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1. Delineation of the GPR15 receptor-mediated Gα protein signalling profile in recombinant mammalian cells

Author

Yufang Deng, Ee Von Moo, Claudia Victoria Pérez Almería, Patrick R. Gentry, Line Vedel, Jesper M. Mathiesen, Hans Bräuner‐Osborne, AIMMS, and Medicinal chemistry

Subjects
Mammals, Pharmacology, Gα protein, General Medicine, Toxicology, Receptors, G-Protein-Coupled, second messenger, Pertussis Toxin, SDG 3 - Good Health and Well-being, GTP-Binding Proteins, Animals, GPR15, BRET, signalling, Signal Transduction
Abstract

The GPR15 receptor is a G protein-coupled receptor (GPCR), which is activated by an endogenous peptide GPR15L(25–81) and a C-terminal peptide fragment GPR15L(71–81). GPR15 signals through the Gi/o pathway to decrease intracellular cyclic adenosine 3′,5′-monophosphate (cAMP). However, the activation profiles of the GPR15 receptor within Gi/o subtypes have not been examined. Moreover, whether the receptor can also couple to Gs, Gq/11 and G12/13 is unclear. Here, GPR15L(25–81) and GPR15L(71–81) are used as pharmacological tool compounds to delineate the GPR15 receptor-mediated Gα protein signalling using a G protein activation assay and second messenger assay conducted on living cells. The results show that the GPR15 receptor preferentially couples to Gi/o rather than other pathways in both assays. Within the Gi/o family, the GPR15 receptor activates all the subtypes (Gi1, Gi2, Gi3, GoA, GoB and Gz). The Emax and activation rates of Gi1, Gi2, Gi3, GoA and GoB are similar, whilst the Emax of Gz is smaller and the activation rate is significantly slower. The potencies of both peptides toward each Gi/o subtype have been determined. Furthermore, the GPR15 receptor signals through Gi/o to inhibit cAMP accumulation, which could be blocked by the application of the Gi/o inhibitor pertussis toxin.

Published
2022

2. Molecular insights into ligand recognition and G protein coupling of the neuromodulatory orphan receptor GPR139

Author

Yali Zhou, Henrik Daver, Boris Trapkov, Lijie Wu, Meng Wu, Kasper Harpsøe, Patrick R. Gentry, Kaiwen Liu, Marina Larionova, Junlin Liu, Na Chen, Hans Bräuner-Osborne, David E. Gloriam, Tian Hua, and Zhi-Jie Liu

Subjects
Cryoelectron microscopy, GTP-Binding Proteins, Extracellular signalling molecules, Nerve Tissue Proteins, Cell Biology, Ligands, Molecular Biology, Letter to the Editor, Receptors, G-Protein-Coupled
Abstract

The G protein-coupled receptor GPR139 is involved in neuromodulation, and one of its agonists is in clinical trials for the treatment of cognitive impairment and negative symptoms of schizophrenia. While GPR139 is a understudied ‘orphan’ receptor, it can be activated by the amino acids L-Trp, L-Phe1 or α-Melanocyte-stimulating hormone (α-MSH) which is an endogenous agonist of melanocortin receptors.2,3 GPR139 activation triggers several G protein pathways of which Gq/11 is the primary.4,5,6,7 Of note, the expression of GPR139 correlates with that of the μ-opioid and dopamine D2 receptors in a broad range of the central nervous system (CNS), which acts as a regulator of μ-opioid and dopamine signaling.6,7,8,9 For example, GPR139 antagonist JNJ-3792165 increases the sensitivity of the μ-opioid receptor to morphine.6 Hitherto, the structural basis of how ligands interact with and activate GPR139 to transduce diverse signals has remained unknown. Furthermore, the more physiologically relevant intermediate states of GPCR–G protein complex structures in the nucleotide-bound forms are also elusive. Here, we report the cryo-electron microscopy (cryo-EM) structures of GPR139 in complex with a key reference ligand JNJ-63533054 which is an analog of agent TAK-04110 in clinical trial, and miniGs/q or Gi in nucleotide-free form, as well as the GPR139–JNJ-63533054–miniGs/q complex in GDP- and GTP-bound states, respectively (Fig. 1a–f).

Published
2021

3. Identification of a Novel Allosteric Site at the M5 Muscarinic Acetylcholine Receptor

Author

Christopher J. Langmead, Mahmuda Yeasmin, Arthur Christopoulos, Geoff Thompson, Alice E. Berizzi, Emma T van der Westhuizen, Celine Valant, David M. Thal, Andrew B. Tobin, Patrick M. Sexton, Ziva Vuckovic, Wessel A.C. Burger, Patrick R. Gentry, and Craig W. Lindsley

Subjects
0303 health sciences, Allosteric modulator, Physiology, Chemistry, Cognitive Neuroscience, Mutagenesis, Allosteric regulation, Cell Biology, General Medicine, Biochemistry, Transmembrane protein, 3. Good health, Cell biology, 03 medical and health sciences, 0302 clinical medicine, Muscarinic acetylcholine receptor, Extracellular, Binding site, Receptor, 030217 neurology & neurosurgery, 030304 developmental biology
Abstract

The M5 muscarinic acetylcholine receptor (mAChR) has emerged as an exciting therapeutic target for the treatment of addiction and behavioral disorders. This has been in part due to promising preclinical studies with the M5 mAChR selective negative allosteric modulator (NAM), ML375. The binding site of ML375 remains unknown, however, making it difficult to develop improved M5 mAChR selective modulators. To determine the possible location of the ML375 binding site, we used radioligand binding and functional assays to show that ML375 does not interact with the well-characterized "common" mAChR allosteric site located in the receptor's extracellular vestibule, nor a previously proposed second allosteric site recognized by the modulator, amiodarone. Molecular docking was used to predict potential allosteric sites within the transmembrane (TM) domain of the M5 mAChR. These predicted sites were assessed using M5-M2 mAChR receptor chimeras and further targeted with site-directed mutagenesis, which enabled the identification of a putative binding site for ML375 at the interface of TMs 2-4. Collectively, these results identify a third allosteric site at the M5 mAChR and highlight the ability of allosteric modulators to selectively target highly conserved proteins.

Published
2021

4. Pharmacological characterization of novel small molecule agonists and antagonists for the orphan receptor GPR139

Author

Lisa Pallareti, Tine F. Rath, Boris Trapkov, Tsonko Tsonkov, Anders Thorup Nielsen, Kasper Harpsøe, Patrick R. Gentry, Hans Bräuner-Osborne, David E. Gloriam, and Simon R. Foster

Subjects
Pharmacology
Abstract

The orphan G protein-coupled receptor GPR139 is predominantly expressed in the central nervous system and has attracted considerable interest as a therapeutic target. However, the biological role of this receptor remains somewhat elusive, in part due to the lack of quality pharmacological tools to investigate GPR139 function. In an effort to understand GPR139 signaling and to identify improved compounds, in this study we performed virtual screening and analog searches, in combination with multiple pharmacological assays. We characterized GPR139-dependent signaling using previously published reference agonists in Ca 2+ mobilization and inositol monophosphate accumulation assays, as well as a novel real-time GPR139 internalization assay. For the four reference agonists tested, the rank order of potency was conserved across signaling and internalization assays: JNJ-63533054 > Compound 1a » Takeda > AC4 > DL43, consistent with previously reported values. We noted an increased efficacy of JNJ-63533054-mediated inositol monophosphate signaling and internalization, relative to Compound 1a. We then performed virtual screening for GPR139 agonist and antagonist compounds that were screened and validated in GPR139 functional assays. We identified four GPR139 agonists that were active in all assays, with similar or reduced potency relative to known compounds. Likewise, compound analogs selected based on GPR139 agonist and antagonist substructure searches behaved similarly to their parent compounds. Thus, we have characterized GPR139 signaling for multiple new ligands using G protein-dependent assays and a new real-time internalization assay. These data add to the GPR139 tool compound repertoire, which could be optimized in future medical chemistry campaigns.

Published
2023

5. Identification of a Novel Allosteric Site at the M

Author

Wessel A C, Burger, Patrick R, Gentry, Alice E, Berizzi, Ziva, Vuckovic, Emma T, van der Westhuizen, Geoff, Thompson, Mahmuda, Yeasmin, Craig W, Lindsley, Patrick M, Sexton, Christopher J, Langmead, Andrew B, Tobin, Arthur, Christopoulos, Celine, Valant, and David M, Thal

Subjects
Molecular Docking Simulation, Binding Sites, Allosteric Regulation, Receptor, Muscarinic M4, Receptor, Muscarinic M1, Receptors, Muscarinic, Allosteric Site
Abstract

The M

Published
2021

6. Crystal structure of the M5 muscarinic acetylcholine receptor

Author

Wessel A.C. Burger, Arthur Christopoulos, Jonathan B. Baell, Emma T van der Westhuizen, Geoff Thompson, Christopher J. Langmead, Celine Valant, Patrick R. Gentry, Kunio Hirata, Ziva Vuckovic, Raphaël Rahmani, Swapna Varghese, Patrick M. Sexton, David M. Thal, Alice E. Berizzi, Craig W. Lindsley, and Andrew B. Tobin

Subjects
Models, Molecular, crystal structure, drug design, Protein Conformation, Allosteric regulation, Ligands, Receptor subtype, 03 medical and health sciences, muscarinic receptor, 0302 clinical medicine, Allosteric Regulation, X-Ray Diffraction, Muscarinic acetylcholine receptor, Extracellular, Inverse agonist, Humans, G protein-coupled receptor, Receptor, 030304 developmental biology, Pharmacology, 0303 health sciences, Multidisciplinary, Binding Sites, Receptor, Muscarinic M5, Ligand, Chemistry, Rational design, Biological Sciences, Receptors, Muscarinic, 3. Good health, Kinetics, Drug development, Crystallization, Neuroscience, 030217 neurology & neurosurgery, Allosteric Site
Abstract

Significance The 5 subtypes of the muscarinic acetylcholine receptors (mAChRs) are expressed throughout the central and peripheral nervous system where they play a vital role in physiology and pathologies. Recently, the M5 mAChR subtype has emerged as an exciting drug target for the treatment of drug addiction. We have determined the atomic structure of the M5 mAChR bound to the clinically used inverse agonist tiotropium. The M5 mAChR structure now allows for a full comparison of all 5 mAChR subtypes and reveals that small differences in the extracellular loop regions can mediate orthosteric and allosteric ligand selectivity. Together, these findings open the door for future structure-based design of selective drugs that target this therapeutically important class of receptors., The human M5 muscarinic acetylcholine receptor (mAChR) has recently emerged as an exciting therapeutic target for treating a range of disorders, including drug addiction. However, a lack of structural information for this receptor subtype has limited further drug development and validation. Here we report a high-resolution crystal structure of the human M5 mAChR bound to the clinically used inverse agonist, tiotropium. This structure allowed for a comparison across all 5 mAChR family members that revealed important differences in both orthosteric and allosteric sites that could inform the rational design of selective ligands. These structural studies, together with chimeric swaps between the extracellular regions of the M2 and M5 mAChRs, provided structural insight into kinetic selectivity, where ligands show differential residency times between related family members. Collectively, our study provides important insights into the nature of orthosteric and allosteric ligand interaction across the mAChR family that could be exploited for the design of selective drugs.

Published
2019

7. Discovery and Optimization of Potent and CNS Penetrant M5-Preferring Positive Allosteric Modulators Derived from a Novel, Chiral N-(Indanyl)piperidine Amide Scaffold

Author

Kellie D. Nance, Colleen M. Niswender, Christopher J. Langmead, Aaron M. Bender, Hyekyung P. Cho, Karl R. Voigtritter, P. Jeffrey Conn, Carrie K. Jones, Thomas M. Bridges, Sichen Chang, Patrick R. Gentry, Vincent B. Luscombe, Kaelyn S. Lingenfelter, Alice E. Berizzi, Jordan C. O’Neill, Craig W. Lindsley, Arthur Christopoulos, Charles W. Locuson, Patrick M. Sexton, and Xiaoyan Zhan

Subjects
0301 basic medicine, Allosteric modulator, Physiology, Stereochemistry, Cognitive Neuroscience, Allosteric regulation, Cell Biology, General Medicine, Biochemistry, Small molecule, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, stomatognathic system, chemistry, Amide, parasitic diseases, Muscarinic acetylcholine receptor, Piperidine, Selectivity, Penetrant (biochemical), 030217 neurology & neurosurgery
Abstract

The pharmacology of the M5 muscarinic acetylcholine receptor (mAChR) is the least understood of the five mAChR subtypes due to a historic lack of selective small molecule tools. To address this shortcoming, we have continued the optimization effort around the prototypical M5 positive allosteric modulator (PAM) ML380 and have discovered and optimized a new series of M5 PAMs based on a chiral N-(indanyl)piperidine amide core with robust SAR, human and rat M5 PAM EC50 values

Published
2018

8. Identification of a novel scaffold for a small molecule GPR139 receptor agonist

Author

Rina Pokhrel, Hans Bräuner-Osborne, Maria Vallianou, Patrick R. Gentry, Mohamed A. Shehata, Simon R. Foster, Daniel Palmer, David E. Gloriam, and Anne Cathrine Nøhr

Subjects
0301 basic medicine, Agonist, medicine.drug_class, lcsh:Medicine, Mutagenesis (molecular biology technique), Nerve Tissue Proteins, CHO Cells, Article, Receptors, G-Protein-Coupled, 03 medical and health sciences, Cricetulus, 0302 clinical medicine, medicine, Animals, Binding site, lcsh:Science, Receptor, G protein-coupled receptor, Binding Sites, Multidisciplinary, biology, Chemistry, Chinese hamster ovary cell, lcsh:R, biology.organism_classification, Small molecule, 3. Good health, 030104 developmental biology, Biochemistry, lcsh:Q, 030217 neurology & neurosurgery
Abstract

GPR139 is an orphan G protein-coupled receptor (GPCR) that is primarily expressed in the brain in regions known to regulate motor control and metabolism. Here, we screened a diverse 4,000 compound library in order to identify GPR139 agonists. We identified 11 initial hits in a calcium mobilization screen, including one compound, AC4, which contains a different chemical scaffold to what has previously been described for GPR139 agonists. Our mutagenesis data shows that AC4 interacts with the same hotspots in the binding site of GPR139 as those reported to interact with the reference agonists 1a and 7c. We additionally tested and validated 160 analogs in a calcium mobilization assay and found 5 compounds with improved potency compared to AC4. In total, we identified 36 GPR139 agonists with potencies in the nanomolar range (90–990 nM). The most potent compounds were confirmed as GPR139 agonists using an orthogonal ERK phosphorylation assay where they displayed a similar rank order of potency. Accordingly, we herein introduce multiple novel GPR139 agonists, including one with a novel chemical scaffold, which can be used as tools for future pharmacological and medicinal chemistry exploration of GPR139.

