Your search keyword '"Scammells, PJ"' showing total 175 results

1. Genetic and chemical validation of Plasmodium falciparum aminopeptidase PfA-M17 as a drug target in the hemoglobin digestion pathway

Author

Edgar, RCS, Siddiqui, G, Hjerrild, K, Malcolm, TR, Vinh, NB, Webb, CT, Holmes, C, MacRaild, CA, Chernih, HC, Suen, WW, Counihan, NA, Creek, DJ, Scammells, PJ, McGowan, S, de Koning-Ward, TF, Edgar, RCS, Siddiqui, G, Hjerrild, K, Malcolm, TR, Vinh, NB, Webb, CT, Holmes, C, MacRaild, CA, Chernih, HC, Suen, WW, Counihan, NA, Creek, DJ, Scammells, PJ, McGowan, S, and de Koning-Ward, TF

Abstract

Plasmodium falciparum, the causative agent of malaria, remains a global health threat as parasites continue to develop resistance to antimalarial drugs used throughout the world. Accordingly, drugs with novel modes of action are desperately required to combat malaria. P. falciparum parasites infect human red blood cells where they digest the host's main protein constituent, hemoglobin. Leucine aminopeptidase PfA-M17 is one of several aminopeptidases that have been implicated in the last step of this digestive pathway. Here, we use both reverse genetics and a compound specifically designed to inhibit the activity of PfA-M17 to show that PfA-M17 is essential for P. falciparum survival as it provides parasites with free amino acids for growth, many of which are highly likely to originate from hemoglobin. We further show that loss of PfA-M17 results in parasites exhibiting multiple digestive vacuoles at the trophozoite stage. In contrast to other hemoglobin-degrading proteases that have overlapping redundant functions, we validate PfA-M17 as a potential novel drug target.

Published

2022

2. Development and Application of Subtype-Selective Fluorescent Antagonists for the Study of the Human Adenosine A1 Receptor in Living Cells

Author

Comeo, E, Trinh, P, Nguyen, AT, Nowell, CJ, Kindon, ND, Soave, M, Stoddart, LA, White, JM, Hill, SJ, Kellam, B, Halls, ML, May, LT, Scammells, PJ, Comeo, E, Trinh, P, Nguyen, AT, Nowell, CJ, Kindon, ND, Soave, M, Stoddart, LA, White, JM, Hill, SJ, Kellam, B, Halls, ML, May, LT, and Scammells, PJ

Abstract

The adenosine A1 receptor (A1AR) is a G-protein-coupled receptor (GPCR) that provides important therapeutic opportunities for a number of conditions including congestive heart failure, tachycardia, and neuropathic pain. The development of A1AR-selective fluorescent ligands will enhance our understanding of the subcellular mechanisms underlying A1AR pharmacology facilitating the development of more efficacious and selective therapies. Herein, we report the design, synthesis, and application of a novel series of A1AR-selective fluorescent probes based on 8-functionalized bicyclo[2.2.2]octylxanthine and 3-functionalized 8-(adamant-1-yl) xanthine scaffolds. These fluorescent conjugates allowed quantification of kinetic and equilibrium ligand binding parameters using NanoBRET and visualization of specific receptor distribution patterns in living cells by confocal imaging and total internal reflection fluorescence (TIRF) microscopy. As such, the novel A1AR-selective fluorescent antagonists described herein can be applied in conjunction with a series of fluorescence-based techniques to foster understanding of A1AR molecular pharmacology and signaling in living cells.

Published

2021

3. 6-Phenylpyrimidin-4-ones as Positive Allosteric Modulators at the M1 mAChR: The Determinants of Allosteric Activity

Author

Jorg, M, van der Westhuizen, ET, Khajehali, E, Burger, WAC, White, JM, Choy, KHC, Tobin, AB, Sexton, PM, Valant, C, Capuano, B, Christopoulos, A, Scammells, PJ, Jorg, M, van der Westhuizen, ET, Khajehali, E, Burger, WAC, White, JM, Choy, KHC, Tobin, AB, Sexton, PM, Valant, C, Capuano, B, Christopoulos, A, and Scammells, PJ

Abstract

Targeting allosteric sites of the M1 muscarinic acetylcholine receptor (mAChR) is an enticing approach to overcome the lack of receptor subtype selectivity observed with orthosteric ligands. This is a promising strategy for obtaining novel therapeutics to treat cognitive deficits observed in Alzheimer’s disease and schizophrenia, while reducing the peripheral side effects such as seen in the current treatment regimes, which are non-subtype selective. We previously described compound 2, the first positive allosteric modulator (PAM) of the M1 mAChR based on a 6-phenylpyrimidin-4-one scaffold, which has been further developed in this study. Herein, we present the synthesis, characterization, and pharmacological evaluation of a series of 6-phenylpyrimidin-4-ones with modifications to the 4-(1-methylpyrazol-4-yl)benzyl pendant. Selected compounds, BQCA, 1, 2, 9i, 13, 14b, 15c, and 15d, were further profiled in terms of their allosteric affinity, cooperativity with acetylcholine (ACh), and intrinsic efficacy. Additionally, 2 and 9i were tested in mouse primary cortical neurons, displaying various degrees of intrinsic agonism and potentiation of the acetylcholine response. Overall, the results suggest that the pendant moiety is important for allosteric binding affinity and the direct agonistic efficacy of the 6-phenylpyrimidin-4-one based M1 mAChR PAMs.

Published

2019

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

Author

Akter, M, Drinkwater, N, Devine, SM, Drew, SC, Krishnarjuna, B, Debono, CO, Wang, G, Scanlon, MJ, Scammells, PJ, McGowan, S, MacRaild, CA, Norton, RS, Akter, M, Drinkwater, N, Devine, SM, Drew, SC, Krishnarjuna, B, Debono, CO, Wang, G, Scanlon, MJ, Scammells, PJ, McGowan, S, MacRaild, CA, and Norton, RS

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

2019

5. The action of a negative allosteric modulator at the dopamine D2 receptor is dependent upon sodium ions

Author

Draper-Joyce, CJ, Verma, RK, Michino, M, Shonberg, J, Kopinathan, A, Herenbrink, CK, Scammells, PJ, Capuano, B, Abramyan, AM, Thal, DM, Javitch, JA, Christopoulos, A, Shi, L, Lane, JR, Draper-Joyce, CJ, Verma, RK, Michino, M, Shonberg, J, Kopinathan, A, Herenbrink, CK, Scammells, PJ, Capuano, B, Abramyan, AM, Thal, DM, Javitch, JA, Christopoulos, A, Shi, L, and Lane, JR

Abstract

Sodium ions (Na+) allosterically modulate the binding of orthosteric agonists and antagonists to many class A G protein-coupled receptors, including the dopamine D2 receptor (D2R). Experimental and computational evidences have revealed that this effect is mediated by the binding of Na+ to a conserved site located beneath the orthosteric binding site (OBS). SB269652 acts as a negative allosteric modulator (NAM) of the D2R that adopts an extended bitopic pose, in which the tetrahydroisoquinoline moiety interacts with the OBS and the indole-2-carboxamide moiety occupies a secondary binding pocket (SBP). In this study, we find that the presence of a Na+ within the conserved Na+-binding pocket is required for the action of SB269652. Using fragments of SB269652 and novel full-length analogues, we show that Na+ is required for the high affinity binding of the tetrahydroisoquinoline moiety within the OBS, and that the interaction of the indole-2-carboxamide moiety with the SBP determines the degree of Na+-sensitivity. Thus, we extend our understanding of the mode of action of this novel class of NAM by showing it acts synergistically with Na+ to modulate the binding of orthosteric ligands at the D2R, providing opportunities for fine-tuning of modulatory effects in future allosteric drug design efforts.

Published

2018

6. Probing the binding site of novel selective positive allosteric modulators at the M1 muscarinic acetylcholine receptor

Author

Khajehali, E, Valant, C, Jorg, M, Tobin, AB, Conn, PJ, Lindsley, CW, Sexton, PM, Scammells, PJ, Christopoulos, A, Khajehali, E, Valant, C, Jorg, M, Tobin, AB, Conn, PJ, Lindsley, CW, Sexton, PM, Scammells, PJ, and Christopoulos, A

Abstract

Subtype-selective allosteric modulation of the M1 muscarinic acetylcholine (ACh) receptor (M1 mAChR) is an attractive approach for the treatment of numerous disorders, including cognitive deficits. The discovery of benzyl quinolone carboxylic acid, BQCA, a selective M1 mAChR positive allosteric modulator (PAM), spurred the subsequent development of newer generation M1 PAMs representing diverse chemical scaffolds, different pharmacodynamic properties and, in some instances, improved pharmacokinetics. Key exemplar molecules from such efforts include PF-06767832 (N-((3R,4S)-3-hydroxytetrahydro-2H-pyran-4-yl)-5-methyl-4-(4-(thiazol-4-yl)benzyl)pyridine-2-carboxamide), VU6004256 (4,6-difluoro-N-(1S,2S)-2-hydroxycyclohexyl-1-((6-(1-methyl-1H-pyrazol-4-yl)pyridine-3-yl)methyl)-1H-indole-3-carboxamide) and MIPS1780 (3-(2-hydroxycyclohexyl)-6-(2-((4-(1-methyl-1H-pyrazol-4-yl)-benzyl)oxy)phenyl)pyrimidin-4(3H)-one). Given these diverse scaffolds and pharmacodynamics, the current study combined pharmacological analysis and site-directed mutagenesis to explore the potential binding site and function of newer M1 mAChR PAMs relative to BQCA. Interestingly, the mechanism of action of the novel PAMs was consistent with a common model of allostery, as previously described for BQCA. Key residues involved in the activity of BQCA, including Y179 in the second extracellular loop (ECL) and W4007.35 in transmembrane domain (TM) 7, were critical for the activity of all PAMs tested. Overall, our data indicate that structurally distinct PAMs share a similar binding site with BQCA, specifically, an extracellular allosteric site defined by residues in TM2, TM7 and ECL2. These findings provide valuable insights into the structural basis underlying modulator binding, cooperativity and signaling at the M1 mAChR, which is essential for the rational design of PAMs with tailored pharmacological properties.

Published

2018

7. A new mechanism of allostery in a G protein-coupled receptor dimer

Author

Lane, JR, Donthamsetti, P, Shonberg, J, Draper-Joyce, CJ, Dentry, S, Michino, M, Shi, L, Lopez, L, Scammells, PJ, Capuano, B, Sexton, PM, Javitch, JA, Christopoulos, A, Lane, JR, Donthamsetti, P, Shonberg, J, Draper-Joyce, CJ, Dentry, S, Michino, M, Shi, L, Lopez, L, Scammells, PJ, Capuano, B, Sexton, PM, Javitch, JA, and Christopoulos, A

Abstract

SB269652 is to our knowledge the first drug-like allosteric modulator of the dopamine D2 receptor (D2R), but it contains structural features associated with orthosteric D2R antagonists. Using a functional complementation system to control the identity of individual protomers within a dimeric D2R complex, we converted the pharmacology of the interaction between SB269652 and dopamine from allosteric to competitive by impairing ligand binding to one of the protomers, indicating that the allostery requires D2R dimers. Additional experiments identified a 'bitopic' pose for SB269652 extending from the orthosteric site into a secondary pocket at the extracellular end of the transmembrane (TM) domain, involving TM2 and TM7. Engagement of this secondary pocket was a requirement for the allosteric pharmacology of SB269652. This suggests a new mechanism whereby a bitopic ligand binds in an extended pose on one G protein-coupled receptor protomer to allosterically modulate the binding of a ligand to the orthosteric site of a second protomer.

Published

2014

8. Synthesis, molecular structure, NMR spectroscopic and computational analysis of a selective adenosine A2A antagonist, ZM 241385

Author

Joerg, M, Agostino, M, Yuriev, E, Mak, FS, Miller, ND, White, JM, Scammells, PJ, Capuano, B, Joerg, M, Agostino, M, Yuriev, E, Mak, FS, Miller, ND, White, JM, Scammells, PJ, and Capuano, B

Published

2013

9. Synthesis and structure-activity relationships of phosphonic arginine mimetics as inhibitors of the M1 and M17 aminopeptidases from plasmodium falciparum

Author

Kannan Sivaraman, K, Paiardini, A, Sieńczyk, M, Ruggeri, C, Oellig, CA, Dalton, JP, Scammells, PJ, Drag, M, McGowan, S, Kannan Sivaraman, K, Paiardini, A, Sieńczyk, M, Ruggeri, C, Oellig, CA, Dalton, JP, Scammells, PJ, Drag, M, and McGowan, S

Abstract

The malaria parasite Plasmodium falciparum employs two metallo- aminopeptidases, PfA-M1 and PfA-M17, which are essential for parasite survival. Compounds that inhibit the activity of either enzyme represent leads for the development of new antimalarial drugs. Here we report the synthesis and structure-activity relationships of a small library of phosphonic acid arginine mimetics that probe the S1 pocket of both enzymes and map the necessary interactions that would be important for a dual inhibitor. © 2013 American Chemical Society.

Published

2013

10. Crystal structure of (4-bromonaphthalen-2-yl) acetonitrile, C12H8BrN

Author

Duthie, Andrew, Scammells, PJ, Tiekink, ERT, Katsifis, A, Duthie, Andrew, Scammells, PJ, Tiekink, ERT, and Katsifis, A

Published

2001

11. Synthesis of 2-Substituted Pyrazolo[3,4-d]pyrimidines

Author

Quinn, RJ, primary, Scammells, PJ, additional, Kennard, CHL, additional, and Smith, G, additional

Published

1991

12. Mono-α-carbamoylethylthio-Substituted Pyrazolo[3,4-d]pyrimidines: the Position of Substitution

Author

Quinn, RJ, primary, Scammells, PJ, additional, and Tucker, DJ, additional

Published

1991

13. 4-Amino-1-phenylpyrazolo[3,4-d]pyrimidin-6(5h)-one, an Isoguanosine Analog

Author

Quinn, RJ, primary and Scammells, PJ, additional

Published

1991

14. Synthesis of 5-Aminopyrazole-4-carbonitriles

Author

Dooley, MJ, Quinn, RJ, and Scammells, PJ

Abstract

A one-pot reaction between substituted hydrazines, malononitrile and triethyl orthoformate leads directly to the formation of 1-substituted 5-aminopyrazole-4-carbonitriles. The scope and limitations of this synthetic procedure are discussed in relation to the well established synthesis of these compounds via substituted hydrazines and ethoxymethylenemalononitrile.

Published

1989

15. Discovery of 2-Methyl-5-(1 H -pyrazol-4-yl)pyridines and Related Heterocycles as Promising M 4 mAChR Positive Allosteric Modulators for the Treatment of Neurocognitive Disorders.

Author

Liu B, Thompson G, Jörg M, Barnes N, Thal DM, Christopoulos A, Capuano B, Valant C, and Scammells PJ

Subjects

Allosteric Regulation drug effects, Humans, Animals, Cricetulus, Neurocognitive Disorders drug therapy, Neurocognitive Disorders metabolism, CHO Cells, Structure-Activity Relationship, Drug Discovery, beta-Arrestins metabolism, Pyrazoles pharmacology, Pyrazoles chemistry, Pyrazoles chemical synthesis, Pyrazoles therapeutic use, Pyridines pharmacology, Pyridines chemical synthesis, Pyridines chemistry, Receptor, Muscarinic M4 agonists, Receptor, Muscarinic M4 metabolism

Abstract

The M 4 muscarinic acetylcholine receptor (mAChR) is a biological target for neurocognitive disorders. Compound 1 is an ago -PAM for the M 4 mAChR. Herein, we report the design, synthesis, and evaluation of novel putative M 4 mAChR PAMs based on 1 . These analogs were screened and then fully characterized in two functional assays (G oB protein activation and CAMYEL activation) to quantify their allosteric and ago -PAM properties against ACh. A selection of 7 M 4 PAMs were assessed for their ability to modulate ACh-mediated β-arrestin recruitment and revealed 4 distinct clusters of M 4 PAM activity: (1) analogs similar to 1 ( 24d ), (2) analogs demonstrating only allosteric agonism ( 23d ), (3) analogs with increased allosteric properties in CAMYEL activation ( 23b / 23f and 24a / 24b ), and (4) analogs with a biased modulatory effect toward β-arrestin recruitment ( 23i ). These novel M 4 chemical tools disclose discrete molecular determinants, allowing further interrogation of the therapeutic roles of cAMP and β-arrestin pathways in neurocognitive disorders.

Published

2024

16. Ligand-Directed Labeling of the Adenosine A 1 Receptor in Living Cells.

Author

Comeo E, Goulding J, Lin CY, Groenen M, Woolard J, Kindon ND, Harwood CR, Platt S, Briddon SJ, Kilpatrick LE, Scammells PJ, Hill SJ, and Kellam B

Subjects

Ligands, Humans, Animals, Ganglia, Spinal metabolism, Ganglia, Spinal cytology, HEK293 Cells, Neurons metabolism, Receptor, Adenosine A1 metabolism, Receptor, Adenosine A1 chemistry, Fluorescent Dyes chemistry

Abstract

The study of protein function and dynamics in their native cellular environment is essential for progressing fundamental science. To overcome the requirement of genetic modification of the protein or the limitations of dissociable fluorescent ligands, ligand-directed (LD) chemistry has most recently emerged as a complementary, bioorthogonal approach for labeling native proteins. Here, we describe the rational design, development, and application of the first ligand-directed chemistry approach for labeling the A 1 AR in living cells. We pharmacologically demonstrate covalent labeling of A 1 AR expressed in living cells while the orthosteric binding site remains available. The probes were imaged using confocal microscopy and fluorescence correlation spectroscopy to study A 1 AR localization and dynamics in living cells. Additionally, the probes allowed visualization of the specific localization of A 1 ARs endogenously expressed in dorsal root ganglion (DRG) neurons. LD probes developed here hold promise for illuminating ligand-binding, receptor signaling, and trafficking of the A 1 AR in more physiologically relevant environments.

Published

2024

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

Author

Edgar RCS, Malcolm TR, Siddiqui G, Giannangelo C, Counihan NA, Challis M, Duffy S, Chowdhury M, Marfurt J, Dans M, Wirjanata G, Noviyanti R, Daware K, Suraweera CD, Price RN, Wittlin S, Avery VM, Drinkwater N, Charman SA, Creek DJ, de Koning-Ward TF, Scammells PJ, and McGowan S

Subjects

Animals, Mice, Drug Resistance, Humans, Malaria, Falciparum drug therapy, Malaria, Falciparum parasitology, Protozoan Proteins antagonists & inhibitors, Protozoan Proteins metabolism, Protozoan Proteins genetics, Female, Antimalarials pharmacology, Plasmodium falciparum drug effects, Plasmodium falciparum enzymology, Plasmodium vivax drug effects, Plasmodium vivax enzymology, Aminopeptidases antagonists & inhibitors, Aminopeptidases metabolism

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., Competing Interests: The authors declare no conflict of interest.

Published

2024

18. Design, synthesis and evaluation of novel 2-phenyl-3-(1H-pyrazol-4-yl)pyridine positive allosteric modulators for the M 4 mAChR.

Author

Jörg M, van der Westhuizen ET, Lu Y, Christopher Choy KH, Shackleford DM, Khajehali E, Tobin AB, Thal DM, Capuano B, Christopoulos A, Valant C, and Scammells PJ

Subjects

Mice, Animals, Cricetinae, Allosteric Regulation, Pyridines pharmacology, Pyridines chemistry, Signal Transduction, CHO Cells, Receptors, Muscarinic metabolism, Acetylcholine metabolism

Abstract

Translation of muscarinic acetylcholine receptor (mAChR) agonists into clinically used therapeutic agents has been difficult due to their poor subtype selectivity. M 4 mAChR subtype-selective positive allosteric modulators (PAMs) may provide better therapeutic outcomes, hence investigating their detailed pharmacological properties is crucial to advancing them into the clinic. Herein, we report the synthesis and comprehensive pharmacological evaluation of M 4 mAChR PAMs structurally related to 1e, Me-C-c, [ 11 C]MK-6884 and [ 18 F]12. Our results show that small structural changes to the PAMs can result in pronounced differences to baseline, potency (pEC 50 ) and maximum effect (E max ) measures in cAMP assays when compared to the endogenous ligand acetylcholine (ACh) without the addition of the PAMs. Eight selected PAMs were further assessed to determine their binding affinity and potential signalling bias profile between cAMP and β-arrestin 2 recruitment. These rigorous analyses resulted in the discovery of the novel PAMs, 6k and 6l, which exhibit improved allosteric properties compared to the lead compound, and probative in vivo exposure studies in mice confirmed that they maintain the ability to cross the blood-brain barrier, making them more suitable for future preclinical assessment., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 Elsevier Masson SAS. All rights reserved.)

Published

2023

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

Author

Calic PPS, Vinh NB, Webb CT, Malcolm TR, Ngo A, Lowes K, Drinkwater N, McGowan S, and Scammells PJ

Subjects

Humans, Plasmodium falciparum, Aminopeptidases, Antimalarials chemistry, Plasmodium, Malaria, Falciparum drug therapy

Abstract

Malaria remains a global health threat and growing resistance to artemisinin-based therapies calls for therapeutic agents with novel mechanisms of action. The Plasmodium spp M1 and M17 metalloaminopeptidases have been identified as attractive new antimalarial drug targets as inhibition of these enzymes results in antiplasmodial activity. Previously identified novel hydroxamic acid 2 as a moderate inhibitor of PfA-M1 and PfA-M17 and a potent inhibitor of P. falciparum. This study has sought to improve the enzymatic inhibitory properties in addition to increasing the drug-likeness of this scaffold by introducing polar moieties into the S1' region of the active site. Structural biology studies on the co-crystallised structures of potent dual-inhibitor 9aa bound to PfA-M1 and PfA-M17 have revealed that there are few direct interactions between the inhibitor and the S1' domain of these enzymes. Structure-based compound design led to the identification of a variety of novel hydroxamic acids that show improved inhibitory activity against PfA-M1 and PfA-M17, in addition to displaying antiplasmodial activity. Notably, compounds with substitutions on the aniline ring resulted in a loss of potency (K i  > 500 nM) toward PfA-M1 and PfA-M17. ioisosteric replacement of the S1-region biaryl ring system with a bromophenyl moiety resulted in increased potency compared to parent 9aa. Elaboration of 9aa to bioisosterically replace the S1 moiety with an aryl bromide, combined with substituted anilines has resulted in potent selective PfA-M1 inhibitors which show strong activity against Pf-3D7, with meta- and para-fluoroaniline groups of 15ag and 15ah forming hydrogen-bonds with residues within the active site. These findings establish the importance of the previously under-utilised S1' domain and will aid the design of future PfA-M1 and PfA-M17 inhibitors., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022 Elsevier Masson SAS. All rights reserved.)

Published

2023

20. Biocompatible Cationic Lipoamino Acids as Counterions for Oral Administration of API-Ionic Liquids.

Author

Lai A, Leong N, Zheng D, Ford L, Nguyen TH, Williams HD, Benameur H, Scammells PJ, and Porter CJH

Subjects

Administration, Oral, Amino Acids, Cations, Fatty Alcohols, Lipids chemistry, Pharmaceutical Preparations chemistry, Solubility, Ionic Liquids chemistry

Abstract

Purpose: The use of ionic liquids (ILs) in drug delivery has focused attention on non-toxic IL counterions. Cationic lipids can be used to form ILs with weakly acidic drugs to enhance drug loading in lipid-based formulations (LBFs). However, cationic lipids are typically toxic. Here we explore the use of lipoaminoacids (LAAs) as cationic IL counterions that degrade or digest in vivo to non-toxic components., Methods: LAAs were synthesised via esterification of amino acids with fatty alcohols to produce potentially digestible cationic LAAs. The LAAs were employed to form ILs with tolfenamic acid (Tol) and the Tol ILs loaded into LBF and examined in vitro and in vivo., Results: Cationic LAAs complexed with Tol to generate lipophilic Tol ILs with high drug loading in LBFs. Assessment of the LAA under simulated digestion conditions revealed that they were susceptible to enzymatic degradation under intestinal conditions, forming biocompatible FAs and amino acids. In vitro dispersion and digestion studies of Tol ILs revealed that formulations containing digestible Tol ILs were able to maintain drug dispersion and solubilisation whilst the LAA were breaking down under digesting conditions. Finally, in vivo oral bioavailability studies demonstrated that oral delivery of a LBF containing a Tol IL comprising a digestible cationic lipid counterion was able to successfully support effective oral delivery of Tol., Conclusions: Digestible LAA cationic lipids are potential IL counterions for weakly acidic drug molecules and digest in situ to form non-toxic breakdown products., (© 2022. The Author(s).)

Published

2022

21. The Design, Synthesis, and Evaluation of Novel 9-Arylxanthenedione-Based Allosteric Modulators for the δ - Opioid Receptor.

Author

Deo O, Alvi S, Pham V, Christopoulos A, Thal DM, Jörg M, Capuano B, Valant C, and Scammells PJ

Subjects

Antidepressive Agents chemistry, Antidepressive Agents pharmacology, Antidepressive Agents therapeutic use, Enkephalin, Leucine pharmacology, Humans, Receptors, Opioid, mu agonists, Xanthenes chemical synthesis, Xanthenes pharmacology, Chronic Pain drug therapy, Depression drug therapy, Receptors, Opioid, delta

Abstract

Chronic pain and depression are both widely prevalent comorbid medical conditions. While efficient, μ-opioid receptor-based medications are associated with life-threatening side effects, including respiratory depression, dependence, and addiction. The δ-opioid receptor is a promising alternative biological target for chronic pain and depression due to its significantly reduced on-target side effects compared to the μ-opioid receptor. A previous study identified two δ-opioid receptor positive allosteric modulators. Herein, we report the design of five series of compounds targeting previously unexplored regions of the originally described SAR. Analogs were assessed for their ability to potentiate the agonist response of Leu-enkephalin. Of the 30 analogs, compound 6g displayed trends toward enhancing the ERK1/2 phosphorylation signaling compared to cAMP inhibition, while compound 11c exhibited a trend in shifting the signaling bias toward cAMP inhibition. Both 6g and 11c emerged as promising tool compounds toward the design of prospective therapeutics requiring specific downstream signaling attributes.

Published

2022

22. Genetic and chemical validation of Plasmodium falciparum aminopeptidase Pf A-M17 as a drug target in the hemoglobin digestion pathway.

Author

Edgar RCS, Siddiqui G, Hjerrild K, Malcolm TR, Vinh NB, Webb CT, Holmes C, MacRaild CA, Chernih HC, Suen WW, Counihan NA, Creek DJ, Scammells PJ, McGowan S, and de Koning-Ward TF

Subjects

Aminopeptidases chemistry, Aminopeptidases genetics, Digestion, Hemoglobins, Humans, Protease Inhibitors, Protozoan Proteins chemistry, Protozoan Proteins genetics, Malaria, Falciparum, Plasmodium falciparum genetics, Plasmodium falciparum metabolism

Abstract

Plasmodium falciparum, the causative agent of malaria, remains a global health threat as parasites continue to develop resistance to antimalarial drugs used throughout the world. Accordingly, drugs with novel modes of action are desperately required to combat malaria. P. falciparum parasites infect human red blood cells where they digest the host's main protein constituent, hemoglobin. Leucine aminopeptidase Pf A-M17 is one of several aminopeptidases that have been implicated in the last step of this digestive pathway. Here, we use both reverse genetics and a compound specifically designed to inhibit the activity of Pf A-M17 to show that Pf A-M17 is essential for P. falciparum survival as it provides parasites with free amino acids for growth, many of which are highly likely to originate from hemoglobin. We further show that loss of Pf A-M17 results in parasites exhibiting multiple digestive vacuoles at the trophozoite stage. In contrast to other hemoglobin-degrading proteases that have overlapping redundant functions, we validate Pf A-M17 as a potential novel drug target., Competing Interests: RE, GS, KH, TM, NV, CW, CH, CM, HC, WS, NC, DC, PS, SM, Td No competing interests declared, (© 2022, Edgar et al.)

Published

2022

23. Examining the Role of the Linker in Bitopic N 6 -Substituted Adenosine Derivatives Acting as Biased Adenosine A 1 Receptor Agonists.

Author

Awalt JK, Nguyen ATN, Fyfe TJ, Thai BS, White PJ, Christopoulos A, Jörg M, May LT, and Scammells PJ

Subjects

Adenosine pharmacology, Adenosine A1 Receptor Agonists pharmacology, Humans, Ligands, Receptor, Adenosine A1, Receptor, Adenosine A3, Receptors, Purinergic P1, Bradycardia, Purinergic P1 Receptor Agonists

Abstract

The adenosine A 1 receptor is a therapeutic target based on its ability to provide cardioprotection during episodes of myocardial ischemia and reperfusion injury. However, the clinical translation of A 1 R agonists has been hindered by dose-limiting adverse effects (bradycardia and hypotension). Previously, we demonstrated that the bitopic agonist VCP746 ( 1 ), consisting of an adenosine pharmacophore linked to an allosteric moiety, can stimulate cardioprotective A 1 R signaling effects in the absence of unwanted bradycardia. This study maps the structure-activity relationships of 1 through modifications to the linker moiety. Derivatives differing in the flexibility, length, and nature of the linker were assessed, which revealed that the linker is tolerant of several modifications including added rigidity. Ligands featuring 1,4-disubstituted 1,2,3-triazoles were the most biased of the novel analogues but also displayed sub-nanomolar potency in a cAMP accumulation assay at the A 2B R. To our knowledge, 10 is the most potent A 2B R agonist published to date.

Published

2022

24. Structural Features of Iperoxo-BQCA Muscarinic Acetylcholine Receptor Hybrid Ligands Determining Subtype Selectivity and Efficacy.

Author

Wakeham MCL, Davie BJ, Chalmers DK, Christopoulos A, Capuano B, Valant C, and Scammells PJ

Subjects

Allosteric Regulation, Animals, CHO Cells, Cricetinae, Humans, Ligands, Quaternary Ammonium Compounds, Isoxazoles, Receptor, Muscarinic M1

Abstract

Selective agonists for the human M 1 and M 4 muscarinic acetylcholine receptors (mAChRs) are attractive candidates for the treatment of cognitive disorders, such as Alzheimer's disease and schizophrenia. Past efforts to optimize a ligand for selective agonism at any one of the M 1 -M 5 mAChR subtypes has proven to be a significant challenge. Recently, research efforts have demonstrated that hybrid ligands may offer a potential solution to the lack of selectivity at mAChRs. In an attempt to design M 1 mAChR selective agonists by hybridizing an M 1 mAChR selective positive allosteric modulator [1-(4-methoxybenzyl)-4-oxo-1,4-dihydroquinoline-3-carboxylic acid] and a potent agonist [(4-[(4,5-dihydro-3-isoxazolyl)oxy]- N , N , N -trimethyl-2-butyn-1-aminium iodide) (iperoxo)], we unexpectedly discovered that these ligands possessed noticeable M 2 /M 4 mAChR selectivity. Evaluation of truncated derivatives of the hybrid ligands at the M 1 -M 5 mAChR subtypes suggests that the allosteric pharmacophore of iperoxo-based mAChR hybrid ligands likely sterically disrupts the allosteric site of the mAChRs, attenuating the efficacy of M 1 /M 3 /M 5 mAChR responses compared to M 2 /M 4 mAChRs, resulting in a preference for the M 2 /M 4 mAChRs. However, at certain intermediate linker lengths, the effects of this apparent disruption of the allosteric site are diminished, restoring nonselective agonism and suggesting a possible allosteric interaction which is favorable to efficacy at all M 1 -M 5 mAChRs.

Published

2022

25. Discovery and development of 2-aminobenzimidazoles as potent antimalarials.

Author

Devine SM, Challis MP, Kigotho JK, Siddiqui G, De Paoli A, MacRaild CA, Avery VM, Creek DJ, Norton RS, and Scammells PJ

Subjects

Antimalarials chemical synthesis, Antimalarials chemistry, Benzimidazoles chemical synthesis, Benzimidazoles chemistry, Dose-Response Relationship, Drug, HEK293 Cells, Humans, Molecular Structure, Parasitic Sensitivity Tests, Structure-Activity Relationship, Antimalarials pharmacology, Benzimidazoles pharmacology, Drug Discovery, Malaria, Falciparum drug therapy, Plasmodium falciparum drug effects

Abstract

The emergence of Plasmodium falciparum resistance to frontline antimalarials, including artemisinin combination therapies, highlights the need for new molecules that act via novel mechanisms of action. Herein, we report the design, synthesis and antimalarial activity of a series of 2-aminobenzimidazoles, featuring a phenol moiety that is crucial to the pharmacophore. Two potent molecules exhibited IC 50 values against P. falciparum 3D7 strain of 42 ± 4 (3c) and 43 ± 2 nM (3g), and high potency against strains resistant to chloroquine (Dd2), artemisinin (Cam3.II C580Y ) and PfATP4 inhibitors (SJ557733), while demonstrating no cytotoxicity against human cells (HEK293, IC 50  > 50 μM). The most potent molecule, possessing a 4,5-dimethyl substituted phenol (3r) displayed an IC 50 value of 6.4 ± 0.5 nM against P. falciparum 3D7, representing a 12-fold increase in activity from the parent molecule. The 2-aminobenzimidazoles containing a N 1 -substituted phenol represent a new class of molecules that have high potency in vitro against P. falciparum malaria and low cytotoxicity. They possessed attractive pharmaceutical properties, including low molecular weight, high ligand efficiency, high solubility, synthetic tractability and low in vitro clearance in human liver microsomes., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2021 Elsevier Masson SAS. All rights reserved.)

Published

2021

26. 1,3-Benzodioxole-Modified Noscapine Analogues: Synthesis, Antiproliferative Activity, and Tubulin-Bound Structure.

Author

Yong C, Devine SM, Abel AC, Tomlins SD, Muthiah D, Gao X, Callaghan R, Steinmetz MO, Prota AE, Capuano B, and Scammells PJ

Subjects

Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Cell Proliferation drug effects, Dioxoles chemical synthesis, Dioxoles chemistry, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Molecular Structure, Polymerization drug effects, Structure-Activity Relationship, Tubulin Modulators chemical synthesis, Tubulin Modulators chemistry, Tumor Cells, Cultured, Antineoplastic Agents pharmacology, Dioxoles pharmacology, Tubulin metabolism, Tubulin Modulators pharmacology

Abstract

Since the revelation of noscapine's weak anti-mitotic activity, extensive research has been conducted over the past two decades, with the goal of discovering noscapine derivatives with improved potency. To date, noscapine has been explored at the 1, 7, 6', and 9'-positions, though the 1,3-benzodioxole motif in the noscapine scaffold that remains unexplored. The present investigation describes the design, synthesis and pharmacological evaluation of noscapine analogues consisting of modifications to the 1,3-benzodioxole moiety. This includes expansion of the dioxolane ring and inclusion of metabolically robust deuterium and fluorine atoms. Favourable structural modifications were subsequently incorporated into multi-functionalised noscapine derivatives that also possessed modifications previously shown to promote anti-proliferative activity in the 1-, 6'- and 9'-positions. Our research efforts afforded the deuterated noscapine derivative 14 e and the dioxino-containing analogue 20 as potent cytotoxic agents with EC 50 values of 1.50 and 0.73 μM, respectively, against breast cancer (MCF-7) cells. Compound 20 also exhibited EC 50 values of <2 μM against melanoma, non-small cell lung carcinoma, and cancers of the brain, kidney and breast in an NCI screen. Furthermore, compounds 14 e and 20 inhibit tubulin polymerisation and are not vulnerable to the overexpression of resistance conferring P-gp efflux pumps in drug-resistant breast cancer cells (NCI ADR/RES ). We also conducted X-ray crystallography studies that yielded the high-resolution structure of 14 e bound to tubulin. Our structural analysis revealed the key interactions between this noscapinoid and tubulin and will assist with the future design of noscapine derivatives with improved properties., (© 2021 Wiley-VCH GmbH.)

Published

2021

27. Enantioenriched Positive Allosteric Modulators Display Distinct Pharmacology at the Dopamine D 1 Receptor.

Author

Fyfe TJ, Scammells PJ, Lane JR, and Capuano B

Subjects

Allosteric Regulation, Animals, CHO Cells, Cricetulus, Dopamine analogs & derivatives, Dopamine chemistry, Dopamine pharmacology, Receptors, Dopamine D1 chemistry, Receptors, Dopamine D1 metabolism

Abstract

(1) Background: Two first-in-class racemic dopamine D 1 receptor (D 1 R) positive allosteric modulator (PAM) chemotypes ( 1 and 2 ) were identified from a high-throughput screen. In particular, due to its selectivity for the D 1 R and reported lack of intrinsic activity, compound 2 shows promise as a starting point toward the development of small molecule allosteric modulators to ameliorate the cognitive deficits associated with some neuropsychiatric disease states; (2) Methods: Herein, we describe the enantioenrichment of optical isomers of 2 using chiral auxiliaries derived from ( R )- and ( S )-3-hydroxy-4,4-dimethyldihydrofuran-2(3 H )-one (d- and l-pantolactone, respectively); (3) Results: We confirm both the racemate and enantiomers of 2 are active and selective for the D 1 R, but that the respective stereoisomers show a significant difference in their affinity and magnitude of positive allosteric cooperativity with dopamine; (4) Conclusions: These data warrant further investigation of asymmetric syntheses of optically pure analogues of 2 for the development of D 1 R PAMs with superior allosteric properties.

Published

2021

28. Lipophilic Salts and Lipid-Based Formulations: Enhancing the Oral Delivery of Octreotide.

Author

Li P, Ford L, Haque S, McInerney MP, Williams HD, Scammells PJ, Thompson PE, Jannin V, Porter CJH, Benameur H, and Pouton CW

Subjects

Administration, Oral, Animals, Caco-2 Cells, Excipients administration & dosage, Excipients chemical synthesis, Gastrointestinal Absorption drug effects, Gastrointestinal Agents administration & dosage, Gastrointestinal Agents chemical synthesis, Humans, Male, Octreotide administration & dosage, Octreotide chemical synthesis, Rats, Rats, Sprague-Dawley, Salts, Drug Compounding methods, Drug Delivery Systems methods, Excipients pharmacokinetics, Gastrointestinal Absorption physiology, Gastrointestinal Agents pharmacokinetics, Octreotide pharmacokinetics

Abstract

Purpose: Successful oral peptide delivery faces two major hurdles: low enzymatic stability in the gastro-intestinal lumen and poor intestinal membrane permeability. While lipid-based formulations (LBF) have the potential to overcome these barriers, effective formulation of peptides remains challenging. Lipophilic salt (LS) technology can increase the apparent lipophilicity of peptides, making them more suitable for LBF., Methods: As a model therapeutic peptide, octreotide (OCT) was converted to the docusate LS (OCT.DoS 2 ), and compared to the commercial acetate salt (OCT.OAc 2 ) in oral absorption studies and related in vitro studies, including parallel artificial membrane permeability assay (PAMPA), Caco-2, in situ intestine perfusion, and simulated digestion in vitro models. The in vivo oral absorption of OCT.DoS 2 and OCT.OAc 2 formulated in self-emulsifying drug delivery systems (SEDDS) was studied in rats., Results: LS formulation improved the solubility and loading of OCT in LBF excipients and OCT.DoS 2 in combination with SEDDS showed higher OCT absorption than the acetate comparator in the in vivo studies in rats. The Caco-2 and in situ intestine perfusion models indicated no increases in permeability for OCT.DoS 2 . However, the in vitro digestion studies showed reduced enzymatic degradation of OCT.DoS 2 when formulated in the SEDDS formulations. Further in vitro dissociation and release studies suggest that the enhanced bioavailability of OCT from SEDDS-incorporating OCT.DoS 2 is likely a result of higher partitioning into and prolonged retention within lipid colloid structures., Conclusion: The combination of LS and LBF enhanced the in vivo oral absorption of OCT primarily via the protective effect of LBF sheltering the peptide from gastrointestinal degradation.

Published

2021

29. Development and Application of Subtype-Selective Fluorescent Antagonists for the Study of the Human Adenosine A 1 Receptor in Living Cells.

Author

Comeo E, Trinh P, Nguyen AT, Nowell CJ, Kindon ND, Soave M, Stoddart LA, White JM, Hill SJ, Kellam B, Halls ML, May LT, and Scammells PJ

Subjects

Adenosine A1 Receptor Antagonists metabolism, Bridged Bicyclo Compounds chemistry, Drug Design, Fluorescence Resonance Energy Transfer, Fluorescent Dyes metabolism, HEK293 Cells, Humans, Kinetics, Ligands, Octanes chemistry, Receptor, Adenosine A1 metabolism, Structure-Activity Relationship, Xanthine chemistry, Xanthine metabolism, Adenosine A1 Receptor Antagonists chemical synthesis, Fluorescent Dyes chemistry, Receptor, Adenosine A1 chemistry

Abstract

The adenosine A 1 receptor (A 1 AR) is a G-protein-coupled receptor (GPCR) that provides important therapeutic opportunities for a number of conditions including congestive heart failure, tachycardia, and neuropathic pain. The development of A 1 AR-selective fluorescent ligands will enhance our understanding of the subcellular mechanisms underlying A 1 AR pharmacology facilitating the development of more efficacious and selective therapies. Herein, we report the design, synthesis, and application of a novel series of A 1 AR-selective fluorescent probes based on 8-functionalized bicyclo[2.2.2]octylxanthine and 3-functionalized 8-(adamant-1-yl) xanthine scaffolds. These fluorescent conjugates allowed quantification of kinetic and equilibrium ligand binding parameters using NanoBRET and visualization of specific receptor distribution patterns in living cells by confocal imaging and total internal reflection fluorescence (TIRF) microscopy. As such, the novel A 1 AR-selective fluorescent antagonists described herein can be applied in conjunction with a series of fluorescence-based techniques to foster understanding of A 1 AR molecular pharmacology and signaling in living cells.

Published

2021

30. Stabilising disproportionation of lipophilic ionic liquid salts in lipid-based formulations.

Author

Lai A, Sahbaz Y, Ford L, Nguyen TH, Haque S, Williams HD, Benameur H, Scammells PJ, and Porter CJH

Subjects

Lipids, Salts, Solubility, Cinnarizine, Ionic Liquids

Abstract

Lipid based formulations (LBFs) can enhance oral bioavailability, however, their utility may be restricted by low drug loading in the formulation. Converting drugs to drug-ionic liquids (drug-ILs) or lipophilic salts can significantly increase lipid solubility but this approach is complicated in some cases by salt disproportionation, leading to a reduction in solubility and physical instability. Here we explore the physical stability of the weakly basic model drug, cinnarizine (CIN), when paired with a decanoate counterion (Dec) to form the drug-IL, cinnarizine decanoate (CIN.Dec). Consistent with published studies of salt disproportionation in aqueous solution, weakly acidic counterions such as Dec lead to the generation of drug-IL lipid solutions with pHs below pH max . This leads to CIN deprotonation to the less soluble free base and precipitation. Subsequent studies however, show that these effects can be reversed by acidification of the formulation (either with excess decanoic acid or other lipid soluble acids), stimulating a pH shift to the salt plateau of CIN.Dec and the formation of stable lipid solutions of CIN.Dec. Altering formulation pH to more acidic conditions, therefore stabilises drug-ILs formed using weakly acidic lipophilic counterions, and is a viable method to promote formulation stability via inhibition of disproportionation of some drug-ILs., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

31. Development of Novel 4-Arylpyridin-2-one and 6-Arylpyrimidin-4-one Positive Allosteric Modulators of the M 1 Muscarinic Acetylcholine Receptor.

Author

Jörg M, Khajehali E, van der Westhuizen ET, C Choy KH, Shackleford DM, Tobin AB, Sexton PM, Valant C, Capuano B, Christopoulos A, and Scammells PJ

Subjects

Allosteric Regulation drug effects, Animals, Blood-Brain Barrier drug effects, Blood-Brain Barrier metabolism, Half-Life, Humans, Mice, Permeability drug effects, Pyridones metabolism, Pyridones pharmacology, Receptor, Muscarinic M1 chemistry, Structure-Activity Relationship, Pyridones chemistry, Receptor, Muscarinic M1 metabolism

Abstract

This study investigated the structure-activity relationships of 4-phenylpyridin-2-one and 6-phenylpyrimidin-4-one M 1 muscarinic acetylcholine receptor (M 1 mAChRs) positive allosteric modulators (PAMs). The presented series focuses on modifications to the core and top motif of the reported leads, MIPS1650 (1) and MIPS1780 (2). Profiling of our novel analogues showed that these modifications result in more nuanced effects on the allosteric properties compared to our previous compounds with alterations to the biaryl pendant. Further pharmacological characterisation of the selected compounds in radioligand binding, IP 1 accumulation and β-arrestin 2 recruitment assays demonstrated that, despite primarily acting as affinity modulators, the PAMs displayed different pharmacological properties across the two cellular assays. The novel PAM 7 f is a potential lead candidate for further development of peripherally restricted M 1 PAMs, due to its lower blood-brain-barrier (BBB) permeability and improved exposure in the periphery compared to lead 2., (© 2020 Wiley-VCH GmbH.)

Published

2021

32. Driving antimalarial design through understanding of target mechanism.

Author

Calic PPS, Mansouri M, Scammells PJ, and McGowan S

Subjects

Binding Sites, Cell Proliferation, Chemistry, Pharmaceutical methods, Crystallography, X-Ray, Dimerization, Humans, Hydrophobic and Hydrophilic Interactions, Mutation, Protein Binding, Protein Domains, Reproducibility of Results, Tetrahydrofolate Dehydrogenase metabolism, Zinc chemistry, Antimalarials pharmacology, Drug Design, Malaria drug therapy, Plasmodium falciparum drug effects, Protozoan Proteins metabolism

Abstract

Malaria continues to be a global health threat, affecting approximately 219 million people in 2018 alone. The recurrent development of resistance to existing antimalarials means that the design of new drug candidates must be carefully considered. Understanding of drug target mechanism can dramatically accelerate early-stage target-based development of novel antimalarials and allows for structural modifications even during late-stage preclinical development. Here, we have provided an overview of three promising antimalarial molecular targets, PfDHFR, PfDHODH and PfA-M1, and their associated inhibitors which demonstrate how mechanism can inform drug design and be effectively utilised to generate compounds with potent inhibitory activity., (© 2020 The Author(s).)

Published

2020

33. 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

34. API ionic liquids: probing the effect of counterion structure on physical form and lipid solubility.

Author

Ford L, Tay E, Nguyen TH, Williams HD, Benameur H, Scammells PJ, and Porter CJH

Abstract

Lipid based formulations (LBFs) are extensively utilised as an enabling technology in drug delivery. The use of ionic liquids (ILs) or lipophilic salts (LS) in drug delivery has also garnered considerable interest due to unique solubility properties. Conversion of active pharmaceutical ingredients (API) to ILs by pairing with an appropriately lipophilic counterion has been shown to decrease melting point of the salt complex and improve solubility in LBFs. However, the relationship between the structure of the counterion, the physicochemical properties of the resulting salts and solubility in LBFs has not been systematically explored. This study investigates the relationship between alkyl sulfate counterion structure and melting temperature ( T m or T g ) in addition to LBF solubility, utilizing cinnarizine and lumefantrine as model weakly basic APIs. Three series of structurally diverse alkyl sulfate counterions were chosen to probe this relationship. Pairing cinnarizine and lumefantrine with a majority of these alkyl sulfate counterions resulted in a reduction in melting temperature and enhanced solubility in model medium chain and long chain LBFs. The chain length of the alkyl sulfate plays a crucial role in performance, and consistently branched alkyl sulfate counterions perform better than straight chain alkyl sulfate counterions, as predicted. Most interestingly, trends in counterion performance were found to be consistent across two APIs with disparate chemical structures. The findings from this study will facilitate the design of counterions which enhance solubility of ionisable drugs and unlock the potential to develop compounds previously restrained by poor solubility., Competing Interests: This article describes intellectual property in the use of ionic liquids/lipophilic salts in drug delivery that has been assigned to Lonza. Authors L. F., H. D. W. and H. B. are from Lonza., (This journal is © The Royal Society of Chemistry.)

Published

2020

35. Subtype-Selective Fluorescent Ligands as Pharmacological Research Tools for the Human Adenosine A 2A Receptor.

Author

Comeo E, Kindon ND, Soave M, Stoddart LA, Kilpatrick LE, Scammells PJ, Hill SJ, and Kellam B

Subjects

Adenosine A2 Receptor Antagonists metabolism, Adenosine A2 Receptor Antagonists pharmacology, Drug Discovery, Fluorescent Dyes metabolism, Fluorescent Dyes pharmacology, HEK293 Cells, Humans, Ligands, Molecular Docking Simulation, Optical Imaging, Pyrimidines metabolism, Pyrimidines pharmacology, Receptor, Adenosine A2A metabolism, Triazoles metabolism, Triazoles pharmacology, Adenosine A2 Receptor Antagonists chemistry, Fluorescent Dyes chemistry, Pyrimidines chemistry, Receptor, Adenosine A2A analysis, Triazoles chemistry

Abstract

Among class A G protein-coupled receptors (GPCR), the human adenosine A 2A receptor (hA 2A AR) remains an attractive drug target. However, translation of A 2A AR ligands into the clinic has proved challenging and an improved understanding of A 2A AR pharmacology could promote development of more efficacious therapies. Subtype-selective fluorescent probes would allow detailed real-time pharmacological investigations both in vitro and in vivo. In the present study, two families of fluorescent probes were designed around the known hA 2A AR selective antagonist preladenant (SCH 420814). Both families of fluorescent antagonists retained affinity at the hA 2A AR, selectivity over all other adenosine receptor subtypes and allowed clear visualization of specific receptor localization through confocal imaging. Furthermore, the Alexa Fluor 647-labeled conjugate allowed measurement of ligand binding affinities of unlabeled hA 2A AR antagonists using a bioluminescence resonance energy transfer (NanoBRET) assay. The fluorescent ligands developed here can therefore be applied to a range of fluorescence-based techniques to further interrogate hA 2A AR pharmacology and signaling.

Published

2020

36. The effect of two selective A 1 -receptor agonists and the bitopic ligand VCP746 on heart rate and regional vascular conductance in conscious rats.

Author

Cooper SL, March J, Sabbatini AR, Hill SJ, Jörg M, Scammells PJ, and Woolard J

Subjects

Adenosine pharmacology, Aminopyridines pharmacology, Animals, Cardiovascular System metabolism, Consciousness, Drug Partial Agonism, Heart Rate drug effects, Ligands, Male, Rats, Sprague-Dawley, Receptor, Adenosine A1 metabolism, Receptor, Adenosine A2A drug effects, Receptor, Adenosine A2A metabolism, Receptor, Adenosine A2B drug effects, Receptor, Adenosine A2B metabolism, Regional Blood Flow drug effects, Thiazoles pharmacology, Adenosine analogs & derivatives, Adenosine A1 Receptor Agonists pharmacology, Adenosine A2 Receptor Agonists pharmacology, Cardiovascular System drug effects, Hemodynamics drug effects, Receptor, Adenosine A1 drug effects, Thiophenes pharmacology

Abstract

Background and Purpose: Adenosine is a local mediator that regulates physiological and pathological processes via activation of four GPCRs (A 1 , A 2A , A 2B , and A 3 ). We have investigated the effect of two A 1 -receptor-selective agonists and the novel A 1 -receptor bitopic ligand VCP746 on the rat cardiovascular system., Experimental Approach: The regional haemodynamic responses of these agonist was investigated in conscious rats. Male Sprague-Dawley rats (350-450 g) were chronically implanted with pulsed Doppler flow probes on the renal, mesenteric arteries and the descending abdominal aorta and the jugular vein and caudal artery catheterized. Cardiovascular responses were measured following intravenous infusion (3 min each dose) of CCPA (120, 400, and 1,200 ng·kg -1 ·min -1 ), capadenoson or adenosine (30, 100, and 300 μg·kg -1 ·min -1 ), or VCP746 (6, 20, and 60 μg·kg -1 ·min -1 ) following pre-dosing with DPCPX (0.1 mg·kg -1 , i.v.) or vehicle., Key Results: CCPA produced a significant A 1 -receptor-mediated decrease in heart rate that was accompanied by vasoconstrictions in the renal and mesenteric vascular beds but an increase in hindquarters vascular conductance. The partial agonist capadenoson also produced an A 1 -receptor-mediated bradycardia. In contrast, VCP746 produced increases in heart rate and renal and mesenteric vascular conductance that were not mediated by A 1 -receptors. In vitro studies confirmed that VCP746 had potent agonist activity at both A 2A - and A 2B -receptors., Conclusions and Implications: These results suggest VCP746 mediates its cardiovascular effects via activation of A 2 rather than A 1 adenosine receptors. This has implications for the design of future bitopic ligands that incorporate A 1 allosteric ligand moieties., (© 2019 The Authors. British Journal of Pharmacology published by John Wiley & Sons Ltd on behalf of British Pharmacological Society.)

Published

2020

37. Ionic Liquid Forms of the Antimalarial Lumefantrine in Combination with LFCS Type IIIB Lipid-Based Formulations Preferentially Increase Lipid Solubility, In Vitro Solubilization Behavior and In Vivo Exposure.

Author

Tay E, Nguyen TH, Ford L, Williams HD, Benameur H, Scammells PJ, and Porter CJH

Abstract

Lipid based formulations (LBFs) are commonly employed to enhance the absorption of highly lipophilic, poorly water-soluble drugs. However, the utility of LBFs can be limited by low drug solubility in the formulation. Isolation of ionizable drugs as low melting, lipophilic salts or ionic liquids (ILs) provides one means to enhance drug solubility in LBFs. However, whether different ILs benefit from formulation in different LBFs is largely unknown. In the current studies, lumefantrine was isolated as a number of different lipophilic salt/ionic liquid forms and performance was assessed after formulation in a range of LBFs. The solubility of lumefantrine in LBF was enhanced 2- to 80-fold by isolation as the lumefantrine docusate IL when compared to lumefantrine free base. The increase in drug loading subsequently enhanced concentrations in the aqueous phase of model intestinal fluids during in vitro dispersion and digestion testing of the LBF. To assess in vivo performance, the systemic exposure of lumefantrine docusate after administration in Type II-MCF, IIIB-MCF, IIIB-LCF, and IV formulations was evaluated after oral administration to rats. In vivo exposure was compared to control lipid and aqueous suspension formulations of lumefantrine free base. Lumefantrine docusate in the Type IIIB-LCF showed significantly higher plasma exposure compared to all other formulations (up to 35-fold higher). The data suggest that isolation of a lipid-soluble IL, coupled with an appropriate formulation, is a viable means to increase drug dose in an oral formulation and to enhance exposure of lumefantrine in vivo ., Competing Interests: This work describes intellectual property in the use of ionic liquids/lipophilic salts in drug delivery that has been assigned to Lonza from Monash University. H.D.W., H.B. and L.F. are all employees of Lonza and participated in the conduct or write up of this study.

Published

2019

38. A Novel Class of N-Sulfonyl and N-Sulfamoyl Noscapine Derivatives that Promote Mitotic Arrest in Cancer Cells.

Author

Yong C, Devine SM, Gao X, Yan A, Callaghan R, Capuano B, and Scammells PJ

Subjects

ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Antineoplastic Agents pharmacology, Cell Line, Tumor, Cell Proliferation drug effects, Drug Screening Assays, Antitumor, Humans, Microtubules metabolism, Molecular Structure, Noscapine pharmacology, Polymerization, Structure-Activity Relationship, Tubulin metabolism, Antineoplastic Agents chemical synthesis, Noscapine analogs & derivatives, Noscapine chemical synthesis, Sulfuric Acids chemistry

Abstract

Noscapine displays weak anticancer efficacy and numerous research efforts have attempted to generate more potent noscapine analogues. These modifications included the replacement of the N-methyl group in the 6'-position with a range of substituents, where N-ethylcarbamoyl substitution was observed to possess enhanced anticancer activity. Herein, we describe advances in this area, namely the synthesis and pharmacological evaluation of a series of N-sulfonyl and N-sulfamoyl noscapine derivatives. A number of these sulfonyl-containing noscapinoids demonstrated improved activities compared to noscapine. ((R)-5-((S)-4,5-Dimethoxy-1,3-dihydroisobenzofuran-1-yl)-4-methoxy-6-((1-methyl-1H-imidazol-4-yl)sulfonyl)-5,6,7,8-tetrahydro[1,3]dioxolo[4,5-g]isoquinoline) (14 q) displayed sub-micromolar activities of 560, 980, 271 and 443 nM against MCF-7, PANC-1, MDA-MB-435 and SK-MEL-5 cells, respectively. This antiproliferative effect was also maintained against drug-resistant NCI/Adr RES cells despite high expression of the multidrug efflux pump, P-glycoprotein., (© 2019 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2019

39. Structure-Kinetic Profiling of Haloperidol Analogues at the Human Dopamine D 2 Receptor.

Author

Fyfe TJ, Kellam B, Sykes DA, Capuano B, Scammells PJ, Lane JR, Charlton SJ, and Mistry SN

Subjects

Animals, CHO Cells, Cricetulus, Dopamine D2 Receptor Antagonists adverse effects, Haloperidol adverse effects, Humans, Kinetics, Receptors, Dopamine D2 chemistry, Structure-Activity Relationship, Dopamine D2 Receptor Antagonists chemistry, Dopamine D2 Receptor Antagonists metabolism, Haloperidol chemistry, Haloperidol metabolism, Receptors, Dopamine D2 metabolism

Abstract

Haloperidol is a typical antipsychotic drug (APD) associated with an increased risk of extrapyramidal side effects (EPSs) and hyperprolactinemia relative to atypical APDs such as clozapine. Both drugs are dopamine D 2 receptor (D 2 R) antagonists, with contrasting kinetic profiles. Haloperidol displays fast association/slow dissociation at the D 2 R, whereas clozapine exhibits relatively slow association/fast dissociation. Recently, we have provided evidence that slow dissociation from the D 2 R predicts hyperprolactinemia, whereas fast association predicts EPS. Unfortunately, clozapine can cause severe side effects independent of its D 2 R action. Our results suggest an optimal kinetic profile for D 2 R antagonist APDs that avoids EPS. To begin exploring this hypothesis, we conducted a structure-kinetic relationship study of haloperidol and revealed that subtle structural modifications dramatically change binding kinetic rate constants, affording compounds with a clozapine-like kinetic profile. Thus, optimization of these kinetic parameters may allow development of novel APDs based on the haloperidol scaffold with improved side-effect profiles.

Published

2019

40. Molecular Determinants of the Intrinsic Efficacy of the Antipsychotic Aripiprazole.

Author

Klein Herenbrink C, Verma R, Lim HD, Kopinathan A, Keen A, Shonberg J, Draper-Joyce CJ, Scammells PJ, Christopoulos A, Javitch JA, Capuano B, Shi L, and Lane JR

Subjects

Antipsychotic Agents chemistry, Aripiprazole chemistry, Binding Sites, Dopamine chemistry, Dopamine metabolism, Dopamine Agonists chemistry, Indoles chemistry, Indoles metabolism, Ligands, Molecular Conformation, Molecular Dynamics Simulation, Mutagenesis, Site-Directed, Mutation, Receptors, Dopamine D2 chemistry, Receptors, Dopamine D2 genetics, Antipsychotic Agents metabolism, Aripiprazole metabolism, Dopamine Agonists metabolism, Receptors, Dopamine D2 metabolism

Abstract

Partial agonists of the dopamine D 2 receptor (D 2 R) have been developed to treat the symptoms of schizophrenia without causing the side effects elicited by antagonists. The receptor-ligand interactions that determine the intrinsic efficacy of such drugs, however, are poorly understood. Aripiprazole has an extended structure comprising a phenylpiperazine primary pharmacophore and a 1,2,3,4-tetrahydroquinolin-2-one secondary pharmacophore. We combined site-directed mutagenesis, analytical pharmacology, ligand fragments, and molecular dynamics simulations to identify the D 2 R-aripiprazole interactions that contribute to affinity and efficacy. We reveal that an interaction between the secondary pharmacophore of aripiprazole and a secondary binding pocket defined by residues at the extracellular portions of transmembrane segments 1, 2, and 7 determines the intrinsic efficacy of aripiprazole. Our findings reveal a hitherto unappreciated mechanism for fine-tuning the intrinsic efficacy of D 2 R agonists.

Published

2019

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

Author

Lee J, Vinh NB, Drinkwater N, Yang W, Kannan Sivaraman K, Schembri LS, Gazdik M, Grin PM, Butler GS, Overall CM, Charman SA, McGowan S, and Scammells PJ

Subjects

Animals, Binding Sites physiology, Enzyme Inhibitors chemistry, Enzyme Inhibitors metabolism, Enzyme Inhibitors pharmacology, Humans, Male, Mice, Protein Binding physiology, Protein Structure, Tertiary, CD13 Antigens antagonists & inhibitors, CD13 Antigens metabolism, Drug Discovery methods

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 ( Pf A-M1). Herein, we describe the rationale that underpins the repurposing of Pf A-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

42. Cryptic pocket formation underlies allosteric modulator selectivity at muscarinic GPCRs.

Author

Hollingsworth SA, Kelly B, Valant C, Michaelis JA, Mastromihalis O, Thompson G, Venkatakrishnan AJ, Hertig S, Scammells PJ, Sexton PM, Felder CC, Christopoulos A, and Dror RO

Subjects

Allosteric Regulation, Allosteric Site, Crystallography, X-Ray, Drug Design, Ligands, Molecular Dynamics Simulation, Mutagenesis, Site-Directed, Receptor, Muscarinic M1 chemistry, Receptors, G-Protein-Coupled chemistry

Abstract

Allosteric modulators are highly desirable as drugs, particularly for G-protein-coupled receptor (GPCR) targets, because allosteric drugs can achieve selectivity between closely related receptors. The mechanisms by which allosteric modulators achieve selectivity remain elusive, however, particularly given recent structures that reveal similar allosteric binding sites across receptors. Here we show that positive allosteric modulators (PAMs) of the M1 muscarinic acetylcholine receptor (mAChR) achieve exquisite selectivity by occupying a dynamic pocket absent in existing crystal structures. This cryptic pocket forms far more frequently in molecular dynamics simulations of the M1 mAChR than in those of other mAChRs. These observations reconcile mutagenesis data that previously appeared contradictory. Further mutagenesis experiments validate our prediction that preventing cryptic pocket opening decreases the affinity of M1-selective PAMs. Our findings suggest opportunities for the design of subtype-specific drugs exploiting cryptic pockets that open in certain receptors but not in other receptors with nearly identical static structures.

Published

2019

43. Subtle modifications to a thieno[2,3-d]pyrimidine scaffold yield negative allosteric modulators and agonists of the dopamine D 2 receptor.

Author

Fyfe TJ, Kellam B, Mistry SN, Scammells PJ, Lane JR, and Capuano B

Subjects

Allosteric Regulation drug effects, Animals, CHO Cells, Cells, Cultured, Cricetulus, Dose-Response Relationship, Drug, Humans, Molecular Structure, Pyrimidines chemical synthesis, Pyrimidines chemistry, Structure-Activity Relationship, Pyrimidines pharmacology, Receptors, Dopamine D2 agonists

Abstract

We recently described a structurally novel series of negative allosteric modulators (NAMs) of the dopamine D 2 receptor (D 2 R) based on thieno[2,3-d]pyrimidine 1, showing it can be structurally simplified to reveal low molecular weight, fragment-like NAMs that retain robust negative cooperativity, such as 3. Herein, we report the synthesis and functional profiling of analogues of 3, placing specific emphasis on examining secondary and tertiary amino substituents at the 4-position, combined with a range of substituents at the 5/6-positions (e.g. aromatic/aliphatic carbocycles). We identify analogues with diverse pharmacology at the D 2 R including NAMs with sub-μM affinity (9h) and, surprisingly, low efficacy partial agonists (9d and 9i)., (Crown Copyright © 2019. Published by Elsevier Masson SAS. All rights reserved.)

Published

2019

44. Probe dependence of allosteric enhancers on the binding affinity of adenosine A 1 -receptor agonists at rat and human A 1 -receptors measured using NanoBRET.

Author

Cooper SL, Soave M, Jörg M, Scammells PJ, Woolard J, and Hill SJ

Subjects

Allosteric Regulation, Animals, HEK293 Cells, Humans, Ligands, Purinergic P1 Receptor Agonists chemistry, Rats, Receptor, Adenosine A1 chemistry, Receptor, Adenosine A1 genetics, Purinergic P1 Receptor Agonists pharmacology, Receptor, Adenosine A1 metabolism

Abstract

Background and Purpose: Adenosine is a local mediator that regulates a number of physiological and pathological processes via activation of adenosine A 1 -receptors. The activity of adenosine can be regulated at the level of its target receptor via drugs that bind to an allosteric site on the A 1 -receptor. Here, we have investigated the species and probe dependence of two allosteric modulators on the binding characteristics of fluorescent and nonfluorescent A 1 -receptor agonists., Experimental Approach: A Nano-luciferase (Nluc) BRET (NanoBRET) methodology was used. This used N-terminal Nluc-tagged A 1 -receptors expressed in HEK293T cells in conjunction with both fluorescent A 1 -receptor agonists (adenosine and NECA analogues) and a fluorescent antagonist CA200645., Key Results: PD 81,723 and VCP171 elicited positive allosteric effects on the binding affinity of orthosteric agonists at both the rat and human A 1 -receptors that showed clear probe dependence. Thus, the allosteric effect on the highly selective partial agonist capadenoson was much less marked than for the full agonists NECA, adenosine, and CCPA in both species. VCP171 and, to a lesser extent, PD 81,723, also increased the specific binding of three fluorescent A 1 -receptor agonists in a species-dependent manner that involved increases in B max and pK D ., Conclusions and Implications: These results demonstrate the power of the NanoBRET ligand-binding approach to study the effect of allosteric ligands on the binding of fluorescent agonists to the adenosine A 1 -receptor in intact living cells. Furthermore, our studies suggest that VCP171 and PD 81,723 may switch a proportion of A 1 -receptors to an active agonist conformation (R*)., (© 2019 The Authors. British Journal of Pharmacology published by John Wiley & Sons Ltd on behalf of British Pharmacological Society.)

Published

2019

45. 6-Phenylpyrimidin-4-ones as Positive Allosteric Modulators at the M 1 mAChR: The Determinants of Allosteric Activity.

Author

Jörg M, van der Westhuizen ET, Khajehali E, Burger WAC, White JM, Choy KHC, Tobin AB, Sexton PM, Valant C, Capuano B, Christopoulos A, and Scammells PJ

Subjects

Allosteric Regulation drug effects, Allosteric Regulation physiology, Animals, CHO Cells, Cells, Cultured, Cricetinae, Cricetulus, Crystallography, X-Ray methods, Mice, Pyrimidines chemical synthesis, Pyrimidines pharmacology, Quinolines chemical synthesis, Quinolines pharmacology, Receptor, Muscarinic M1 agonists, Receptor, Muscarinic M1 physiology

Abstract

Targeting allosteric sites of the M 1 muscarinic acetylcholine receptor (mAChR) is an enticing approach to overcome the lack of receptor subtype selectivity observed with orthosteric ligands. This is a promising strategy for obtaining novel therapeutics to treat cognitive deficits observed in Alzheimer's disease and schizophrenia, while reducing the peripheral side effects such as seen in the current treatment regimes, which are non-subtype selective. We previously described compound 2, the first positive allosteric modulator (PAM) of the M 1 mAChR based on a 6-phenylpyrimidin-4-one scaffold, which has been further developed in this study. Herein, we present the synthesis, characterization, and pharmacological evaluation of a series of 6-phenylpyrimidin-4-ones with modifications to the 4-(1-methylpyrazol-4-yl)benzyl pendant. Selected compounds, BQCA, 1, 2, 9i, 13, 14b, 15c, and 15d, were further profiled in terms of their allosteric affinity, cooperativity with acetylcholine (ACh), and intrinsic efficacy. Additionally, 2 and 9i were tested in mouse primary cortical neurons, displaying various degrees of intrinsic agonism and potentiation of the acetylcholine response. Overall, the results suggest that the pendant moiety is important for allosteric binding affinity and the direct agonistic efficacy of the 6-phenylpyrimidin-4-one based M 1 mAChR PAMs.

Published

2019

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

Author

Akter M, Drinkwater N, Devine SM, Drew SC, Krishnarjuna B, Debono CO, Wang G, Scanlon MJ, Scammells PJ, McGowan S, MacRaild CA, and Norton RS

Subjects

Amino Acid Sequence, Antigens, Protozoan, Benzimidazoles chemistry, Binding Sites, Cell Membrane metabolism, Crystallography, X-Ray, Furans chemistry, Hydrophobic and Hydrophilic Interactions, Ligands, Models, Molecular, Molecular Probes metabolism, Molecular Structure, Peptides metabolism, Protein Binding, Pyrazoles chemistry, Pyrimidines chemistry, Pyrroles chemistry, Quinazolinones chemistry, Structure-Activity Relationship, Sulfonamides chemistry, Magnetic Resonance Spectroscopy methods, Membrane Proteins antagonists & inhibitors, Molecular Probes chemistry, Peptides chemistry, Protozoan Proteins antagonists & inhibitors

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., (© 2019 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2019

47. Unlocking the full potential of lipid-based formulations using lipophilic salt/ionic liquid forms.

Author

Williams HD, Ford L, Igonin A, Shan Z, Botti P, Morgen MM, Hu G, Pouton CW, Scammells PJ, Porter CJH, and Benameur H

Subjects

Animals, Drug Compounding, Legislation, Drug, Drug Delivery Systems, Ionic Liquids chemistry, Lipids chemistry, Salts chemistry

Abstract

Lipid-based formulations (LBF) are widely used by industry and accepted by the regulatory authorities for oral drug delivery in the pharmaceutical and consumer healthcare market. Innovation in the LBF field is however needed in order to meet the demands of modern drugs, their more challenging problem statements and growing needs for achieving optimal pharmacokinetics (i.e., no food-effects, low variability) on approval. This review describes a new lipophilic salt / ionic liquid approach in combination with LBF, and how this salt strategy can be used to better tailor the properties of a drug to LBFs. The potential advantages of lipophilic salts are discussed in the context of dose escalation studies during toxicological evaluation, reducing the pill burden, increasing drug absorption of new drugs and in life-cycle management. Commentary on lipophilic salt synthesis, scale-up, LBF design and the regulatory aspects are also provided. These topics are discussed in the broad context of bringing the widely recognized advantages of LBFs to a broader spectrum of drugs., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

48. Overcoming P-Glycoprotein-Mediated Drug Resistance with Noscapine Derivatives.

Author

Muthiah D, Henshaw GK, DeBono AJ, Capuano B, Scammells PJ, and Callaghan R

Subjects

ATP Binding Cassette Transporter, Subfamily B isolation & purification, ATP Binding Cassette Transporter, Subfamily B metabolism, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Drug Screening Assays, Antitumor, Humans, MCF-7 Cells, Neoplasms pathology, Noscapine analogs & derivatives, Papaver chemistry, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Tubulin Modulators pharmacology, Tubulin Modulators therapeutic use, Vinblastine pharmacology, Antineoplastic Combined Chemotherapy Protocols pharmacology, Drug Resistance, Multiple drug effects, Drug Resistance, Neoplasm drug effects, Neoplasms drug therapy, Noscapine pharmacology

Abstract

The antitussive agent noscapine has been shown to inhibit the proliferation of cancer cells by disruption of tubulin dynamic. However, the efficacy of several anticancer drugs that inhibit tublin dynamics (vinca alkaloids and taxanes) is reduced by the multidrug resistance phenotype. These compounds are substrates for P-glycoprotein (P-gp)-mediated extrusion from cells. Consequently, the antiproliferative activity of noscapine and a series of derivatives was measured in drug-sensitive and drug-resistant cells that overexpress P-gp. None of the noscapine derivatives displayed lower potency in cells overexpressing P-gp, thereby suggesting a lack of interaction with this pump. However, the cellular efflux of a fluorescent substrate by P-gp was potently inhibited by noscapine and most derivatives. Further investigation with purified, reconstituted P-gp demonstrated that inhibition of P-gp function was due to direct interaction of noscapine derivatives with the transporter. Moreover, coadministration of vinblastine with two of the noscapine derivatives displayed synergistic inhibition of proliferation, even in P-gp-expressing resistant cell lines. Therefore, noscapine derivatives offer a dual benefit of overcoming the significant impact of P-gp in conferring multidrug resistance and synergy with tubulin-disrupting anticancer drugs., (Copyright © 2019 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2019

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

Author

Vinh NB, Drinkwater N, Malcolm TR, Kassiou M, Lucantoni L, Grin PM, Butler GS, Duffy S, Overall CM, Avery VM, Scammells PJ, and McGowan S

Subjects

Aminopeptidases metabolism, Antimalarials metabolism, Antimalarials pharmacology, Binding Sites, Catalytic Domain, Cell Survival drug effects, Drug Resistance drug effects, HEK293 Cells, Humans, Hydroxamic Acids metabolism, Hydroxamic Acids pharmacology, Molecular Docking Simulation, Plasmodium drug effects, Protease Inhibitors metabolism, Protease Inhibitors pharmacology, Protozoan Proteins metabolism, Structure-Activity Relationship, Aminopeptidases antagonists & inhibitors, Antimalarials chemistry, Hydroxamic Acids chemistry, Plasmodium enzymology, Protease Inhibitors chemistry, Protozoan Proteins antagonists & inhibitors

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

2019

50. A Thieno[2,3- d]pyrimidine Scaffold Is a Novel Negative Allosteric Modulator of the Dopamine D 2 Receptor.

Author

Fyfe TJ, Zarzycka B, Lim HD, Kellam B, Mistry SN, Katrich V, Scammells PJ, Lane JR, and Capuano B

Subjects

Allosteric Regulation, Allosteric Site, Animals, CHO Cells, Cricetinae, Cricetulus, Haloperidol chemistry, Haloperidol metabolism, Humans, Isotope Labeling, Kinetics, Molecular Conformation, Molecular Docking Simulation, Protein Binding, Pyrimidines chemical synthesis, Pyrimidines metabolism, Receptors, Dopamine D2 genetics, Receptors, Dopamine D2 metabolism, Structure-Activity Relationship, Tritium chemistry, Pyrimidines chemistry, Receptors, Dopamine D2 chemistry

Abstract

Recently, a novel negative allosteric modulator (NAM) of the D 2 -like dopamine receptors 1 was identified through virtual ligand screening. This ligand comprises a thieno[2,3- d]pyrimidine scaffold that does not feature in known dopaminergic ligands. Herein, we provide pharmacological validation of an allosteric mode of action for 1, revealing that it is a NAM of dopamine efficacy and identify the structural determinants of this allostery. We find that key structural moieties are important for functional affinity and negative cooperativity, while functionalization of the thienopyrimidine at the 5- and 6-positions results in analogues with divergent cooperativity profiles. Successive compound iterations have yielded analogues exhibiting a 10-fold improvement in functional affinity, as well as enhanced negative cooperativity with dopamine affinity and efficacy. Furthermore, our study reveals a fragment-like core that maintains low μM affinity and robust negative cooperativity with markedly improved ligand efficiency.

Published

2019