Your search keyword '"Scanlon MJ"' showing total 8 results

1. Rapid Elaboration of Fragments into Leads Applied to Bromodomain-3 Extra-Terminal Domain.

Author

Adams LA, Wilkinson-White LE, Gunzburg MJ, Headey SJ, Mohanty B, Scanlon MJ, Capuano B, Mackay JP, and Doak BC

Subjects

Structure-Activity Relationship, Protein Domains, Ligands, Proteins metabolism, Drug Design

Abstract

The development of low-affinity fragment hits into higher-affinity leads is a major hurdle in fragment-based drug design. Here, we demonstrate the Rapid Elaboration of Fragments into Leads (REFiL) by applying an integrated workflow that provides a systematic approach to generate higher-affinity binders without the need for structural information. The workflow involves the selection of commercial analogues of fragment hits to generate preliminary structure-activity relationships. This is followed by parallel microscale chemistry using chemoinformatically designed reagent libraries to rapidly explore chemical diversity. After a fragment screen against bromodomain-3 extra-terminal (BRD3-ET) domain, we applied the REFiL workflow, which allowed us to develop a series of ligands that bind to BRD3-ET. With REFiL, we were able to rapidly improve binding affinity > 30-fold. REFiL can be applied readily to a broad range of proteins without the need for a structure, allowing the efficient evolution of low-affinity fragments into higher-affinity leads and chemical probes.

Published

2023

2. Rapid Elaboration of Fragments into Leads by X-ray Crystallographic Screening of Parallel Chemical Libraries (REFiL X ).

Author

Bentley MR, Ilyichova OV, Wang G, Williams ML, Sharma G, Alwan WS, Whitehouse RL, Mohanty B, Scammells PJ, Heras B, Martin JL, Totsika M, Capuano B, Doak BC, and Scanlon MJ

Subjects

Crystallography, X-Ray, Drug Evaluation, Preclinical, Models, Molecular, Molecular Conformation, Small Molecule Libraries pharmacology, Solubility, Small Molecule Libraries chemistry

Abstract

A bottleneck in fragment-based lead development is the lack of systematic approaches to elaborate the initial fragment hits, which usually bind with low affinity to their target. Herein, we describe an analysis using X-ray crystallography of a diverse library of compounds prepared using microscale parallel synthesis. This approach yielded an 8-fold increase in affinity and detailed structural information for the resulting complex, providing an efficient and broadly applicable approach to early fragment development.

Published

2020

3. Design, Synthesis, and Characterization of Cyclic Peptidomimetics of the Inducible Nitric Oxide Synthase Binding Epitope That Disrupt the Protein-Protein Interaction Involving SPRY Domain-Containing Suppressor of Cytokine Signaling Box Protein (SPSB) 2 and Inducible Nitric Oxide Synthase.

Author

Harjani JR, Yap BK, Leung EW, Lucke A, Nicholson SE, Scanlon MJ, Chalmers DK, Thompson PE, Norton RS, and Baell JB

Subjects

Animals, Binding Sites drug effects, Macrophages drug effects, Macrophages metabolism, Mice, Models, Molecular, Molecular Conformation, Molecular Dynamics Simulation, Nitric Oxide Synthase Type II metabolism, Peptides chemical synthesis, Peptides chemistry, Peptidomimetics chemical synthesis, Peptidomimetics chemistry, Protein Binding drug effects, Suppressor of Cytokine Signaling Proteins metabolism, B30.2-SPRY Domain drug effects, Drug Design, Nitric Oxide Synthase Type II antagonists & inhibitors, Peptides pharmacology, Peptidomimetics pharmacology, Suppressor of Cytokine Signaling Proteins antagonists & inhibitors

Abstract

SPRY domain-containing suppressor of cytokine signaling box protein (SPSB) 2-deficient macrophages have been found to exhibit prolonged expression of inducible nitric oxide synthase (iNOS) and enhanced killing of persistent pathogens, suggesting that inhibitors of the SPSB2-iNOS interaction have potential as novel anti-infectives. In this study, we describe the design, synthesis, and characterization of cyclic peptidomimetic inhibitors of the SPSB2-iNOS interaction constrained by organic linkers to improve stability and druggability. SPR, ITC, and (19)F NMR analyses revealed that the most potent cyclic peptidomimetic bound to the iNOS binding site of SPSB2 with low nanomolar affinity (KD 29 nM), a 10-fold improvement over that of the linear peptide DINNN (KD 318 nM), and showed strong inhibition of SPSB2-iNOS interaction in macrophage cell lysates. This study exemplifies a novel approach to cyclize a Type II β-turn linear peptide and provides a foundation for future development of this group of inhibitors as new anti-infectives.

Published

2016

4. Promiscuous 2-aminothiazoles (PrATs): a frequent hitting scaffold.

Author

Devine SM, Mulcair MD, Debono CO, Leung EW, Nissink JW, Lim SS, Chandrashekaran IR, Vazirani M, Mohanty B, Simpson JS, Baell JB, Scammells PJ, Norton RS, and Scanlon MJ

Subjects

Drug Discovery, High-Throughput Screening Assays, Magnetic Resonance Spectroscopy, Molecular Structure, Surface Plasmon Resonance, Thiazoles chemistry

Abstract

We have identified a class of molecules, known as 2-aminothiazoles (2-ATs), as frequent-hitting fragments in biophysical binding assays. This was exemplified by 4-phenylthiazol-2-amine being identified as a hit in 14/14 screens against a diverse range of protein targets, suggesting that this scaffold is a poor starting point for fragment-based drug discovery. This prompted us to analyze this scaffold in the context of an academic fragment library used for fragment-based drug discovery (FBDD) and two larger compound libraries used for high-throughput screening (HTS). This analysis revealed that such "promiscuous 2-aminothiazoles" (PrATs) behaved as frequent hitters under both FBDD and HTS settings, although the problem was more pronounced in the fragment-based studies. As 2-ATs are present in known drugs, they cannot necessarily be deemed undesirable, but the combination of their promiscuity and difficulties associated with optimizing them into a lead compound makes them, in our opinion, poor scaffolds for fragment libraries.

Published

2015

5. Ligand-induced conformational change of Plasmodium falciparum AMA1 detected using 19F NMR.

Author

Ge X, MacRaild CA, Devine SM, Debono CO, Wang G, Scammells PJ, Scanlon MJ, Anders RF, Foley M, and Norton RS

Subjects

Antigens, Protozoan genetics, Antimalarials chemistry, Fluorine Radioisotopes, Ligands, Membrane Proteins antagonists & inhibitors, Membrane Proteins genetics, Mutation, Nuclear Magnetic Resonance, Biomolecular, Protein Binding, Protein Conformation, Protozoan Proteins antagonists & inhibitors, Protozoan Proteins genetics, Recombinant Proteins chemistry, Recombinant Proteins genetics, Antigens, Protozoan chemistry, Membrane Proteins chemistry, Plasmodium falciparum metabolism, Protozoan Proteins chemistry

Abstract

We established an efficient means of probing ligand-induced conformational change in the malaria drug target AMA1 using 19F NMR. AMA1 was labeled with 5-fluorotryptophan (5F-Trp), and the resulting 5F-Trp resonances were assigned by mutagenesis of the native Trp residues. By introducing additional Trp residues at strategic sites within a ligand-responsive loop, we detected distinct conformational consequences when various peptide and small-molecule ligands bound AMA1. Our results demonstrate an increase in flexibility in this loop caused by the native ligand, as inferred from, but not directly observed in, crystal structures. In addition, we found evidence for long-range allosteric changes in AMA1 that are not observed crystallographically. This method will be valuable in ongoing efforts to identify and characterize therapeutically relevant inhibitors of protein-protein interactions involving AMA1 and is generalizable to the study of ligand-induced conformational change in a wide range of other drug targets.

Published

2014

6. Probing the fibrate binding specificity of rat liver fatty acid binding protein.

Author

Chuang S, Velkov T, Horne J, Wielens J, Chalmers DK, Porter CJ, and Scanlon MJ

Subjects

Animals, Binding Sites, Carboxylic Acids chemistry, Clofibric Acid chemistry, Clofibric Acid pharmacology, Esters chemistry, Fatty Acid-Binding Proteins chemistry, Fenofibrate analogs & derivatives, Fenofibrate chemistry, Fenofibrate metabolism, Hypolipidemic Agents chemistry, Hypolipidemic Agents pharmacology, Ligands, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Conformation, Rats, Spectrometry, Fluorescence, Substrate Specificity, Temperature, Thermodynamics, Clofibric Acid metabolism, Fatty Acid-Binding Proteins metabolism, Hypolipidemic Agents metabolism, Liver metabolism

Abstract

Liver-fatty acid binding protein (L-FABP) is found in high levels in enterocytes and is involved in cytosolic solubilization of fatty acids. In addition, L-FABP has been shown to bind endogenous and exogenous lipophilic compounds, suggesting that it may also play a role in modulating their absorption and disposition within enterocytes. Previously, we have described binding of L-FABP to a range of drugs, including a series of fibrates. In the present study, we have generated structural models of L-FABP-fibrate complexes and undertaken thermodynamic analysis of the binding of fibrates containing either a carboxylic acid or ester functionality. Analysis of the current data reveals that both the location and the energetics of binding are different for fibrates that contain a carboxylate compared to those that do not. As such, the data presented in this study suggest potential mechanisms that underpin molecular recognition and dictate specificity in the interaction between fibrates and L-FABP.

Published

2009

7. Characterization of the drug binding specificity of rat liver fatty acid binding protein.

Author

Chuang S, Velkov T, Horne J, Porter CJ, and Scanlon MJ

Subjects

Anilino Naphthalenesulfonates, Animals, Ligands, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Structure, Pharmaceutical Preparations metabolism, Protein Binding, Rats, Spectrometry, Fluorescence, Substrate Specificity, Fatty Acid-Binding Proteins chemistry, Fatty Acid-Binding Proteins metabolism, Pharmaceutical Preparations chemistry

Abstract

Liver-fatty acid binding protein (L-FABP) is found in high levels in enterocytes and is involved in the cytosolic solubilization of fatty acids during fat absorption. In the current studies, the interaction of L-FABP with a range of lipophilic drugs has been evaluated to explore the potential for L-FABP to provide an analogous function during the absorption of lipophilic drugs. Binding affinity for L-FABP was assessed by displacement of a fluorescent marker, 1-anilinonaphthalene-8-sulfonic acid (ANS), and the binding site location was determined via nuclear magnetic resonance chemical shift perturbation studies. It was found that the majority of drugs bound to L-FABP at two sites, with the internal site generally having a higher affinity for the compounds tested. Furthermore, in contrast to the interaction of L-FABP with fatty acids, it was demonstrated that a terminal carboxylate is not required for specific binding of lipophilic drugs at the internal site of L-FABP.

Published

2008

8. Conformational selection of inhibitors and substrates by proteolytic enzymes: implications for drug design and polypeptide processing.

Author

Fairlie DP, Tyndall JD, Reid RC, Wong AK, Abbenante G, Scanlon MJ, March DR, Bergman DA, Chai CL, and Burkett BA

Subjects

Amino Acid Sequence, Binding Sites, Chromatography, High Pressure Liquid, Circular Dichroism, Crystallography, X-Ray, Drug Design, Endopeptidases metabolism, HIV Protease chemistry, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Sequence Data, Molecular Structure, Protein Binding, Protein Structure, Secondary, Substrate Specificity, Endopeptidases chemistry, Protease Inhibitors chemistry

Abstract

Inhibitors of proteolytic enzymes (proteases) are emerging as prospective treatments for diseases such as AIDS and viral infections, cancers, inflammatory disorders, and Alzheimer's disease. Generic approaches to the design of protease inhibitors are limited by the unpredictability of interactions between, and structural changes to, inhibitor and protease during binding. A computer analysis of superimposed crystal structures for 266 small molecule inhibitors bound to 48 proteases (16 aspartic, 17 serine, 8 cysteine, and 7 metallo) provides the first conclusive proof that inhibitors, including substrate analogues, commonly bind in an extended beta-strand conformation at the active sites of all these proteases. Representative superimposed structures are shown for (a) multiple inhibitors bound to a protease of each class, (b) single inhibitors each bound to multiple proteases, and (c) conformationally constrained inhibitors bound to proteases. Thus inhibitor/substrate conformation, rather than sequence/composition alone, influences protease recognition, and this has profound implications for inhibitor design. This conclusion is supported by NMR, CD, and binding studies for HIV-1 protease inhibitors/substrates which, when preorganized in an extended conformation, have significantly higher protease affinity. Recognition is dependent upon conformational equilibria since helical and turn peptide conformations are not processed by proteases. Conformational selection explains the resistance of folded/structured regions of proteins to proteolytic degradation, the susceptibility of denatured proteins to processing, and the higher affinity of conformationally constrained 'extended' inhibitors/substrates for proteases. Other approaches to extended inhibitor conformations should similarly lead to high-affinity binding to a protease.

Published

2000