Published
2019

9. Discovery of 3-aminopicolinamides as metabotropic glutamate receptor subtype 4 (mGlu4) positive allosteric modulator warheads engendering CNS exposure and in vivo efficacy

Author

Pedro M. Garcia-Barrantes, Colleen M. Niswender, J. Scott Daniels, Corey R. Hopkins, Rocco D. Gogliotti, P. Jeffrey Conn, Carrie K. Jones, Darren W. Engers, Analisa D. Thompson, Patrick R. Gentry, Anna L. Blobaum, Ryan D. Morrison, Joseph D. Panarese, and Craig W. Lindsley

Subjects
Central Nervous System, 0301 basic medicine, Allosteric modulator, Clinical Biochemistry, Allosteric regulation, Pharmaceutical Science, Pharmacology, Catalepsy, Receptors, Metabotropic Glutamate, Biochemistry, Article, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, Allosteric Regulation, In vivo, Drug Discovery, medicine, Animals, Humans, Potency, Structure–activity relationship, Molecular Biology, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Metabotropic glutamate receptor 4, Organic Chemistry, medicine.disease, Amides, Rats, Disease Models, Animal, 030104 developmental biology, Metabotropic glutamate receptor, Picolines, Molecular Medicine, 030217 neurology & neurosurgery
Abstract

This letter describes the further chemical optimization of the picolinamide-derived family of mGlu4 PAMs wherein we identified a 3-amino substituent to the picolinamide warhead that engendered potency, CNS penetration and in vivo efficacy. From this optimization campaign, VU0477886 emerged as a potent (EC50 = 95 nM, 89% Glu Max) mGlu4 PAM with an attractive DMPK profile (brain:plasma Kp = 1.3), rat CLp = 4.0 mL/min/kg, t1/2 = 3.7 h) and robust efficacy in our standard preclinical Parkinson's disease model, haloperidol-induced catalepsy (HIC).

Published
2016

10. Discovery and Optimization of Potent and CNS Penetrant M

Author

Aaron M, Bender, Hyekyung P, Cho, Kellie D, Nance, Kaelyn S, Lingenfelter, Vincent B, Luscombe, Patrick R, Gentry, Karl, Voigtritter, Alice E, Berizzi, Patrick M, Sexton, Christopher J, Langmead, Arthur, Christopoulos, Charles W, Locuson, Thomas M, Bridges, Sichen, Chang, Jordan C, O'Neill, Xiaoyan, Zhan, Colleen M, Niswender, Carrie K, Jones, P Jeffrey, Conn, and Craig W, Lindsley

Subjects
Male, Molecular Structure, Cholinergic Agents, Brain, Amides, Receptors, Muscarinic, Article, Rats, Sprague-Dawley, Structure-Activity Relationship, Allosteric Regulation, Piperidines, Drug Discovery, Microsomes, Liver, Animals, Humans
Abstract

[Image: see text] The pharmacology of the M(5) muscarinic acetylcholine receptor (mAChR) is the least understood of the five mAChR subtypes due to a historic lack of selective small molecule tools. To address this shortcoming, we have continued the optimization effort around the prototypical M(5) positive allosteric modulator (PAM) ML380 and have discovered and optimized a new series of M(5) PAMs based on a chiral N-(indanyl)piperidine amide core with robust SAR, human and rat M(5) PAM EC(50) values

Published
2018

11. Discovery of (S)-2-Cyclopentyl-N-((1-isopropylpyrrolidin2-yl)-9-methyl-1-oxo-2,9-dihydro-1H-pyrrido[3,4-b]indole-4-carboxamide (VU0453379): A Novel, CNS Penetrant Glucagon-Like Peptide 1 Receptor (GLP-1R) Positive Allosteric Modulator (PAM)

Author

Lindsey C. Morris, Carrie K. Jones, Ryan D. Morrison, Emily Days, Kellie D. Nance, Colleen M. Niswender, Kevin D. Niswender, Chuck W. Locuson, C. David Weaver, Analisa D. Thompson, Patrick R. Gentry, Craig W. Lindsley, and J. Scott Daniels

Subjects
Male, endocrine system, Allosteric modulator, Indoles, Pyrrolidines, Brief Article, medicine.drug_class, Allosteric regulation, Carboxamide, Pharmacology, Glucagon-Like Peptide-1 Receptor, chemistry.chemical_compound, Islets of Langerhans, Structure-Activity Relationship, Allosteric Regulation, Glucagon-Like Peptide 1, Drug Discovery, Insulin Secretion, medicine, Receptors, Glucagon, Structure–activity relationship, Animals, Insulin, Receptor, Indole test, Catalepsy, Chemistry, Venoms, Pancreatic islets, Drug Synergism, High-Throughput Screening Assays, Mice, Inbred C57BL, medicine.anatomical_structure, Biochemistry, Microsomes, Liver, Molecular Medicine, Exenatide, Haloperidol, Penetrant (biochemical), Peptides, Central Nervous System Agents
Abstract

A duplexed, functional multiaddition high throughput screen and subsequent iterative parallel synthesis effort identified the first highly selective and CNS penetrant glucagon-like peptide-1R (GLP-1R) positive allosteric modulator (PAM). PAM (S)-9b potentiated low-dose exenatide to augment insulin secretion in primary mouse pancreatic islets, and (S)-9b alone was effective in potentiating endogenous GLP-1R to reverse haloperidol-induced catalepsy.

Published
2014

12. Development of a Highly Potent, Novel M5 Positive Allosteric Modulator (PAM) Demonstrating CNS Exposure: 1-((1H-Indazol-5-yl)sulfoneyl)-N-ethyl-N-(2-(trifluoromethyl)benzyl)piperidine-4-carboxamide (ML380)

Author

Colleen M. Niswender, Meredith J. Noetzel, Michael R. Wood, Patrick R. Gentry, Peter Chase, Masaya Kokubo, Thomas M. Bridges, Emery Smith, P. Jeffrey Conn, Atin Lamsal, Craig W. Lindsley, Peter Hodder, J. Scott Daniels, and Hyekyung P. Cho

Subjects
Central Nervous System, Male, Indazoles, Allosteric modulator, Brief Article, Stereochemistry, medicine.drug_class, Allosteric regulation, Drug Evaluation, Preclinical, Carboxamide, Substrate Specificity, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Allosteric Regulation, Piperidines, Drug Discovery, Muscarinic acetylcholine receptor, medicine, Animals, Humans, Potency, 030304 developmental biology, Sulfonamides, 0303 health sciences, Receptor, Muscarinic M5, Trifluoromethyl, Chemistry, Drug discovery, High-Throughput Screening Assays, Rats, 3. Good health, Molecular Medicine, Piperidine, 030217 neurology & neurosurgery
Abstract

A functional high throughput screen identified a novel chemotype for the positive allosteric modulation (PAM) of the muscarinic acetylcholine receptor (mAChR) subtype 5 (M5). Application of rapid analog, iterative parallel synthesis efficiently optimized M5 potency to arrive at the most potent M5 PAMs prepared to date and provided tool compound 8n (ML380) demonstrating modest CNS penetration (human M5 EC50 = 190 nM, rat M5 EC50 = 610 nM, brain to plasma ratio (Kp) of 0.36).

Published
2014

13. M5Receptor Activation Produces Opposing Physiological Outcomes in Dopamine Neurons Depending on the Receptor's Location

Author

Craig W. Lindsley, Zixiu Xiang, M. R. Wood, Patrick R. Gentry, Colleen M. Niswender, David Sulzer, P.J. Conn, Thomas M. Bridges, Daniel J. Foster, and José E. Lizardi-Ortiz

Subjects
Indoles, Dopamine, Substantia nigra, CHO Cells, Striatum, In Vitro Techniques, Biology, Transfection, Membrane Potentials, Rats, Sprague-Dawley, Mice, Cricetulus, medicine, Animals, Receptor, Mice, Knockout, Receptor, Muscarinic M5, Dose-Response Relationship, Drug, Pars compacta, Dopaminergic Neurons, General Neuroscience, Dopaminergic, Brain, Long-term potentiation, Articles, Rats, Mice, Inbred C57BL, medicine.anatomical_structure, Animals, Newborn, nervous system, Calcium, Neuron, Neuroscience, Protein Binding, medicine.drug
Abstract

Of the five muscarinic receptor subtypes, the M5receptor is the only one detectable in midbrain dopaminergic neurons, making it an attractive potential therapeutic target for treating disorders in which dopaminergic signaling is disrupted. However, developing an understanding of the role of M5in regulating midbrain dopamine neuron function has been hampered by a lack of subtype-selective compounds. Here, we extensively characterize the novel compound VU0238429 and demonstrate that it acts as a positive allosteric modulator with unprecedented selectivity for the M5receptor. We then used VU0238429, along with M5knock-out mice, to elucidate the role of this receptor in regulating substantia nigra pars compacta (SNc) neuron physiology in both mice and rats. In sagittal brain slices that isolate the SNc soma from their striatal terminals, activation of muscarinic receptors induced Ca2+mobilization and inward currents in SNc dopamine neurons, both of which were potentiated by VU0238429 and absent in M5knock-out mice. Activation of M5also increased the spontaneous firing rate of SNc neurons, suggesting that activation of somatodendritic M5increases the intrinsic excitability of SNc neurons. However, in coronal slices of the striatum, potentiation of M5with VU0238429 resulted in an inhibition in dopamine release as monitored with fast scan cyclic voltammetry. Accordingly, activation of M5can lead to opposing physiological outcomes depending on the location of the receptor. Although activation of somatodendritic M5receptors on SNc neurons leads to increased neuronal firing, activation of M5receptors in the striatum induces an inhibition in dopamine release.

Published
2014

14. Drugs for Allosteric Sites on Receptors

Author

Craig W. Lindsley, Patrick R. Gentry, Thomas P. Mathews, and Cody J. Wenthur

Subjects
Pharmacology, Molecular switch, Drug discovery, Stereochemistry, Allosteric regulation, Druggability, Computational biology, Biology, Ligands, Toxicology, Small molecule, Article, Receptors, G-Protein-Coupled, Structure-Activity Relationship, Allosteric Regulation, Pharmaceutical Preparations, Allosteric enzyme, Drug Design, biology.protein, Humans, Signal transduction, Allosteric Site, Signal Transduction, G protein-coupled receptor
Abstract

The presence of druggable, topographically distinct allosteric sites on a wide range of receptor families has offered new paradigms for small molecules to modulate receptor function. Moreover, ligands that target allosteric sites offer significant advantages over the corresponding orthosteric ligands in terms of selectivity, including subtype selectivity within receptor families, and can also impart improved physicochemical properties. However, allosteric ligands are not a panacea. Many chemical issues (e.g., flat structure-activity relationships) and pharmacological issues (e.g., ligand-biased signaling) that are allosteric centric have emerged. Notably, the fact that allosteric sites are less evolutionarily conserved leads to improved selectivity; however, this can also lead to species differences that can hinder safety assessment. Many allosteric ligands possess molecular switches, wherein a small structural change (chemical or metabolic) can modulate the mode of pharmacology or receptor subtype selectivity. As the field has matured, as described here, key principles and strategies have emerged for the design of ligands/drugs for allosteric sites.

Published
2014

15. Discovery of the First M5-Selective and CNS Penetrant Negative Allosteric Modulator (NAM) of a Muscarinic Acetylcholine Receptor: (S)-9b-(4-Chlorophenyl)-1-(3,4-difluorobenzoyl)-2,3-dihydro-1H-imidazo[2,1-a]isoindol-5(9bH)-one (ML375)

Author

Peter Chase, Thomas M. Bridges, Nathan R. Kett, Colleen M. Niswender, Patrick R. Gentry, Peter Hodder, Michael R. Wood, Masaya Kokubo, J. Scott Daniels, P. Jeffrey Conn, Hyekyung P. Cho, Emery Smith, Craig W. Lindsley, and Joel M. Harp

Subjects
Allosteric modulator, biology, Stereochemistry, Chemistry, Drug discovery, Allosteric regulation, Pharmacology, biology.organism_classification, Drug Discovery, Muscarinic acetylcholine receptor, Molecular Medicine, Structure–activity relationship, Cricetulus, Receptor, IC50
Abstract

A functional high throughput screen and subsequent multidimensional, iterative parallel synthesis effort identified the first muscarinic acetylcholine receptor (mAChR) negative allosteric modulator (NAM) selective for the M5 subtype. ML375 is a highly selective M5 NAM with submicromolar potency (human M5 IC50 = 300 nM, rat M5 IC50 = 790 nM, M1–M4 IC50 > 30 μM), excellent multispecies PK, high CNS penetration, and enantiospecific inhibition.

Published
2013

16. Molecular Mechanisms of Action of M5 Muscarinic Acetylcholine Receptor Allosteric Modulators

Author

Sandra Den Hoedt, Christopher J. Langmead, Patrick R. Gentry, Arthur Christopoulos, Patrick M. Sexton, Alice E. Berizzi, and Patricia Rueda

Subjects
0301 basic medicine, Agonist, Atropine, Allosteric modulator, Carbachol, Indazoles, Indoles, medicine.drug_class, Inositol Phosphates, Allosteric regulation, CHO Cells, Pharmacology, Partial agonist, 03 medical and health sciences, Radioligand Assay, 0302 clinical medicine, Cricetulus, Allosteric Regulation, Cricetinae, Muscarinic acetylcholine receptor, medicine, Animals, Humans, Sulfonamides, Receptor, Muscarinic M5, Phenoxybenzamine, Chemistry, Imidazoles, Cooperative binding, Acetylcholine, 030104 developmental biology, Molecular Medicine, 030217 neurology & neurosurgery, Allosteric Site, medicine.drug
Abstract

Recently, the first subtype-selective allosteric modulators of the M5 muscarinic acetylcholine receptor (mAChR) have been described, but their molecular mechanisms of action remain unknown. Using radioligand-binding and functional assays of inositol phosphate (IP) accumulation and Ca(2+) mobilization in a recombinant cell line stably expressing the human M5 mAChR, we investigated the effects of the positive allosteric modulator (PAM), ML380, and negative allosteric modulator, ML375. In functional assays, ML380 caused robust enhancements in the potency of the full agonists, acetylcholine (ACh), carbachol, and oxotremorine-M, while significantly increasing the maximal response to the partial agonist, pilocarpine. ML380 also demonstrated direct allosteric agonist activity. In contrast, ML375 displayed negative cooperativity with each of the agonists in a manner that varied with the pathway investigated and progressively reduced the maximal pilocarpine response. Radioligand-binding affinity cooperativity estimates were consistent with values derived from functional assays in some instances but not others, suggesting additional allosteric effects on orthosteric ligand efficacy. For ML375 this was confirmed in IP assays performed after reduction of receptor reserve by the alkylating agent, phenoxybenzamine, as it reduced the maximal ACh response. In contrast, ML380 enhanced only ACh potency after receptor alkylation, with no effect on maximal response, consistent with studies of the M1 mAChR with the prototypical PAM, BQZ12. Interaction studies between ML380 and ML375 also indicated that they most likely used an overlapping allosteric site. Our findings indicate that novel small-molecule modulators of the M5 mAChR display mixed mechanisms of action compared with previously characterized modulators of other mAChRs.

Published
2016

17. In Vivo Structure−Activity Relationship Study of Dorsomorphin Analogues Identifies Selective VEGF and BMP Inhibitors

Author

Corey R. Hopkins, R. Nathan Daniels, Craig W. Lindsley, Charles C. Hong, Jijun Hao, Joshua N. Ho, Kaleh A. Karim, Patrick R. Gentry, and Jana A. Lewis

Subjects
Vascular Endothelial Growth Factor A, Embryo, Nonmammalian, animal structures, Angiogenesis, Drug Evaluation, Preclinical, Biology, Pharmacology, Bone morphogenetic protein, Biochemistry, Article, Structure-Activity Relationship, chemistry.chemical_compound, In vivo, Animals, Receptor, Zebrafish, General Medicine, biology.organism_classification, Vascular Endothelial Growth Factor Receptor-2, Embryonic stem cell, BMPR2, Cell biology, Vascular endothelial growth factor, Pyrimidines, chemistry, Bone Morphogenetic Proteins, embryonic structures, Quinolines, Pyrazoles, Molecular Medicine
Abstract

The therapeutic potential of small molecule signaling inhibitors is often limited by off-target effects. Recently, in a screen for compounds that perturb the zebrafish embryonic dorsoventral axis, we identified dorsomorphin, the first selective inhibitor of bone morphogenetic protein (BMP) signaling. Here we show that dorsomorphin has significant "off-target" effects against the VEGF (vascular endothelial growth factor) type-2 receptor (Flk1/KDR) and disrupts zebrafish angiogenesis. Since both BMP and VEGF signals are known to be involved in vascular development, we sought to determine whether dorsomorphin's antiangiogenic effects are due to its impact on the BMP or VEGF signals through the development of analogues that target BMP but not VEGF signaling and vice versa. In a structure-activity relationship (SAR) study of dorsomorphin analogues based primarily on their effects on live zebrafish embryos, we identified highly selective and potent BMP inhibitors as well as selective VEGF inhibitors. One of the BMP inhibitors, DMH1, which exclusively targets the BMP but not the VEGF pathway, dorsalized the embryonic axis without disrupting the angiogenic process, demonstrating that BMP signaling was not involved in the angiogenic process. This is one of the first full-scale SAR studies performed in vertebrates and demonstrates the potential of zebrafish as an attractive complementary platform for drug development that incorporates an assessment of in vivo bioactivity and selectivity in the context of a living organism.

Published
2010

18. Synthesis and Structure-Activity Relationships of Allosteric Potentiators of the M4Muscarinic Acetylcholine Receptor

Author

Alexander S. Kane, Thomas M. Bridges, Craig W. Lindsley, Ashley E. Brady, Patrick R. Gentry, P. Jeffrey Conn, J. Phillip Kennedy, Carrie K. Jones, Jana K. Shirey, and John T. Brogan

Subjects
Pharmacology, Receptor, Muscarinic M4, Stereochemistry, Organic Chemistry, CHO Cells, Muscarinic Agonists, Biochemistry, Article, Structure-Activity Relationship, Cricetulus, Allosteric Regulation, Cricetinae, Drug Discovery, Animals, Molecular Medicine, University medical, General Pharmacology, Toxicology and Pharmaceutics
Abstract

J. Phillip Kennedy[a],+, Thomas M. Bridges[b],+, Patrick R. Gentry[b], John T. Brogan[a], Alexander S. Kane[b], Carrie K. Jones[b],[c], Ashley E. Brady[b], Jana K. Shirey[b], P. Jeffrey Conn [Prof.][b], and Craig W. Lindsley [Prof.]*,[a],[b] [a] Department of Chemistry, Vanderbilt University 12475 MRB4, Nashville, TN 37232-6600 (USA) [b] Vanderbilt Program in Drug Discovery, Department of Pharmacology Vanderbilt University Medical Center 12475 MRB4, Nashville, TN 37232-6600 (USA)

Published
2009

19. Synthesis and SAR of analogues of the M1 allosteric agonist TBPB. Part I: Exploration of alternative benzyl and privileged structure moieties

Author

Nicole R. Miller, Kwango Kim, Ashley E. Brady, Micah L. Breininger, Thomas M. Bridges, John T. Brogan, P. Jeffrey Conn, J. Phillip Kennedy, Carrie K. Jones, Craig W. Lindsley, R. Nathan Daniels, and Patrick R. Gentry

Subjects
Agonist, Time Factors, medicine.drug_class, Stereochemistry, Chemistry, Pharmaceutical, Clinical Biochemistry, Allosteric regulation, Pharmaceutical Science, Ligands, Biochemistry, Chemical synthesis, Article, Inhibitory Concentration 50, Structure-Activity Relationship, Allosteric Regulation, Piperidines, Drug Discovery, medicine, Humans, Structure–activity relationship, Binding site, skin and connective tissue diseases, Molecular Biology, Binding Sites, Dose-Response Relationship, Drug, Bicyclic molecule, Chemistry, Receptor, Muscarinic M1, Organic Chemistry, Highly selective, Acetylcholine, Models, Chemical, Drug Design, Molecular Medicine, Benzimidazoles, Selectivity, Allosteric Site
Abstract

This Letter describes the first account of the synthesis and SAR, developed through an iterative analogue library approach, of analogues of the highly selective M1 allosteric agonist TBPB. With slight structural changes, mAChR selectivity was maintained, but the degree of partial M1 agonism varied considerably.

Published
2008

20. Centrally Active Allosteric Potentiators of the M4 Muscarinic Acetylcholine Receptor Reverse Amphetamine-Induced Hyperlocomotor Activity in Rats

Author

Satyawan Jadhav, P. Jeffrey Conn, Patrick R. Gentry, Ashley E. Brady, Craig W. Lindsley, Huiyong Yin, Carrie K. Jones, Thomas M. Bridges, Justin U. Heiman, Analisa D. Thompson, J. Phillip Kennedy, Micah L. Breininger, and Jana K. Shirey

Subjects
Agonist, Pyridines, medicine.drug_class, Dopamine, Allosteric regulation, Thiophenes, Motor Activity, Pharmacology, Article, chemistry.chemical_compound, Allosteric Regulation, Mesencephalon, Muscarinic acetylcholine receptor, medicine, Muscarinic acetylcholine receptor M4, Animals, Receptor, Muscarinic M4, Chemistry, Muscarinic acetylcholine receptor M2, Potentiator, Acetylcholine, Rats, Molecular Medicine, Xanomeline, medicine.drug
Abstract

Previous clinical and animal studies suggest that selective activators of M(1) and/or M(4) muscarinic acetylcholine receptors (mAChRs) have potential as novel therapeutic agents for treatment of schizophrenia and Alzheimer's disease. However, highly selective centrally penetrant activators of either M(1) or M(4) have not been available, making it impossible to determine the in vivo effects of selective activation of these receptors. We previously identified VU10010 [3-amino-N-(4-chlorobenzyl)-4, 6-dimethylthieno[2,3-b]pyridine-2-carboxamide] as a potent and selective allosteric potentiator of M(4) mAChRs. However, unfavorable physiochemical properties prevented use of this compound for in vivo studies. We now report that chemical optimization of VU10010 has afforded two centrally penetrant analogs, VU0152099 [3-amino-N-(benzo[d][1,3]dioxol-5-ylmethyl)-4,6-dimethylthieno[2,3-b]pyridine carboxamide] and VU0152100 [3-amino-N-(4-methoxybenzyl)-4,6-dimethylthieno[2,3-b]pyridine carboxamide], that are potent and selective positive allosteric modulators of M(4). VU0152099 and VU0152100 had no agonist activity but potentiated responses of M(4) to acetylcholine. Both compounds were devoid of activity at other mAChR subtypes or at a panel of other GPCRs. The improved physiochemical properties of VU0152099 and VU0152100 allowed in vivo dosing and evaluation of behavioral effects in rats. Interestingly, these selective allosteric potentiators of M(4) reverse amphetamine-induced hyperlocomotion in rats, a model that is sensitive to known antipsychotic agents and to nonselective mAChR agonists. This is consistent with the hypothesis that M(4) plays an important role in regulating midbrain dopaminergic activity and raises the possibility that positive allosteric modulation of M(4) may mimic some of the antipsychotic-like effects of less selective mAChR agonists.

Published
2008

21. Further optimization of the M5 NAM MLPCN probe ML375: tactics and challenges

Author

Michael R. Wood, Craig W. Lindsley, Masaya Kokubo, Hyekyung P. Cho, P. Jeffrey Conn, Frank W. Byers, Haruto Kurata, Patrick R. Gentry, J. Scott Daniels, Thomas M. Bridges, and Colleen M. Niswender

Subjects
Allosteric modulator, Indoles, Stereochemistry, Clinical Biochemistry, Allosteric regulation, Pharmaceutical Science, Biochemistry, Article, Structure-Activity Relationship, Allosteric Regulation, Drug Discovery, Structure–activity relationship, Distribution (pharmacology), Animals, Humans, Molecular Biology, Receptor, Muscarinic M5, Chemistry, Organic Chemistry, Imidazoles, Brain, Highly selective, Rats, Plasma exposure, Microsomes, Liver, Molecular Medicine, Half-Life, Protein Binding
Abstract

This Letter describes the continued optimization of the MLPCN probe ML375, a highly selective M5 negative allosteric modulator (NAM), through a combination of matrix libraries and iterative parallel synthesis. True to certain allosteric ligands, SAR was shallow, and the matrix library approach highlighted the challenges with M5 NAM SAR within in this chemotype. Once again, enantiospecific activity was noted, and potency at rat and human M5 were improved over ML375, along with slight enhancement in physiochemical properties, certain in vitro DMPK parameters and CNS distribution. Attempts to further enhance pharmacokinetics with deuterium incorporation afforded mixed results, but pretreatment with a pan-P450 inhibitor (1-aminobenzotriazole; ABT) provided increased plasma exposure.

Published
2014

22. Discovery, Synthesis and Characterization of a Highly Muscarinic Acetylcholine Receptor (mAChR)-Selective M5-Orthosteric Antagonist, VU0488130 (ML381): A Novel Molecular Probe

Author

Michael R. Wood, Colleen M. Niswender, Ryan D. Morrison, Patrick R. Gentry, Craig W. Lindsley, Peter Chase, J. Scott Daniels, Thomas M. Bridges, P. Jeffrey Conn, Hyekyung P. Cho, Frank W. Byers, Peter Hodder, Thomas J. Utley, Emery Smith, Masaya Kokubo, and Anuruddha Rajapakse

Subjects
Drug Evaluation, Preclinical, Muscarinic Antagonists, Pharmacology, Biochemistry, Article, Drug Discovery, Muscarinic acetylcholine receptor, Muscarinic acetylcholine receptor M5, Muscarinic acetylcholine receptor M4, medicine, Animals, Humans, General Pharmacology, Toxicology and Pharmaceutics, Receptor, Muscarinic M5, Chemistry, Organic Chemistry, Antagonist, Acetophenones, Muscarinic acetylcholine receptor M3, Muscarinic acetylcholine receptor M2, Isoxazoles, Muscarinic acetylcholine receptor M1, Rats, Molecular Probes, Molecular Medicine, Acetylcholine, Half-Life, Protein Binding, medicine.drug
Abstract

Of the five G-protein-coupled muscarinic acetylcholine receptors (mAChRs; M1–M5), M5 is the least explored and understood due to a lack of mAChR subtype-selective ligands. We recently performed a high-throughput functional screen and identified a number of weak antagonist hits that are selective for the M5 receptor. Here, we report an iterative parallel synthesis and detailed molecular pharmacologic profiling effort that led to the discovery of the first highly selective, central nervous system (CNS)-penetrant M5-orthosteric antagonist, with sub-micromolar potency (hM5 IC50=450 nM, hM5 Ki=340 nM, M1–M4 IC50 >30 μM), enantiospecific inhibition, and an acceptable drug metabolism and pharmacokinetics (DMPK) profile for in vitro and electrophysiology studies. This compound will be a powerful tool and molecular probe for the further investigation into the role of M5 in addiction and other diseases.

Published
2014

23. Discovery of the first M5-selective and CNS penetrant negative allosteric modulator (NAM) of a muscarinic acetylcholine receptor: (S)-9b-(4-chlorophenyl)-1-(3,4-difluorobenzoyl)-2,3-dihydro-1H-imidazo[2,1-a]isoindol-5(9bH)-one (ML375)

Author

Patrick R, Gentry, Masaya, Kokubo, Thomas M, Bridges, Nathan R, Kett, Joel M, Harp, Hyekyung P, Cho, Emery, Smith, Peter, Chase, Peter S, Hodder, Colleen M, Niswender, J Scott, Daniels, P Jeffrey, Conn, Michael R, Wood, and Craig W, Lindsley

Subjects
Male, Indoles, Receptor, Muscarinic M5, Drug Evaluation, Preclinical, Imidazoles, Brain, CHO Cells, Article, Rats, Substrate Specificity, Structure-Activity Relationship, Cricetulus, Allosteric Regulation, Cricetinae, Drug Discovery, Animals, Humans
Abstract

A functional high throughput screen and subsequent multi-dimensional, iterative parallel synthesis effort identified the first muscarinic acetylcholine receptor (mAChR) negative allosteric modulator (NAM) selective for the M5 subtype. ML375 is a highly selective M5 NAM with sub-micromolar potency (human M5 IC50 = 300 nM, rat M5 IC50 = 790 nM, M1–4 IC50 >30 μM), excellent multi-species PK, high CNS penetration, and enantiospecific inhibition.

Published
2013

24. Discovery of ML326: the first sub-micromolar, selective M5 PAM

Author

Peter Chase, Thomas M. Bridges, Colleen M. Niswender, Peter Hodder, Julie L. Engers, Patrick R. Gentry, Emery Smith, J. Scott Daniels, Atin Lamsal, P. Jeffrey Conn, Paige N. Vinson, Craig W. Lindsley, and Michael R. Wood

Subjects
Indoles, Dose-Response Relationship, Drug, Molecular Structure, Extramural, Chemistry, Drug discovery, Stereochemistry, Isatin, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Ether, Biochemistry, Receptors, Muscarinic, Article, Rats, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Molecular Medicine, Structure–activity relationship, Animals, Humans, Selectivity, Molecular Biology
Abstract

This letter describes the further chemical optimization of the M5 PAM MLPCN probes ML129 and ML172. A multi-dimensional iterative parallel synthesis effort quickly explored isatin replacements and a number of southern heterobiaryl variations with no improvement over ML129 and ML172. An HTS campaign identified several weak M5 PAMs (M5 EC50 >10 μM) with a structurally related isatin core that possessed a southern phenethyl ether linkage. While SAR within the HTS series was very shallow and unable to be optimized, grafting the phenethyl ether linkage onto the ML129/ML172 cores led to the first sub-micromolar M5 PAM, ML326 (VU0467903), (human and rat M5 EC50s of 409 nM and 480 nM, respectively) with excellent mAChR selectivity (M1-M4 EC50s

Published
2013

25. Spirocyclic replacements for the isatin in the highly selective, muscarinic M1 PAM ML137: the continued optimization of an MLPCN probe molecule

Author

J. Scott Daniels, Thomas J. Utley, Patrick R. Gentry, Douglas J. Sheffler, P. Jeffrey Conn, Michael S. Poslusney, Craig W. Lindsley, Michael R. Wood, Colleen M. Niswender, Bruce J. Melancon, and Thomas M. Bridges

Subjects
Isatin, Ketone, Pyrrolidines, Stereochemistry, Clinical Biochemistry, Allosteric regulation, Pharmaceutical Science, Biochemistry, Article, chemistry.chemical_compound, Structure-Activity Relationship, Allosteric Regulation, Drug Discovery, Muscarinic acetylcholine receptor, Molecule, Structure–activity relationship, Animals, Humans, Spiro Compounds, Molecular Biology, chemistry.chemical_classification, Organic Chemistry, Receptor, Muscarinic M1, Muscarinic acetylcholine receptor M1, Highly selective, Rats, chemistry, Molecular Medicine, Protein Binding
Abstract

This Letter describes the further optimization of an MLPCN probe molecule (ML137) through the introduction of 5- and 6-membered spirocycles in place of the isatin ketone. Interestingly divergent structure–activity relationships, when compared to earlier M1 PAMs, are presented. These novel spirocycles possess improved efficacy relative to ML137, while also maintaining high selectivity for the human and rat muscarinic M1 receptor subtype.

Published
2012

26. Isatin replacements applied to the highly selective, muscarinic M1 PAM ML137: continued optimization of an MLPCN probe molecule

Author

Margrith E. Mattmann, Michael S. Poslusney, Michael R. Wood, Patrick R. Gentry, Colleen M. Niswender, Bruce J. Melancon, James C. Tarr, P. Jeffrey Conn, Craig W. Lindsley, Thomas M. Bridges, Thomas J. Utley, J. Scott Daniels, and Douglas J. Sheffler

Subjects
Isatin, Monoamine Oxidase Inhibitors, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Subtype selectivity, Biochemistry, Article, chemistry.chemical_compound, Inhibitory Concentration 50, Drug Discovery, Muscarinic acetylcholine receptor, medicine, Moiety, Molecule, Molecular Biology, Molecular Structure, Organic Chemistry, Receptor, Muscarinic M1, Muscarinic acetylcholine receptor M1, Highly selective, chemistry, Molecular Probes, Molecular Medicine, Acetylcholine, medicine.drug
Abstract

This Letter describes the continued optimization of an MLPCN probe molecule (ML137) with a focused effort on the replacement/modification of the isatin moiety present in this highly selective M(1) PAM. A diverse range of structures were validated as viable replacements for the isatin, many of which engendered sizeable improvements in their ability to enhance the potency and efficacy of acetylcholine when compared to ML137. Muscarinic receptor subtype selectivity for the M(1) receptor was also maintained.

Published
2012

27. ChemInform Abstract: Synthesis and SAR of Novel, 4-(Phenylsulfamoyl)phenylacetamide mGlu4 Positive Allosteric Modulators (PAMs) Identified by Functional High-Throughput Screening (HTS)

Author

Colleen M. Niswender, Julie D. Bolinger, P. Jeffrey Conn, Darren W. Engers, Usha N. Menon, Richard Williams, Corey R. Hopkins, C. David Weaver, Craig W. Lindsley, and Patrick R. Gentry

Subjects
Chemistry, High-throughput screening, Allosteric regulation, General Medicine, Combinatorial chemistry
Abstract

Herein we disclose the synthesis and SAR of a series of 4-(phenylsulfamoyl)phenylacetamide compounds as mGlu(4) positive allosteric modulators (PAMs) that were identified via a functional HTS. An iterative parallel approach to these compounds culminated in the discovery of VU0364439 (11) which represents the most potent (19.8 nM) mGlu(4) PAM reported to date.

Published
2010

29. Synthesis and SAR of novel, 4-(phenylsulfamoyl)phenylacetamide mGlu4 positive allosteric modulators (PAMs) identified by functional high-throughput screening (HTS)

Author

C. David Weaver, Julie D. Bolinger, P. Jeffrey Conn, Usha N. Menon, Richard Williams, Colleen M. Niswender, Craig W. Lindsley, Patrick R. Gentry, Darren W. Engers, and Corey R. Hopkins

Subjects
Sulfonamides, Aniline Compounds, Chemistry, medicine.drug_class, Stereochemistry, High-throughput screening, Organic Chemistry, Clinical Biochemistry, Allosteric regulation, Pharmaceutical Science, Carboxamide, Receptors, Metabotropic Glutamate, Biochemistry, Chemical synthesis, Small molecule, Article, Structure-Activity Relationship, Allosteric Regulation, Drug Discovery, medicine, Molecular Medicine, Structure–activity relationship, Molecular Biology
Abstract

Herein we disclose the synthesis and SAR of a series of 4-(phenylsulfamoyl)phenylacetamide compounds as mGlu(4) positive allosteric modulators (PAMs) that were identified via a functional HTS. An iterative parallel approach to these compounds culminated in the discovery of VU0364439 (11) which represents the most potent (19.8 nM) mGlu(4) PAM reported to date.

Published
2010

30. ChemInform Abstract: Synthesis and SAR of a Novel Positive Allosteric Modulator (PAM) of the Metabotropic Glutamate Receptor 4 (mGluR4)

Author

Richard Williams, Kari A. Johnson, Patrick R. Gentry, Craig W. Lindsley, P. Jeffrey Conn, Corey R. Hopkins, Colleen M. Niswender, and Charles David Weaver

Subjects
Allosteric modulator, In vivo, Chemistry, Metabotropic glutamate receptor 4, Biophysics, General Medicine
Abstract

This Letter describes the synthesis and SAR of the novel positive allosteric modulator, VU0155041, a compound that has shown in vivo efficacy in rodent models of Parkinson's disease. The synthesis takes advantage of an iterative parallel synthesis approach to rapidly synthesize and evaluate a number of analogs of VU0155041.

Published
2010

31. Chemical lead optimization of a pan Gq mAChR M1, M3, M5 positive allosteric modulator (PAM) lead. Part II: development of a potent and highly selective M1 PAM

Author

Thomas M. Bridges, J. Phillip Kennedy, Meredith J. Noetzel, Micah L. Breininger, Patrick R. Gentry, P.J. Conn, and Craig W. Lindsley

Subjects
Structure-Activity Relationship, Allosteric Regulation, Drug Design, Organic Chemistry, Clinical Biochemistry, Drug Discovery, Cholinergic Agents, Pharmaceutical Science, Molecular Medicine, Molecular Biology, Biochemistry, Receptors, Muscarinic, Article
Abstract

This Letter describes a chemical lead optimization campaign directed at VU0119498, a pan G(q) mAChR M(1), M(3), M(5) positive allosteric modulator (PAM) with the goal of developing a selective M(1) PAM. An iterative library synthesis approach delivered a potent (M(1) EC(50)=830 nM) and highly selective M(1) PAM (30 microM vs M(2)-M(5)).

Published
2009

32. Chemical Lead Optimization of a pan Gq mAChR M1, M3, M5 Positive Allosteric Modulator (PAM) Lead. Part I. Development of the first highly selective M5 PAM

Author

Craig W. Lindsley, P. Jeffrey Conn, Hyekyung P. Cho, Patrick R. Gentry, Micah L. Breininger, J. Phillip Kennedy, Thomas M. Bridges, and Corey R. Hopkins

Subjects
Allosteric modulator, Stereochemistry, Clinical Biochemistry, Allosteric regulation, Biphenyl derivatives, Pharmaceutical Science, CHO Cells, Biochemistry, Chemical synthesis, Article, Mice, Structure-Activity Relationship, Cricetulus, Allosteric Regulation, Cricetinae, Drug Discovery, Structure–activity relationship, Animals, Molecular Biology, Mice, Knockout, Receptor, Muscarinic M3, Receptor, Muscarinic M5, Chemistry, Organic Chemistry, Receptor, Muscarinic M1, M1 muscarinic receptor, Muscarinic acetylcholine receptor M3, Highly selective, High-Throughput Screening Assays, Drug Design, Molecular Medicine
Abstract

This Letter describes a chemical lead optimization campaign directed at VU0238429, the first M(5)-preferring positive allosteric modulator (PAM), discovered through analog work around VU0119498, a pan G(q) mAChR M(1), M(3), M(5) PAM. An iterative library synthesis approach delivered the first selective M(5) PAM (no activity at M(1)-M(4) @ 30microM), and an important tool compound to study the role of M(5) in the CNS.

Published
2009

33. Synthesis and SAR of a Novel Positive Allosteric Modulator (PAM) of the Metabotropic Glutamate Receptor 4 (mGluR4)

Author

Craig W. Lindsley, Richard Williams, Kari A. Johnson, Colleen M. Niswender, P. Jeffrey Conn, Corey R. Hopkins, Patrick R. Gentry, and Charles David Weaver

Subjects
Allosteric modulator, Cyclohexanecarboxylic Acids, Clinical Biochemistry, Allosteric regulation, Pharmaceutical Science, Receptors, Metabotropic Glutamate, Biochemistry, Chemical synthesis, Article, Structure-Activity Relationship, Allosteric Regulation, In vivo, Drug Discovery, Structure–activity relationship, Animals, Anilides, Molecular Biology, Chemistry, Metabotropic glutamate receptor 4, Organic Chemistry, Parkinson Disease, Ligand (biochemistry), Rats, Disease Models, Animal, Metabotropic receptor, Biophysics, Molecular Medicine, Allosteric Site
Abstract

This Letter describes the synthesis and SAR of the novel positive allosteric modulator, VU0155041, a compound that has shown in vivo efficacy in rodent models of Parkinson's disease. The synthesis takes advantage of an iterative parallel synthesis approach to rapidly synthesize and evaluate a number of analogs of VU0155041.

Published
2009

34. P2‐207: Discovery of a highly M5‐preferring muscarinic acetylcholine receptor allosteric potentiator

Author

Colleen M. Niswender, P. Jeffrey Conn, C. David Weaver, Joy E. Marlo, Craig W. Lindsley, Patrick R. Gentry, and Thomas M. Bridges

Subjects
Epidemiology, Chemistry, Health Policy, Muscarinic acetylcholine receptor M3, Muscarinic acetylcholine receptor M2, Muscarinic acetylcholine receptor M1, Pharmacology, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Nicotinic agonist, Developmental Neuroscience, Muscarinic acetylcholine receptor, Muscarinic acetylcholine receptor M5, Muscarinic acetylcholine receptor M4, Neurology (clinical), Geriatrics and Gerontology, Acetylcholine receptor
Published
2009

35. P2.105 The development of positive allosteric modulators of mGluR4 for the treatment of Parkinson's disease

Author

S. Zhou, Satyawan Jadhav, Corey R. Hopkins, Rocco D. Gogliotti, Kari A. Johnson, C.K. Jones, Craig W. Lindsley, P.J. Conn, Darren W. Engers, Charles David Weaver, Usha N. Menon, Richard A Williams, Colleen M. Niswender, Analisa D. Thompson, Y.-Y. Cheung, James M. Salovich, Patrick R. Gentry, Emily Days, and Rocio Zamorano

Subjects
Parkinson's disease, Neurology, business.industry, Allosteric regulation, Medicine, Neurology (clinical), Geriatrics and Gerontology, business, medicine.disease, Neuroscience
Published
2009

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