Your search keyword '"Cécile Béguin"' showing total 24 results

1. Selective κ opioid antagonists nor-BNI, GNTI and JDTic have low affinities for non-opioid receptors and transporters.

Author

Thomas A Munro, Xi-Ping Huang, Carmela Inglese, Maria Grazia Perrone, Ashlee Van't Veer, F Ivy Carroll, Cécile Béguin, William A Carlezon, Nicola A Colabufo, Bruce M Cohen, and Bryan L Roth

Subjects

Medicine, Science

Abstract

Nor-BNI, GNTI and JDTic induce selective κ opioid antagonism that is delayed and extremely prolonged, but some other effects are of rapid onset and brief duration. The transient effects of these compounds differ, suggesting that some of them may be mediated by other targets.In binding assays, the three antagonists showed no detectable affinity (K(i)≥10 µM) for most non-opioid receptors and transporters (26 of 43 tested). There was no non-opioid target for which all three compounds shared detectable affinity, or for which any two shared sub-micromolar affinity. All three compounds showed low nanomolar affinity for κ opioid receptors, with moderate selectivity over μ and δ (3 to 44-fold). Nor-BNI bound weakly to the α(2C)-adrenoceptor (K(i) = 630 nM). GNTI enhanced calcium mobilization by noradrenaline at the α(1A)-adrenoceptor (EC₅₀ = 41 nM), but did not activate the receptor, displace radioligands, or enhance PI hydrolysis. This suggests that it is a functionally-selective allosteric enhancer. GNTI was also a weak M₁ receptor antagonist (K(B) = 3.7 µM). JDTic bound to the noradrenaline transporter (K(i) = 54 nM), but only weakly inhibited transport (IC₅₀ = 1.1 µM). JDTic also bound to the opioid-like receptor NOP (K(i) = 12 nM), but gave little antagonism even at 30 µM. All three compounds exhibited rapid permeation and active efflux across Caco-2 cell monolayers.Across 43 non-opioid CNS targets, only GNTI exhibited a potent functional effect (allosteric enhancement of α(1A)-adrenoceptors). This may contribute to GNTI's severe transient effects. Plasma concentrations of nor-BNI and GNTI may be high enough to affect some peripheral non-opioid targets. Nonetheless, κ opioid antagonism persists for weeks or months after these transient effects dissipate. With an adequate pre-administration interval, our results therefore strengthen the evidence that nor-BNI, GNTI and JDTic are highly selective κ opioid antagonists.

Published

2013

2. 8-epi-Salvinorin B: crystal structure and affinity at the κ opioid receptor

Author

Thomas A. Munro, Katharine K. Duncan, Richard J. Staples, Wei Xu, Lee-Yuan Liu-Chen, Cécile Béguin, William A. