, Plasmodium parasites digest human hemoglobin to obtain free amino acids for protein production and maintenance of osmotic pressure. The Plasmodium M1 and M17 aminopeptidases are both postulated to have an essential role in the terminal stages of the hemoglobin digestion process and are validated drug targets for the design of new dualtarget anti-malarial compounds. In this study, we profiled the substrate specificity fingerprints and kinetic behaviors of M1 and M17 aminopeptidases from Plasmodium falciparum and Plasmodium vivax, and the mouse model species, Plasmodium berghei. We found that although the Plasmodium M1 aminopeptidases share a largely similar, broad specificity at the P1 position, the P. falciparum M1 displays the greatest diversity in specificity and P. berghei M1 showing a preference for charged P1 residues. In contrast, the Plasmodium M17 aminopeptidases share a highly conserved preference for hydrophobic residues at the P1 position. The aminopeptidases also demonstrated intra-peptide sequence specificity, particularly the M1 aminopeptidases, which showed a definitive preference for peptides with fewer negatively charged intrapeptide residues. When tested with a panel of peptides of increasing length, each aminopeptidase exhibited unique catalytic behavioral responses to the increase in peptide length, although all six aminopeptidases exhibited an increase in cooperativity as peptide length increased. Overall the P. vivax and P. berghei enzymes were generally faster than the P. falciparum enzymes, which we postulate is due to subtle differences in structural dynamicity. Together, these results build a kinetic profile that allows us to better understand the catalytic nuances of the M1 and M17 aminopeptidases from different Plasmodium species.

Published

2020

14. Metal Dependent Dynamic Equilibrium: A Regulatory Mechanism for M17 Aminopeptidases fromPlasmodium falciparumandPlasmodium vivax

Author

Sheena McGowan, Natalie A. Borg, Sarah C. Atkinson, Matthew J Belousoff, Hariprasad Venugopal, Tess R. Malcolm, and Nyssa Drinkwater

Subjects

biology, Stereochemistry, Chemistry, Metal ions in aqueous solution, Active site, Plasmodium falciparum, Random hexamer, Exopeptidase, biology.organism_classification, Metal, Tetramer, visual_art, biology.protein, visual_art.visual_art_medium, Dynamic equilibrium

Abstract

M17 leucyl aminopeptidases are metal-dependent exopeptidases that rely on oligomerization to diversify their functional roles. The M17 aminopeptidases fromPlasmodium falciparum(PfA-M17) andPlasmodium vivax(Pv-M17) function as catalytically active hexamers to acquire free amino acids from human hemoglobin and are drug targets for the design of novel anti-malarial agents. In this study, we found that the active site metal ions essential for catalytic activity have a secondary structural role mediating the formation of active hexamers. We found thatPfA-M17 andPv-M17 exist in a metal-dependent dynamic equilibrium between active hexameric species and smaller inactive species, that can be controlled by manipulating the identity and concentration of metal ions available. Mutation of residues involved in metal ion binding impaired catalytic activity and the formation of active hexamers. Structural resolution of thePv-M17 hexameric species revealed thatPfA-M17 andPv-M17 bind metal ions and substrates in a conserved fashion, althoughPv-M17 forms the active hexamer more readily and processes substrates faster thanPfA-M17. On the basis of solution studies and structures determined by cryo-electron microscopy, we propose a dynamic equilibrium between monomer dimer tetramer hexamer, which becomes directional towards the large oligomeric states with the addition of metal ions. M17 aminopeptidases can exploit this sophisticated metal-dependent dynamic equilibrium to regulate formation of the catalytically active hexamer and therefore regulate catalysis.

Published

2020

15. A Structure-Activity Relationship Study of Novel Hydroxamic Acid Inhibitors around the S1 Subsite of Human Aminopeptidase N

Author

Nyssa Drinkwater, Jisook Lee, Peter J. Scammells, and Sheena McGowan

Subjects

Pharmacology, Human Aminopeptidase N, Hydroxamic acid, Binding Sites, Stereochemistry, Angiogenesis, Aminopeptidase N, Organic Chemistry, CD13 Antigens, Hydroxamic Acids, Biochemistry, Transmembrane protein, In vitro, chemistry.chemical_compound, Kinetics, Structure-Activity Relationship, chemistry, Drug Design, Drug Discovery, Molecular Medicine, Structure–activity relationship, Humans, General Pharmacology, Toxicology and Pharmaceutics, Benzamide

Abstract

Aminopeptidase N (APN/CD13) is a zinc-dependent ubiquitous transmembrane ectoenzyme that is widely present in different types of cells. APN is one of the most extensively studied metalloaminopeptidases as an anti-cancer target due to its significant role in the regulation of metastasis and angiogenesis. Previously, we identified a potent and selective APN inhibitor, N-(2-(Hydroxyamino)-2-oxo-1-(3',4',5'-trifluoro-[1,1'-biphenyl]-4-yl)ethyl)-4-(methylsulfonamido)benzamide (3). Herein, we report the further modifications performed to explore SAR around the S1 subsite of APN and to improve the physicochemical properties. A series of hydroxamic acid analogues were synthesised, and the pharmacological activities were evaluated in vitro. N-(1-(3'-Fluoro-[1,1'-biphenyl]-4-yl)-2-(hydroxyamino)-2-oxoethyl)-4-(methylsulfonamido)benzamide (6 f) was found to display an extremely potent inhibitory activity in the sub-nanomolar range.

Published

2020

16. Crystal structure of a β-aminopeptidase from an AustralianBurkholderiasp

Author

Dena Lyras, Geoff Dumsday, Priscilla A. Johanesen, Marietta John-White, Sheena McGowan, and Nyssa Drinkwater

Subjects

Models, Molecular, Protein Conformation, alpha-Helical, 0301 basic medicine, Peptidomimetic, Amino Acid Motifs, Gene Expression, Crystal structure, Wastewater, Crystallography, X-Ray, Aminopeptidases, 01 natural sciences, Biochemistry, Aminopeptidase, Substrate Specificity, Research Communications, chemistry.chemical_compound, Structural Biology, Catalytic Domain, Cloning, Molecular, chemistry.chemical_classification, biology, medicine.diagnostic_test, Chemistry, Condensed Matter Physics, Monomer, Hydrophobic and Hydrophilic Interactions, Protein Binding, Proteases, Burkholderia, Stereochemistry, Recombinant Fusion Proteins, Proteolysis, Genetic Vectors, Biophysics, 03 medical and health sciences, Bacterial Proteins, Escherichia coli, Genetics, medicine, Humans, Protein Interaction Domains and Motifs, 010405 organic chemistry, biology.organism_classification, 0104 chemical sciences, 030104 developmental biology, Enzyme, Protein Conformation, beta-Strand, Peptidomimetics, Protein Multimerization, Peptides

Abstract

β-Aminopeptidases are a unique group of enzymes that have the unusual capability to hydrolyze N-terminal β-amino acids from synthetic β-peptides. β-Peptides can form secondary structures mimicking α-peptide-like structures that are resistant to degradation by most known proteases and peptidases. These characteristics of β-peptides give them great potential as peptidomimetics. Here, the X-ray crystal structure of BcA5-BapA, a β-aminopeptidase from a Gram-negativeBurkholderiasp. that was isolated from activated sludge from a wastewater-treatment plant in Australia, is reported. The crystal structure of BcA5-BapA was determined to a resolution of 2.0 Å and showed a tetrameric assembly typical of the β-aminopeptidases. Each monomer consists of an α-subunit (residues 1–238) and a β-subunit (residues 239–367). Comparison of the structure of BcA5-BapA with those of other known β-aminopeptidases shows a highly conserved structure and suggests a similar proteolytic mechanism of action.

Published

2017

17. X‐ray crystal structure of cytochrome P450 monooxygenase CYP101J2 from Sphingobium yanoikuyae strain B2

Author

Geoffrey J. Dumsday, Nyssa Drinkwater, Priscilla A. Johanesen, Sheena McGowan, Birgit Unterweger, and Dena Lyras

Subjects

Models, Molecular, Protein Conformation, alpha-Helical, 0301 basic medicine, Protein Folding, Stereochemistry, Gene Expression, Crystallography, X-Ray, Hydroxylation, Biochemistry, Sphingobium, Substrate Specificity, 03 medical and health sciences, chemistry.chemical_compound, Bacterial Proteins, Cytochrome P-450 Enzyme System, Structural Biology, Protein Interaction Domains and Motifs, Cloning, Molecular, Molecular Biology, Binding Sites, Eucalyptol, 030102 biochemistry & molecular biology, biology, Strain (chemistry), Chemistry, Cytochrome P450, Substrate (chemistry), Monooxygenase, Cyclohexanols, biology.organism_classification, Recombinant Proteins, 3. Good health, Sphingomonadaceae, Monoterpenes, biology.protein, Protein Conformation, beta-Strand, Protein folding, Protein Binding

Abstract

The cytochrome P450 monooxygenases (P450s) catalyze a vast array of oxygenation reactions that can be useful in biocatalytic applications. CYP101J2 from Sphingobium yanoikuyae is a P450 that catalyzes the hydroxylation of 1,8-cineole. Here we report the crystallization and X-ray structure elucidation of recombinant CYP101J2 to 1.8 Å resolution. The CYP101J2 structure shows the canonical P450-fold and has an open conformation in the absence of substrate. Analysis of the structure revealed that CYP101J2, in the absence of substrate, forms a well-ordered substrate-binding channel that suggests a unique form of substrate guidance in comparison to other bacterial 1,8-cineole-hydroxylating P450 enzymes. Proteins 2017; 85:945-950. © 2016 Wiley Periodicals, Inc.

Published

2017

18. M1 aminopeptidases as drug targets: broad applications or therapeutic niche?

Author

Tess R. Malcolm, Jisook Lee, Sheena McGowan, Nyssa Drinkwater, and Wei Yang

Subjects

0301 basic medicine, Drug, Anti malarial, Research groups, M1 aminopeptidase, media_common.quotation_subject, Niche, Special Issue: Proteases, Antineoplastic Agents, Computational biology, Review Article, Pharmacology, Biology, Biochemistry, Aminopeptidase, Aminopeptidases, drug discovery, 03 medical and health sciences, Antimalarials, 0302 clinical medicine, anti‐cancer, inhibitors, Animals, Humans, Molecular Biology, Review Articles, media_common, Mechanism (biology), Drug discovery, anti‐malarial, Cell Biology, 030104 developmental biology, 030220 oncology & carcinogenesis

Abstract

M1 aminopeptidase enzymes are a diverse family of metalloenzymes characterized by conserved structure and reaction specificity. Excluding viruses, M1 aminopeptidases are distributed throughout all phyla, and have been implicated in a wide range of functions including cell maintenance, growth and development, and defense. The structure and catalytic mechanism of M1 aminopeptidases are well understood, and make them ideal candidates for the design of small‐molecule inhibitors. As a result, many research groups have assessed their utility as therapeutic targets for both infectious and chronic diseases of humans, and many inhibitors with a range of target specificities and potential therapeutic applications have been developed. Herein, we have aimed to address these studies, to determine whether the family of M1 aminopeptidases does in fact present a universal target for the treatment of a diverse range of human diseases. Our analysis indicates that early validation of M1 aminopeptidases as therapeutic targets is often overlooked, which prevents the enzymes from being confirmed as drug targets. This validation cannot be neglected, and needs to include a thorough characterization of enzymes’ specific roles within complex physiological pathways. Furthermore, any chemical probes used in target validation must be carefully designed to ensure that specificity over the closely related enzymes has been achieved. While many drug discovery programs that target M1 aminopeptidases remain in their infancy, certain inhibitors have shown promise for the treatment of a range of conditions including malaria, hypertension, and cancer., The large family of therapeutically interesting M1 aminopeptidase enzymes has enormous potential to provide important drug targets. However, conservation of sequence, structure, and substrate specificity results in substantial challenges, and necessitates the need for careful target validation. Some studies have achieved this, and successfully validated M1 aminopeptidases as targets for the treatment of malaria, hypertension, and cancer.

Published

2017

19. Circumventing the stability-function trade-off in an engineered FN3 domain

Author

Benjamin T. Porebski, Daniel Christ, Morag R. Hunter, Peter R. Schofield, Rodrigo Vazquez-Lombardi, Ashley M. Buckle, Paul J. Conroy, Sheena McGowan, David E. Hoke, and Nyssa Drinkwater

Subjects

0301 basic medicine, Scaffold, 030102 biochemistry & molecular biology, Bioengineering, Protein engineering, Plasma protein binding, consensus design, loop grafting, protein engineering, stability-function trade-off, X-ray crystallography, Biochemistry, Stability (probability), 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, chemistry, Biophysics, Chemical stability, Thermal stability, Original Article, Lysozyme, Molecular Biology, Function (biology), Biotechnology

Abstract

The favorable biophysical attributes of non-antibody scaffolds make them attractive alternatives to monoclonal antibodies. However, due to the well-known stability-function trade-off, these gains tend to be marginal after functional selection. A notable example is the fibronectin Type III (FN3) domain, FNfn10, which has been previously evolved to bind lysozyme with 1 pM affinity (FNfn10-α-lys), but suffers from poor thermodynamic and kinetic stability. To explore this stability-function compromise further, we grafted the lysozyme-binding loops from FNfn10-α-lys onto our previously engineered, ultra-stable FN3 scaffold, FN3con. The resulting variant (FN3con-α-lys) bound lysozyme with a markedly reduced affinity, but retained high levels of thermal stability. The crystal structure of FNfn10-α-lys in complex with lysozyme revealed unanticipated interactions at the protein-protein interface involving framework residues of FNfn10-α-lys, thus explaining the failure to transfer binding via loop grafting. Utilizing this structural information, we redesigned FN3con-α-lys and restored picomolar binding affinity to lysozyme, while maintaining thermodynamic stability (with a thermal melting temperature 2-fold higher than that of FNfn10-α-lys). FN3con therefore provides an exceptional window of stability to tolerate deleterious mutations, resulting in a substantial advantage for functional design. This study emphasizes the utility of consensus design for the generation of highly stable scaffolds for downstream protein engineering studies.

Published

2016

20. Structure and substrate fingerprint of aminopeptidase P from Plasmodium falciparum

Author

Natalie B. Vinh, Peter J. Scammells, Khadija Mohamed, Sheena McGowan, Nyssa Drinkwater, Wioletta Rut, Komagal Kannan Sivaraman, Rebecca S. Bamert, and Marcin Drag

Subjects

Models, Molecular, 0301 basic medicine, Protein Conformation, Proteolysis, Plasmodium falciparum, Drug resistance, Biology, Crystallography, X-Ray, Aminopeptidases, Biochemistry, Aminopeptidase, Substrate Specificity, 03 medical and health sciences, Escherichia coli, medicine, Animals, Protease inhibitor (pharmacology), Molecular Biology, chemistry.chemical_classification, 030102 biochemistry & molecular biology, medicine.diagnostic_test, Cell Biology, medicine.disease, biology.organism_classification, Amino acid, 030104 developmental biology, Enzyme, chemistry, Dimerization, Malaria

Abstract

Malaria is one of the world's most prevalent parasitic diseases, with over 200 million cases annually. Alarmingly, the spread of drug-resistant parasites threatens the effectiveness of current antimalarials and has made the development of novel therapeutic strategies a global health priority. Malaria parasites have a complicated lifecycle, involving an asymptomatic ‘liver stage’ and a symptomatic ‘blood stage’. During the blood stage, the parasites utilise a proteolytic cascade to digest host hemoglobin, which produces free amino acids absolutely necessary for parasite growth and reproduction. The enzymes required for hemoglobin digestion are therefore attractive therapeutic targets. The final step of the cascade is catalyzed by several metalloaminopeptidases, including aminopeptidase P (APP). We developed a novel platform to examine the substrate fingerprint of APP from Plasmodium falciparum (PfAPP) and to show that it can catalyze the removal of any residue immediately prior to a proline. Further, we have determined the crystal structure of PfAPP and present the first examination of the 3D structure of this essential malarial enzyme. Together, these analyses provide insights into potential mechanisms of inhibition that could be used to develop novel antimalarial therapeutics.

Published

2016

21. Active site metals mediate an oligomeric equilibrium in Plasmodium M17 aminopeptidases

Author

Hariprasad Venugopal, Sarah C. Atkinson, Matthew J. Belousoff, Sheena McGowan, Nyssa Drinkwater, Natalie A. Borg, and Tess R. Malcolm

Subjects

WT, wild type, Models, Molecular, Protein Conformation, alpha-Helical, 0301 basic medicine, Plasmodium, metalloprotease, Dimer, leucine aminopeptidase, Protozoan Proteins, Gene Expression, Random hexamer, Crystallography, X-Ray, Aminopeptidases, Biochemistry, Aminopeptidase, Substrate Specificity, chemistry.chemical_compound, Catalytic Domain, Magnesium, Cloning, Molecular, Dynamic equilibrium, biology, SAXS, small-angle X-ray scattering, regulation, Cobalt, Dipeptides, MM, metal-binding mutant, Recombinant Proteins, Enzyme structure, Zinc, Leu-Mec, L-Leucine-7-amido-4-methyl-coumarin, Cys-Gly, cysteine-glycinyl, Research Article, Protein Binding, Cations, Divalent, Stereochemistry, MDFF, Molecular dynamic flexible fitting, Plasmodium falciparum, oligomerization, 03 medical and health sciences, Tetramer, Escherichia coli, Protein Interaction Domains and Motifs, Molecular Biology, Manganese, AUC, analytical ultracentrifugation, 030102 biochemistry & molecular biology, SEC-MALS, size exclusion chromatography multi-angle light scattering, Cryoelectron Microscopy, Active site, Cell Biology, Exopeptidase, Kinetics, 030104 developmental biology, chemistry, Mutation, biology.protein, Protein Conformation, beta-Strand, Protein Multimerization, NCS, noncrystallographic symmetry, Plasmodium vivax, LAP, leucine aminopeptidase

Abstract

M17 leucyl aminopeptidases are metal-dependent exopeptidases that rely on oligomerization to diversify their functional roles. The M17 aminopeptidases from Plasmodium falciparum (PfA-M17) and Plasmodium vivax (Pv-M17) function as catalytically active hexamers to generate free amino acids from human hemoglobin and are drug targets for the design of novel antimalarial agents. However, the molecular basis for oligomeric assembly is not fully understood. In this study, we found that the active site metal ions essential for catalytic activity have a secondary structural role mediating the formation of active hexamers. We found that PfA-M17 and Pv-M17 exist in a metal-dependent dynamic equilibrium between active hexameric species and smaller inactive species that can be controlled by manipulating the identity and concentration of metals available. Mutation of residues involved in metal ion binding impaired catalytic activity and the formation of active hexamers. Structural resolution of Pv-M17 by cryoelectron microscopy and X-ray crystallography together with solution studies revealed that PfA-M17 and Pv-M17 bind metal ions and substrates in a conserved fashion, although Pv-M17 forms the active hexamer more readily and processes substrates faster than PfA-M17. On the basis of these studies, we propose a dynamic equilibrium between monomer ↔ dimer ↔ tetramer ↔ hexamer, which becomes directional toward the large oligomeric states with the addition of metal ions. This sophisticated metal-dependent dynamic equilibrium may apply to other M17 aminopeptidases and underpin the moonlighting capabilities of this enzyme family.

Published

2021

22. Identification of the Binding Site of Apical Membrane Antigen 1 (AMA1) Inhibitors Using a Paramagnetic Probe

Author

Peter J. Scammells, Mansura Akter, Martin J. Scanlon, Simon C. Drew, Bankala Krishnarjuna, Geqing Wang, Raymond S. Norton, Nyssa Drinkwater, Sheena McGowan, Cael Debono, Shane M. Devine, and Christopher A. MacRaild

Subjects

Models, Molecular, Magnetic Resonance Spectroscopy, Protozoan Proteins, Peptide, Antigens, Protozoan, Plasma protein binding, Crystallography, X-Ray, Ligands, 01 natural sciences, Biochemistry, Structure-Activity Relationship, parasitic diseases, Drug Discovery, Pyrroles, Amino Acid Sequence, General Pharmacology, Toxicology and Pharmaceutics, Apical membrane antigen 1, Binding site, Spin label, Furans, Peptide sequence, Quinazolinones, Pharmacology, chemistry.chemical_classification, Sulfonamides, Binding Sites, Molecular Structure, 010405 organic chemistry, Chemistry, Organic Chemistry, Cell Membrane, Membrane Proteins, Apical membrane, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Pyrimidines, Molecular Probes, Biophysics, Molecular Medicine, Pyrazoles, Benzimidazoles, Molecular probe, Peptides, Hydrophobic and Hydrophilic Interactions, Protein Binding

Abstract

Apical membrane antigen 1 (AMA1) is essential for the invasion of host cells by malaria parasites. Several small-molecule ligands have been shown to bind to a conserved hydrophobic cleft in Plasmodium falciparum AMA1. However, a lack of detailed structural information on the binding pose of these molecules has hindered their further optimisation as inhibitors. We have developed a spin-labelled peptide based on RON2, the native binding partner of AMA1, to probe the binding sites of compounds on PfAMA1. The crystal structure of this peptide bound to PfAMA1 shows that it binds at one end of the hydrophobic groove, leaving much of the binding site unoccupied and allowing fragment hits to bind without interference. In paramagnetic relaxation enhancement (PRE)-based NMR screening, the 1 H relaxation rates of compounds binding close to the probe were enhanced. Compounds experienced different degrees of PRE as a result of their different orientations relative to the spin label while bound to AMA1. Thus, PRE-derived distance constraints can be used to identify binding sites and guide further hit optimisation.

Published

2018

23. Hydroxamic Acid Inhibitors Provide Cross-Species Inhibition of Plasmodium M1 and M17 Aminopeptidases

Author

Sandra Duffy, Peter J. Scammells, Peter M. Grin, Tess R. Malcolm, Georgina S. Butler, Vicky M. Avery, Leonardo Lucantoni, Christopher M. Overall, Sheena McGowan, Natalie B. Vinh, Nyssa Drinkwater, and Michael Kassiou

Subjects

Plasmodium, Cell Survival, Plasmodium vivax, Drug Resistance, Protozoan Proteins, Hydroxamic Acids, 01 natural sciences, Aminopeptidases, 03 medical and health sciences, chemistry.chemical_compound, Antimalarials, Structure-Activity Relationship, Catalytic Domain, parasitic diseases, Drug Discovery, Structure–activity relationship, Humans, Protease Inhibitors, Binding site, 030304 developmental biology, Metalloexopeptidase, chemistry.chemical_classification, 0303 health sciences, Hydroxamic acid, Binding Sites, biology, Chemistry, Plasmodium falciparum, biology.organism_classification, 3. Good health, 0104 chemical sciences, Molecular Docking Simulation, 010404 medicinal & biomolecular chemistry, Enzyme, HEK293 Cells, Biochemistry, Molecular Medicine, Hemoglobin

Abstract

There is an urgent clinical need for antimalarial compounds that target malaria caused by both Plasmodium falciparum and Plasmodium vivax. The M1 and M17 metalloexopeptidases play key roles in Plasmodium hemoglobin digestion and are validated drug targets. We used a multitarget strategy to rationally design inhibitors capable of potent inhibition of the M1 and M17 aminopeptidases from both P. falciparum ( Pf-M1 and Pf-M17) and P. vivax ( Pv-M1 and Pv-M17). The novel chemical series contains a hydroxamic acid zinc binding group to coordinate catalytic zinc ion/s, and a variety of hydrophobic groups to probe the S1' pockets of the four target enzymes. Structural characterization by cocrystallization showed that selected compounds utilize new and unexpected binding modes; most notably, compounds substituted with bulky hydrophobic substituents displace the Pf-M17 catalytic zinc ion. Excitingly, key compounds of the series potently inhibit all four molecular targets and show antimalarial activity comparable to current clinical candidates.

Published

2018

24. Cephamycins inhibit pathogen sporulation and effectively treat recurrent Clostridioides difficile infection

Author

Yogitha N, Srikhanta, Melanie L, Hutton, Milena M, Awad, Nyssa, Drinkwater, Julie, Singleton, Sophie L, Day, Bliss A, Cunningham, Sheena, McGowan, and Dena, Lyras

Subjects

Male, Spores, Bacterial, Cell Survival, Clostridioides difficile, Bacterial Toxins, Gene Expression Regulation, Bacterial, Anti-Bacterial Agents, Mice, Inbred C57BL, Disease Models, Animal, Mice, Genes, Bacterial, Vancomycin, Chlorocebus aethiops, Clostridium Infections, Animals, Penicillin-Binding Proteins, Cephamycins, Vero Cells

Abstract

Spore-forming bacteria encompass a diverse range of genera and species, including important human and animal pathogens, and food contaminants. Clostridioides difficile is one such bacterium and is a global health threat because it is the leading cause of antibiotic-associated diarrhoea in hospitals. A crucial mediator of C. difficile disease initiation, dissemination and re-infection is the formation of spores that are resistant to current therapeutics, which do not target sporulation. Here, we show that cephamycin antibiotics inhibit C. difficile sporulation by targeting spore-specific penicillin-binding proteins. Using a mouse disease model, we show that combined treatment with the current standard-of-care antibiotic, vancomycin, and a cephamycin prevents disease recurrence. Cephamycins were found to have broad applicability as an anti-sporulation strategy, as they inhibited sporulation in other spore-forming pathogens, including the food contaminant Bacillus cereus. This study could directly and immediately affect treatment of C. difficile infection and advance drug development to control other important spore-forming bacteria that are problematic in the food industry (B. cereus), are potential bioterrorism agents (Bacillus anthracis) and cause other animal and human infections.

Published

2018

25. X-ray crystal structures of an orally available aminopeptidase inhibitor, Tosedostat, bound to anti-malarial drug targets P f A-M1 and P f A-M17

Author

Alessandro Paiardini, Nyssa Drinkwater, Komagal Kannan Sivaraman, Sheena McGowan, and Rebecca S. Bamert

Subjects

Drug, media_common.quotation_subject, medicine.medical_treatment, Drug resistance, Pharmacology, Biochemistry, Aminopeptidase, 03 medical and health sciences, 0302 clinical medicine, Structural Biology, Tosedostat, medicine, Molecular Biology, 030304 developmental biology, media_common, chemistry.chemical_classification, 0303 health sciences, Protease, biology, Plasmodium falciparum, biology.organism_classification, 3. Good health, Enzyme, chemistry, Structural biology, 030220 oncology & carcinogenesis

Abstract

New anti-malarial treatments are desperately required to face the spread of drug resistant parasites. Inhibition of metalloaminopeptidases, PfA-M1 and PfA-M17, is a validated therapeutic strategy for treatment of Plasmodium falciparum malaria. Here, we describe the crystal structures of PfA-M1 and PfA-M17 bound to chemotherapeutic agent Tosedostat. The inhibitor occupies the enzymes' putative product egress channels in addition to the substrate binding pockets; however, adopts different binding poses when bound to PfA-M1 and PfA-M17. These findings will be valuable for the continued development of selective inhibitors of PfA-M1 and PfA-M17. Proteins 2015; 83:789–795. © 2015 Wiley Periodicals, Inc.

Published

2015

26. A metal-dependent switch moderates activity of the hexameric M17 aminopeptidases

Author

Nyssa Drinkwater, Tess R. Malcolm, Ashley M. Buckle, Blake T. Riley, Komagal Kannan Sivaraman, Itamar Kass, Brooke K. Hayes, Natalie A. Borg, Sarah C. Atkinson, Sheena McGowan, and Wei Yang

Subjects

chemistry.chemical_classification, 0303 health sciences, biology, medicine.diagnostic_test, 010405 organic chemistry, Chemistry, Stereochemistry, Proteolysis, Active site, Trimer, 01 natural sciences, Aminopeptidase, Cofactor, 0104 chemical sciences, 03 medical and health sciences, chemistry.chemical_compound, Enzyme, biology.protein, medicine, Function (biology), DNA, 030304 developmental biology

Abstract

The metal-dependent M17 aminopeptidases are conserved throughout all kingdoms of life. The large enzyme family is characterised by a conserved binuclear metal center and a distinctive homohexameric arrangement. To understand the mechanistic role of the hexameric assembly, we undertook an investigation of the structure and dynamics of the M17 aminopeptidase fromP. falciparum,PfA-M17. We describe a novel structure ofPfA-M17, which shows that the active sites of each trimer are linked by a dynamic loop, and that the loop movement is coupled with a drastic rearrangement of the binuclear metal center and substrate-binding pocket. Molecular dynamics simulations, supported by biochemical analyses ofPfA-M17 variants, demonstrate that this rearrangement is inherent toPfA-M17, and that the transition between the active and inactive states is part of a dynamic regulatory mechanism. Key to the mechanism is a re-modelling of the binuclear metal center, which occurs in response to a signal from the neighbouring active site, and serves to moderate the rate of proteolysis under different environmental conditions. Therefore, this work has identified the precise mechanism by which oligomerization contributes toPfA-M17 function. Further, it has described a novel role for metal cofactors in the regulation of enzymes with implications for the wide range of metalloenzymes that operate via a two-metal ion catalytic center including DNA processing enzymes and metalloproteases.

Published

2018

27. Thermal sensitivity and flexibility of the Cε3 domains in immunoglobulin E

Author

Katy A, Doré, Anna M, Davies, Nyssa, Drinkwater, Andrew J, Beavil, James M, McDonnell, and Brian J, Sutton

Subjects

Models, Molecular, Glycosylation, Domain flexibility, Amino Acid Motifs, Gene Expression, Crystallography, X-Ray, DSF, differential scanning fluorimetry, Phase Transition, Protein Structure, Secondary, Article, Humans, Protein Interaction Domains and Motifs, Protein Structure, Quaternary, Antibody, Protein Unfolding, Binding Sites, Thermal unfolding, Protein Stability, Receptors, IgE, Temperature, Man, mannose, Immunoglobulin E, GlcNAc, N-acetylglucosamine, Recombinant Proteins, Immunoglobulin Fc Fragments, Carbohydrate Sequence, Fcε3–4, sub-fragment of IgE-Fc consisting of the dimer of Cε3 and Cε4 domains, Differential scanning fluorimetry, Protein Multimerization, Protein Binding

Abstract

Immunoglobulin E (IgE) is the antibody that plays a central role in the mechanisms of allergic diseases such as asthma. Interactions with its receptors, FcεRI on mast cells and CD23 on B cells, are mediated by the Fc region, a dimer of the Cε2, Cε3 and Cε4 domains. A sub-fragment lacking the Cε2 domains, Fcε3–4, also binds to both receptors, although receptor binding almost exclusively involves the Cε3 domains. This domain also contains the N-linked glycosylation site conserved in other isotypes. We report here the crystal structures of IgE-Fc and Fcε3–4 at the highest resolutions yet determined, 1.75 Å and 2.0 Å respectively, revealing unprecedented detail regarding the carbohydrate and its interactions with protein domains. Analysis of the crystallographic B-factors of these, together with all earlier IgE-Fc and Fcε3–4 structures, shows that the Cε3 domains exhibit the greatest intrinsic flexibility and quaternary structural variation within IgE-Fc. Intriguingly, both well-ordered carbohydrate and disordered polypeptide can be seen within the same Cε3 domain. A simplified method for comparing the quaternary structures of the Cε3 domains in free and receptor-bound IgE-Fc structures is presented, which clearly delineates the FcεRI and CD23 bound states. Importantly, differential scanning fluorimetric analysis of IgE-Fc and Fcε3–4 identifies Cε3 as the domain most susceptible to thermally-induced unfolding, and responsible for the characteristically low melting temperature of IgE., Highlights • The Cε3 domains of IgE are most susceptible to thermally induced unfolding determined by differential scanning fluorimetry. • The Cε3 domains are responsible for the characteristically low melting temperature of IgE. • The Cε3 domains exhibit the greatest intrinsic flexibility. • Quaternary structural diversity of Cε3 domains is compared across all known structures using a simplified single parameter. • Human IgE-Fc and Fcε3–4 domain structures are determined at the highest resolutions yet reported (1.75 Å and 2.0 Å).

Published

2017

28. Human immunoglobulin E flexes between acutely bent and extended conformations

Author

Lindsay K. Shuttleworth, Andrew J. Beavil, Amanda K. F. Oxbrow, Alistair James Henry, Michael W-P Kao, James M. McDonnell, Benjamin P. Cossins, Jean Delgado, Hanna Hailu, Michael John Wright, Nyssa Drinkwater, Brian J. Sutton, Katharine Cain, and Anthony H. Keeble

Subjects

B-Lymphocytes, Chemistry, Stereochemistry, Receptors, IgE, Bent molecular geometry, Molecular biophysics, Calorimetry, Immunoglobulin E, Surface Plasmon Resonance, Crystallography, X-Ray, Fragment crystallizable region, Article, Protein Structure, Tertiary, Crystallography, Molecular dynamics, Protein structure, Förster resonance energy transfer, Structural Biology, Fluorescence Resonance Energy Transfer, Hypersensitivity, Molecule, Humans, Surface plasmon resonance, Molecular Biology

Abstract

Crystallographic and solution studies have shown that IgE molecules are acutely bent in their Fc region. Crystal structures reveal the Cɛ2 domain pair folded back onto the Cɛ3-Cɛ4 domains, but is the molecule exclusively bent or can the Cɛ2 domains adopt extended conformations and even 'flip' from one side of the molecule to the other? We report the crystal structure of IgE-Fc captured in a fully extended, symmetrical conformation and show by molecular dynamics, calorimetry, stopped-flow kinetic, surface plasmon resonance (SPR) and Forster resonance energy transfer (FRET) analyses that the antibody can indeed adopt such extended conformations in solution. This diversity of conformational states available to IgE-Fc offers a new perspective on IgE function in allergen recognition, as part of the B-cell receptor and as a therapeutic target in allergic disease.

Published

2014

29. Structure and Characterisation of a Key Epitope in the Conserved C-Terminal Domain of the Malaria Vaccine Candidate MSP2

Author

Raymond S. Norton, Bankala Krishnarjuna, Garima Jaipuria, Karyn L. Wilde, Tamir Dingjan, Romain Rouet, Nyssa Drinkwater, Christopher A. MacRaild, Sheena McGowan, Daniel Christ, Jack S. Richards, Jeffrey Seow, Robin F. Anders, Hanudatta S. Atreya, and Rodrigo A.V. Morales

Subjects

0301 basic medicine, Models, Molecular, medicine.drug_class, Protein Conformation, Plasmodium falciparum, Protozoan Proteins, Antibodies, Protozoan, Antigens, Protozoan, Calorimetry, Monoclonal antibody, Crystallography, X-Ray, Epitope, 03 medical and health sciences, Epitopes, Mice, Antigen, Structural Biology, parasitic diseases, Malaria Vaccines, medicine, Animals, Merozoite surface protein, Molecular Biology, biology, Linear epitope, Malaria vaccine, Antibodies, Monoclonal, Surface Plasmon Resonance, biology.organism_classification, Virology, Molecular biology, 030104 developmental biology, biology.protein, Antibody, Protein Binding

Abstract

Merozoite surface protein 2 (MSP2) is an intrinsically disordered antigen that is abundant on the surface of the malaria parasite Plasmodium falciparum. The two allelic families of MSP2, 3D7 and FC27, differ in their central variable regions, which are flanked by highly conserved C-terminal and N-terminal regions. In a vaccine trial, full-length 3D7 MSP2 induced a strain-specific protective immune response despite the detectable presence of conserved region antibodies. This work focuses on the conserved C-terminal region of MSP2, which includes the only disulphide bond in the protein and encompasses key epitopes recognised by the mouse monoclonal antibodies 4D11 and 9H4. Although the 4D11 and 9H4 epitopes are overlapping, immunofluorescence assays have shown that the mouse monoclonal antibody 4D11 binds to MSP2 on the merozoite surface with a much stronger signal than 9H4. Understanding the structural basis for this antigenic difference between these antibodies will help direct the design of a broad-spectrum and MSP2-based malaria vaccine. 4D11 and 9H4 were reengineered into antibody fragments variable region fragment (Fv) and single-chain Fv (scFv)] and were validated as suitable models for their full-sized IgG counterparts by surface plasmon resonance and isothermal titration calorimetry. An alanine scan of the 13-residue epitope 3D7-MSP2(207-222) identified the minimal binding epitope of 4D11 and the key residues involved in binding. A 2.2-angstrom crystal structure of 4D11 Fv bound to the eight-residue epitope NKENCGAA provided valuable insight into the possible conformation of the C-terminal region of MSP2 on the parasite. This work underpins continued efforts to optimise recombinant MSP2 constructs for evaluation as potential vaccine candidates. (C) 2017 Elsevier Ltd. All rights reserved.

Published

2016

30. Structure-Activity Studies of β-Hairpin Peptide Inhibitors of the Plasmodium falciparum AMA1-RON2 Interaction

Author

Martin J. Scanlon, James G. Beeson, Jamie S. Simpson, Damien R. Drew, San Sui Lim, Geqing Wang, Robin F. Anders, Sheena McGowan, Biswaranjan Mohanty, Raymond S. Norton, David K. Chalmers, Christopher A. MacRaild, Philip E. Thompson, and Nyssa Drinkwater

Subjects

0301 basic medicine, Models, Molecular, Protein Conformation, Protozoan Proteins, Peptide, Antigens, Protozoan, Biology, Crystallography, X-Ray, Plasmodium, 03 medical and health sciences, Antimalarials, Structure-Activity Relationship, Structural Biology, parasitic diseases, Apical membrane antigen 1, Binding site, Molecular Biology, Cell invasion, chemistry.chemical_classification, 030102 biochemistry & molecular biology, Drug discovery, Membrane Proteins, Plasmodium falciparum, biology.organism_classification, 030104 developmental biology, chemistry, Biochemistry, Rhoptry neck, Mutant Proteins, Peptides, Protein Binding

Abstract

The interaction between apical membrane antigen 1 (AMA1) and rhoptry neck protein 2 (RON2) plays a key role in the invasion of red blood cells by Plasmodium parasites. Disruption of this critical protein-protein interaction represents a promising avenue for antimalarial drug discovery. In this work, we exploited a 13-residue β-hairpin based on the C-terminal loop of RON2 to probe a conserved binding site on Plasmodium falciparum AMA1. A series of mutations was synthetically engineered into β-hairpin peptides to establish structure-activity relationships. The best mutations improved the binding affinity of the β-hairpin peptide by ~7-fold for 3D7 AMA1 and ~14-fold for FVO AMA1. We determined the crystal structures of several β-hairpin peptides in complex with AMA1 in order to define the structural features and specific interactions that contribute to improved binding affinity. The same mutations in the longer RON2sp2 peptide (residues 2027-2055 of RON2) increased the binding affinity by >30-fold for 3D7 and FVO AMA1, producing KD values of 2.1nM and 0.4nM, respectively. To our knowledge, this is the most potent strain-transcending peptide reported to date and represents a valuable tool to characterize the AMA1-RON2 interaction.

Published

2016

31. Potent dual inhibitors of Plasmodium falciparum M1 and M17 aminopeptidases through optimization of S1 pocket interactions

Author

Chiara Ruggeri, Sasdekumar Loganathan, Vicky M. Avery, Peter J. Scammells, Nyssa Drinkwater, Rebecca S. Bamert, Andrew K. Powell, Susan A. Charman, Sheena McGowan, John P. Holleran, Natalie B. Vinh, Alessandro Paiardini, and Shailesh N. Mistry

Subjects

0301 basic medicine, Dual inhibition, Models, Molecular, aminopeptidase inhibitors, hydroxamic acid, malaria, plasmodium falciparum, zinc-binding group, aminopeptidases, antimalarials, hek293 cells, humans, hydroxamic acids, malaria, falciparum, models, molecular, protease inhibitors, protozoan proteins, structure-activity relationship, zinc, drug discovery3003 pharmaceutical science, organic chemistry, pharmacology, medicine.medical_treatment, Plasmodium falciparum, Protozoan Proteins, Biology, Hydroxamic Acids, 01 natural sciences, Aminopeptidases, 03 medical and health sciences, chemistry.chemical_compound, models, Antimalarials, Structure-Activity Relationship, falciparum, Resistant strain, Drug Discovery, medicine, Structure–activity relationship, Humans, Protease Inhibitors, molecular, Malaria, Falciparum, Hydroxamic acid, Protease, 010405 organic chemistry, HEK 293 cells, General Medicine, medicine.disease, biology.organism_classification, 3. Good health, 0104 chemical sciences, Zinc, 030104 developmental biology, HEK293 Cells, Biochemistry, chemistry, P. falciparum, Malaria, Aminopeptidase inhibitors, hydroxamic acid, zinc-binding group, Malaria

Abstract

© 2016 Elsevier Masson SAS. Malaria remains a global health problem, and though international efforts for treatment and eradication have made some headway, the emergence of drug-resistant parasites threatens this progress. Antimalarial therapeutics acting via novel mechanisms are urgently required. Plasmodium falciparum M1 and M17 are neutral aminopeptidases which are essential for parasite growth and development. Previous work in our group has identified inhibitors capable of dual inhibition of PfA-M1 and PfA-M17, and revealed further regions within the protease S1 pockets that could be exploited in the development of ligands with improved inhibitory activity. Herein, we report the structure-based design and synthesis of novel hydroxamic acid analogues that are capable of potent inhibition of both PfA-M1 and PfA-M17. Furthermore, the developed compounds potently inhibit Pf growth in culture, including the multi-drug resistant strain Dd2. The ongoing development of dual PfA-M1/PfA-M17 inhibitors continues to be an attractive strategy for the design of novel antimalarial therapeutics.

Published

2016

32. Missing Fragments: Detecting Cooperative Binding in Fragment-Based Drug Design

Author

Alan E. Mark, Pramod C. Nair, Nyssa Drinkwater, and Alpeshkumar K. Malde

Subjects

Drug, Fragment (logic), Chemistry, media_common.quotation_subject, Organic Chemistry, Drug Discovery, False positive paradox, Binding pocket, Cooperative binding, Computational biology, Bioinformatics, Biochemistry, media_common

Abstract

The aim of fragment-based drug design (FBDD) is to identify molecular fragments that bind to alternate subsites within a given binding pocket leading to cooperative binding when linked. In this study, the binding of fragments to human phenylethanolamine N-methyltransferase is used to illustrate how (a) current protocols may fail to detect fragments that bind cooperatively, (b) theoretical approaches can be used to validate potential hits, and (c) apparent false positives obtained when screening against cocktails of fragments may in fact indicate promising leads.

Published

2012

33. Molecular recognition of physiological substrate noradrenaline by the adrenaline-synthesizing enzyme PNMT and factors influencing its methyltransferase activity

Author

Jennifer L. Martin, Munish Puri, Christine L. Gee, Nyssa Drinkwater, Kevin R. Criscione, Gary L. Grunewald, and Michael J. McLeish

Subjects

chemistry.chemical_classification, endocrine system, Binding Sites, Epinephrine, Ligand, Chemistry, Stereochemistry, Phenylethanolamine N-Methyltransferase, Substrate (chemistry), Cell Biology, Crystallography, X-Ray, Biochemistry, Article, Substrate Specificity, Enzyme catalysis, Norepinephrine, chemistry.chemical_compound, Molecular recognition, Enzyme, Humans, Peptide bond, Carboxylate, Binding site, Molecular Biology, Protein Binding

Abstract

Substrate specificity is critically important for enzyme catalysis. In the adrenaline-synthesizing enzyme PNMT (phenylethanolamine N-methyltransferase), minor changes in substituents can convert substrates into inhibitors. Here we report the crystal structures of six human PNMT complexes, including the first structure of the enzyme in complex with its physiological ligand R-noradrenaline. Determining this structure required rapid soak methods because of the tendency for noradrenaline to oxidize. Comparison of the PNMT–noradrenaline complex with the previously determined PNMT–p-octopamine complex demonstrates that these two substrates form almost equivalent interactions with the enzyme and show that p-octopamine is a valid model substrate for PNMT. The crystal structures illustrate the adaptability of the PNMT substrate binding site in accepting multi-fused ring systems, such as substituted norbornene, as well as noradrenochrome, the oxidation product of noradrenaline. These results explain why only a subset of ligands recognized by PNMT are methylated by the enzyme; bulky substituents dictate the binding orientation of the ligand and can thereby place the acceptor amine too far from the donor methyl group for methylation to occur. We also show how the critical Glu185 catalytic residue can be replaced by aspartic acid with a loss of only 10-fold in catalytic efficiency. This is because protein backbone movements place the Asp185 carboxylate almost coincident with the carboxylate of Glu185. Conversely, replacement of Glu185 by glutamine reduces catalytic efficiency almost 300-fold, not only because of the loss of charge, but also because the variant residue does not adopt the same conformation as Glu185.

Published

2009

34. Structural basis for epitope masking and strain specificity of a conserved epitope in an intrinsically disordered malaria vaccine candidate

Author

Daniel Christ, Jeffrey Seow, Christopher A. MacRaild, Rodrigo A.V. Morales, Sheena McGowan, Robin F. Anders, Raymond S. Norton, Bankala Krishnarjuna, Romain Rouet, and Nyssa Drinkwater

Subjects

medicine.drug_class, Plasmodium falciparum, Protozoan Proteins, Antigens, Protozoan, Biology, Monoclonal antibody, Epitope, Article, 03 medical and health sciences, Epitopes, Antigen, parasitic diseases, Malaria Vaccines, medicine, Humans, Merozoite surface protein, 030304 developmental biology, Genetics, 0303 health sciences, Multidisciplinary, Linear epitope, Malaria vaccine, 030302 biochemistry & molecular biology, Antibodies, Monoclonal, biology.organism_classification, Virology, 3. Good health, biology.protein, Antibody

Abstract

Merozoite surface protein 2 (MSP2) is an intrinsically disordered, membrane-anchored antigen of the malaria parasite Plasmodium falciparum. MSP2 can elicit a protective, albeit strain-specific, antibody response in humans. Antibodies are generated to the conserved N- and C-terminal regions but many of these react poorly with the native antigen on the parasite surface. Here we demonstrate that recognition of a conserved N-terminal epitope by mAb 6D8 is incompatible with the membrane-bound conformation of that region, suggesting a mechanism by which native MSP2 escapes antibody recognition. Furthermore, crystal structures and NMR spectroscopy identify transient, strain-specific interactions between the 6D8 antibody and regions of MSP2 beyond the conserved epitope. These interactions account for the differential affinity of 6D8 for the two allelic families of MSP2, even though 6D8 binds to a fully conserved epitope. These results highlight unappreciated mechanisms that may modulate the specificity and efficacy of immune responses towards disordered antigens.

Published

2015

35. Screening the medicines for Malaria Venture 'Malaria Box' against the Plasmodium falciparum aminopeptidases, M1, M17 and M18

Author

Shailesh N. Mistry, Peter J. Scammells, Alessandro Paiardini, Rebecca S. Bamert, Komagal Kannan-Sivaraman, Sheena McGowan, and Nyssa Drinkwater

Subjects

Plasmodium falciparum, malaria, Plasmodium, antimalerial, aminopeptidases, Drug Evaluation, Preclinical, Protozoan Proteins, lcsh:Medicine, Pharmacology, Aminopeptidases, 03 medical and health sciences, Antimalarials, Structure-Activity Relationship, medicine, Structure–activity relationship, Multiplex, Protease Inhibitors, lcsh:Science, 030304 developmental biology, 0303 health sciences, Multidisciplinary, biology, 030306 microbiology, Drug discovery, Mechanism (biology), lcsh:R, agricultural and biological sciences (all), biochemistry, genetics and molecular biology (all), medicine (all), biology.organism_classification, medicine.disease, 3. Good health, Molecular Docking Simulation, Parasitic disease, Molecular targets, lcsh:Q, Malaria, Research Article

Abstract

Malaria is a parasitic disease that remains a global health burden. The ability of the parasite to rapidly develop resistance to therapeutics drives an urgent need for the delivery of new drugs. The Medicines for Malaria Venture have compounds known for their antimalarial ac- tivity, but not necessarily the molecular targets. In this study, we assess the ability of the “MMV 400” compounds to inhibit the activity of three metalloaminopeptidases from Plasmo- dium falciparum, PfA-M1, PfA-M17 and PfM18 AAP. We have developed a multiplex assay system to allow rapid primary screening of compounds against all three metalloaminopepti- dases, followed by detailed analysis of promising compounds. Our results show that there were no PfM18AAP inhibitors, whereas two moderate inhibitors of the neutral aminopepti- dases PfA-M1 and PfA-M17 were identified. Further investigation through structure-activity relationship studies and molecular docking suggest that these compounds are competitive inhibitors with novel binding mechanisms, acting through either non-classical zinc coordina- tion or independently of zinc binding altogether. Although it is unlikely that inhibition of PfA- M1 and/or PfA-M17 is the primary mechanism responsible for the antiplasmodial activity re- ported for these compounds, their detailed characterization, as presented in this work, pave the way for their further optimization as a novel class of dual PfA-M1/PfA-M17 inhibitors uti- lising non-classical zinc binding groups.

Published

2015

36. From crystal to compound: structure-based antimalarial drug discovery

Author

Nyssa Drinkwater and Sheena McGowan

Subjects

Plasmodium falciparum, Protozoan Proteins, Drug resistance, Biology, Biochemistry, Models, Biological, Antimalarials, Drug Discovery, medicine, Global health, Animals, Humans, Molecular Biology, Compound structure, Life Cycle Stages, Resistance development, Molecular Structure, business.industry, Drug discovery, Plasmodium parasite, Cell Biology, medicine.disease, Drug Resistance, Multiple, Biotechnology, Risk analysis (engineering), Drug development, business, Malaria

Abstract

Despite a century of control and eradication campaigns, malaria remains one of the world's most devastating diseases. Our once-powerful therapeutic weapons are losing the war against the Plasmodium parasite, whose ability to rapidly develop and spread drug resistance hamper past and present malaria-control efforts. Finding new and effective treatments for malaria is now a top global health priority, fuelling an increase in funding and promoting open-source collaborations between researchers and pharmaceutical consortia around the world. The result of this is rapid advances in drug discovery approaches and technologies, with three major methods for antimalarial drug development emerging: (i) chemistry-based, (ii) target-based, and (iii) cell-based. Common to all three of these approaches is the unique ability of structural biology to inform and accelerate drug development. Where possible, SBDD (structure-based drug discovery) is a foundation for antimalarial drug development programmes, and has been invaluable to the development of a number of current pre-clinical and clinical candidates. However, as we expand our understanding of the malarial life cycle and mechanisms of resistance development, SBDD as a field must continue to evolve in order to develop compounds that adhere to the ideal characteristics for novel antimalarial therapeutics and to avoid high attrition rates pre- and post-clinic. In the present review, we aim to examine the contribution that SBDD has made to current antimalarial drug development efforts, covering hit discovery to lead optimization and prevention of parasite resistance. Finally, the potential for structural biology, particularly high-throughput structural genomics programmes, to identify future targets for drug discovery are discussed.

Published

2014

37. Two-pronged attack: dual inhibition of Plasmodium falciparum M1 and M17 metalloaminopeptidases by a novel series of hydroxamic acid-based inhibitors

Author

Komagal Kannan Sivaraman, Marcin Drag, Alessandro Paiardini, Nyssa Drinkwater, Shailesh N. Mistry, Vicky M. Avery, Chiara Ruggeri, Sabine Fletcher, Sheena McGowan, Peter J. Scammells, and Sasdekumar Loganathan

Subjects

Models, Molecular, Cell Survival, Plasmodium falciparum, Protozoan Proteins, Pharmacology, Hydroxamic Acids, Plasmodium, Aminopeptidases, chemistry.chemical_compound, Antimalarials, Structure-Activity Relationship, Drug Discovery, parasitic diseases, medicine, Structure–activity relationship, Humans, Protease Inhibitors, Antimalarial Agent, Artemisinin, Mode of action, Hydroxamic acid, biology, biology.organism_classification, medicine.disease, 3. Good health, HEK293 Cells, chemistry, Molecular Medicine, Malaria, medicine.drug

Abstract

Plasmodium parasites, the causative agents of malaria, have developed resistance to most of our current antimalarial therapies, including artemisinin combination therapies which are widely described as our last line of defense. Antimalarial agents with a novel mode of action are urgently required. Two Plasmodium falciparum aminopeptidases, PfA-M1 and PfA-M17, play crucial roles in the erythrocytic stage of infection and have been validated as potential antimalarial targets. Using compound-bound crystal structures of both enzymes, we have used a structure-guided approach to develop a novel series of inhibitors capable of potent inhibition of both PfA-M1 and PfA-M17 activity and parasite growth in culture. Herein we describe the design, synthesis, and evaluation of a series of hydroxamic acid-based inhibitors and demonstrate the compounds to be exciting new leads for the development of novel antimalarial therapeutics.

Published

2014

38. Fragment-based screening by X-ray crystallography, MS and isothermal titration calorimetry to identify PNMT (phenylethanolamine N-methyltransferase) inhibitors

Author

Hoan Vu, Kimberly M. Lovell, Brett M. Collins, Gary L. Grunewald, Michael J. McLeish, Nyssa Drinkwater, Sally-Ann Poulsen, Thomas E. Prisinzano, Jennifer L. Martin, and Kevin R. Criscione

Subjects

chemistry.chemical_classification, Models, Molecular, Benzimidazole, Binding Sites, Drug discovery, Stereochemistry, Phenylethanolamine N-Methyltransferase, Isothermal titration calorimetry, Cell Biology, Calorimetry, Ligand (biochemistry), Crystallography, X-Ray, Ligands, Biochemistry, Phenylethanolamine N-methyltransferase, Mass Spectrometry, Phenylethanolamine, chemistry.chemical_compound, Kinetics, Enzyme, chemistry, Transferase, Benzimidazoles, Enzyme Inhibitors, Molecular Biology

Abstract

CNS (central nervous system) adrenaline (epinephrine) is implicated in a wide range of physiological and pathological conditions. PNMT (phenylethanolamine N-methyltransferase) catalyses the final step in the biosynthesis of adrenaline, the conversion of noradrenaline (norepinephrine) to adrenaline by methylation. To help elucidate the role of CNS adrenaline, and to develop potential drug leads, potent, selective and CNS-active inhibitors are required. The fragment screening approach has advantages over other lead discovery methods including high hit rates, more efficient hits and the ability to sample chemical diversity more easily. In the present study we applied fragment-based screening approaches to the enzyme PNMT. We used crystallography as the primary screen and identified 12 hits from a small commercial library of 384 drug-like fragments. The hits include nine chemicals with two fused rings and three single-ring chemical systems. Eight of the hits come from three chemical classes: benzimidazoles (a known class of PNMT inhibitor), purines and quinolines. Nine of the hits have measurable binding affinities (∼5-700 μM) as determined by isothermal titration calorimetry and all nine have ligand efficiencies of 0.39 kcal/mol per heavy atom or better (1 kcal ≈4.184 kJ). We synthesized five elaborated benzimidazole compounds and characterized their binding to PNMT, showing for the first time how this class of inhibitors interact with the noradrenaline-binding site. Finally, we performed a pilot study with PNMT for fragment-based screening by MS showing that this approach could be used as a fast and efficient first-pass screening method prior to characterization of binding mode and affinity of hits. © The Authors Journal compilation © 2010 Biochemical Society.

Published

2010

39. Enzyme adaptation to inhibitor binding: a cryptic binding site in phenylethanolamine N-methyltransferase

Author

Jennifer L. Martin, Qian Wu, Christine L. Gee, Michael J. McLeish, Joel D. A. Tyndall, Nyssa Drinkwater, and Gary L. Grunewald

Subjects

Models, Molecular, Methyltransferase, Molecular model, Stereochemistry, Protein Conformation, Crystallography, X-Ray, chemistry.chemical_compound, Drug Discovery, Transferase, Binding site, chemistry.chemical_classification, Binding Sites, biology, Molecular Structure, Chemistry, Phenylethanolamine N-Methyltransferase, Active site, Isoquinolines, Phenylethanolamine N-methyltransferase, Phenylethanolamine, Enzyme, Mutation, biology.protein, Molecular Medicine, Thermodynamics, Crystallization, Protein Binding

Abstract

Shape complementarity is a fundamental principle of inhibitor design. Here we show that an enzyme for which the crystal structure has been determined (phenylethanolamine N-methyltransferase, PNMT) conceals a cryptic binding site. This site is revealed upon binding of inhibitors that are double the size of the physiological substrate. These large inhibitors are not predicted to bind in that they protrude through the accessible surface calculated from a PNMT/7-aminosulfonyl-1,2,3,4-tetrahydroisoquinoline (SK&F 29661) crystal structure, yet they are potent inhibitors of PNMT. We determined structures of the enzyme complexed with large inhibitors and found that the volume of the active site increases by 140 angstrom(3) upon binding. Changes in active site size and shape are brought about by unfavorable side chain conformations and rigid body helix motions. The energetic cost is modest, estimated at 2-3 kcal/mol from mutational analyses. Our findings further underline the importance of protein flexibility in structure-based inhibitor design studies.

Published

2007

40. Comparison of the binding of 3-fluoromethyl-7-sulfonyl-1,2,3,4-tetrahydroisoquinolines with their isosteric sulfonamides to the active site of phenylethanolamine N-methyltransferase

Author

Gary L. Grunewald, Jennifer L. Martin, Kevin R. Criscione, Rachel C. Regier, Christine L. Gee, Mitchell R. Seim, and Nyssa Drinkwater

Subjects

Male, Models, Molecular, Molecular model, Stereochemistry, In Vitro Techniques, Crystallography, X-Ray, Chemical synthesis, Sulfone, Rats, Sprague-Dawley, chemistry.chemical_compound, Radioligand Assay, Structure-Activity Relationship, Receptors, Adrenergic, alpha-2, Drug Discovery, Animals, Humans, Sulfones, Sulfonyl, chemistry.chemical_classification, Sulfonamides, Binding Sites, biology, Molecular Structure, Hydrogen bond, Phenylethanolamine N-Methyltransferase, Active site, Brain, Hydrogen Bonding, Stereoisomerism, Isoquinolines, Rats, Phenylethanolamine, chemistry, Lipophilicity, biology.protein, Molecular Medicine

Abstract

3-Fluoromethyl-7-(N-substituted aminosulfonyl)-1,2,3,4-tetrahydroisoquinolines (14, 16, and 18-22) are highly potent and selective inhibitors of phenylethanolamine N-methyltransferase (PNMT). Molecular modeling studies with 3-fluoromethyl-7-(N-alkyl aminosulfonyl)-1,2,3,4-tetrahydroisoquinolines, such as 16, suggested that the sulfonamide -NH- could form a hydrogen bond with the side chain of Lys57. However, SAR studies and analysis of the crystal structure of human PNMT (hPNMT) in complex with 7 indicated that the sulfonamide oxygens, and not the sulfonamide -NH-, formed favorable interactions with the enzyme. Thus, we hypothesized that replacement of the sulfonamide -NH- with a methylene group could result in compounds that would retain potency at PNMT and that would have increased lipophilicity, thus increasing the likelihood they will cross the blood brain barrier. A series of 3-fluoromethyl-7-sulfonyl-1,2,3,4-tetrahydroisoquinolines (23-30) were synthesized and evaluated for their PNMT inhibitory potency and affinity for the alpha2-adrenoceptor. A comparison of these compounds with their isosteric sulfonamides (14, 16, and 18-22) showed that the sulfones were more lipophilic but less potent than their corresponding sulfonamides. Sulfone 24 (hPNMT Ki = 1.3 microM) is the most potent compound in this series and is quite selective for PNMT versus the alpha2-adrenoceptor, but 24 is less potent than the corresponding sulfonamide, 16 (hPNMT Ki = 0.13 microM). We also report the crystal structure of hPNMT in complex with sulfonamide 15, from which a potential hydrogen bond acceptor within the hPNMT active site has been identified, the main chain carbonyl oxygen of Asn39. The interaction of this residue with the sulfonamide -NH- is likely responsible for much of the enhanced inhibitory potency of the sulfonamides versus the sulfones.

Published

2006

41. Human IgE flips between two acutely bent structuresviaan ensemble of extended conformations

Author

Andrew J. Beavil, Anthony H. Keeble, Michael John Wright, Alistair James Henry, Ben Cossins, James M. McDonnell, Brian J. Sutton, and Nyssa Drinkwater

Subjects

Molecular dynamics, Förster resonance energy transfer, biology, Structural Biology, Stereochemistry, Chemistry, Bent molecular geometry, B-cell receptor, biology.protein, Molecule, Antibody, Immunoglobulin E, Fragment crystallizable region

Abstract

Immunoglobulin E (IgE) antibodies mediate allergic reactions, and their binding to FcaRI is responsible for longterm sensitisation of mast cells and basophils [1]. Disruption of this interaction is a validated strategy for therapeutic intervention in allergic diseases including asthma [2]. IgE is known to display an acutely and asymmetrically bent conformation in the Fc region through which it binds to FcaRI; this bend becomes even more acute upon receptor engagement, as shown both crystallographically and in solution [3-7]. We report the crystal structure of a complex formed between IgE-Fc and two bound Fab fragments of a inhibitory anti-IgE antibody, and show that IgE-Fc can also adopt a totally extended conformation. The IgE-Fc has adopted a completely symmetrical conformation that requires an “unbending” of approximately 120° from the previously characterised structure. Molecular dynamics simulation reveals a series of stable conformations for free IgE-Fc that suggest a pathway from the acutely bent crystal structure through stable, extended conformations close to that seen in the Fab complex. We show by ITC, stoppedflow kinetic and FRET analyses that IgE-Fc adopts extended conformations in solution, and that these are an intrinsic property of IgEFc, not induced by Fab binding. We propose that IgE-Fc passes through these extended conformations as it flips between two bent conformations in which the CΣ2 domains fold back on opposite faces of the CΣ3-CΣ4 domains. The ability of IgE to exist in both bent and extended conformations may be essential for allergen recognition by IgE-Fc when bound to FcΣRI on the surface of mast cells, and as the B cell receptor respectively. Understanding the full range of conformations accessible to the free IgE molecule is also key to developing IgE-targeted therapies for allergic disease.

Published

2013

42. Fragment-based screening by X-ray crystallography, MS and isothermal titration calorimetry to identify PNMT (phenylethanolamine N-methyltransferase) inhibitors.

Author

Nyssa Drinkwater, Hoan Vu, Kimberly M. Lovell, Kevin R. Criscione, Brett M. Collins, Thomas E. Prisinzano, Sally‑Ann Poulsen, Michael J. McLeish, Gary L. Grunewald, and Jennifer L. Martin

Subjects

*ENZYME inhibitors, *X-ray crystallography, *VOLUMETRIC analysis, *CALORIMETRY, *METHYLTRANSFERASES, *CENTRAL nervous system, *ADRENALINE

Abstract

CNS (central nervous system) adrenaline (epinephrine) is implicated in a wide range of physiological and pathological conditions. PNMT (phenylethanolamine N-methyltransferase) catalyses the final step in the biosynthesis of adrenaline, the conversion of noradrenaline (norepinephrine) to adrenaline by methylation. To help elucidate the role of CNS adrenaline, and to develop potential drug leads, potent, selective and CNS-active inhibitors are required. The fragment screening approach has advantages over other lead discovery methods including high hit rates, more efficient hits and the ability to sample chemical diversity more easily. In the present study we applied fragment-based screening approaches to the enzyme PNMT. We used crystallography as the primary screen and identified 12 hits from a small commercial library of 384 drug-like fragments. The hits include nine chemicals with two fused rings and three single-ring chemical systems. Eight of the hits come from three chemical classes: benzimidazoles (a known class of PNMT inhibitor), purines and quinolines. Nine of the hits have measurable binding affinities (~5–700 μM) as determined by isothermal titration calorimetry and all nine have ligand efficiencies of 0.39 kcal/mol per heavy atom or better (1 kcal≈4.184 kJ). We synthesized five elaborated benzimidazole compounds and characterized their binding to PNMT, showing for the first time how this class of inhibitors interact with the noradrenaline-binding site. Finally, we performed a pilot study with PNMT for fragment-based screening by MS showing that this approach could be used as a fast and efficient first-pass screening method prior to characterization of binding mode and affinity of hits. [ABSTRACT FROM AUTHOR]

Published

2010

43. Molecular recognition of physiological substrate noradrenaline by the adrenaline-synthesizing enzyme PNMT and factors influencing its methyltransferase activity.

Author

Nyssa Drinkwater, Christine L. Gee, Munish Puri, Kevin R. Criscione, Michael J. McLeish, Gary L. Grunewald, and Jennifer L. Martin

Subjects

*MOLECULAR recognition, *NORADRENALINE, *METHYLTRANSFERASES, *OXIDIZING agents, *LIGANDS (Biochemistry), *CATALYSIS, *COMPLEX compounds, *OXIDATION

Abstract

Substrate specificity is critically important for enzyme catalysis. In the adrenaline-synthesizing enzyme PNMT (phenylethanolamine N-methyltransferase), minor changes in substituents can convert substrates into inhibitors. Here we report the crystal structures of six human PNMT complexes, including the first structure of the enzyme in complex with its physiological ligand R-noradrenaline. Determining this structure required rapid soak methods because of the tendency for noradrenaline to oxidize. Comparison of the PNMT–noradrenaline complex with the previously determined PNMT–p-octopamine complex demonstrates that these two substrates form almost equivalent interactions with the enzyme and show that p-octopamine is a valid model substrate for PNMT. The crystal structures illustrate the adaptability of the PNMT substrate binding site in accepting multi-fused ring systems, such as substituted norbornene, as well as noradrenochrome, the oxidation product of noradrenaline. These results explain why only a subset of ligands recognized by PNMT are methylated by the enzyme; bulky substituents dictate the binding orientation of the ligand and can thereby place the acceptor amine too far from the donor methyl group for methylation to occur. We also show how the critical Glu185 catalytic residue can be replaced by aspartic acid with a loss of only 10-fold in catalytic efficiency. This is because protein backbone movements place the Asp185 carboxylate almost coincident with the carboxylate of Glu185. Conversely, replacement of Glu185 by glutamine reduces catalytic efficiency almost 300-fold, not only because of the loss of charge, but also because the variant residue does not adopt the same conformation as Glu185. [ABSTRACT FROM AUTHOR]

Published

2009

44. Enzyme Adaptation to Inhibitor Binding: A Cryptic Binding Site in Phenylethanolamine N-Methyltransferase.

Author

Christine L. Gee, Nyssa Drinkwater, Joel D. A. Tyndall, Gary L. Grunewald, Qian Wu, Michael J. McLeish, and Jennifer L. Martin

Published

2007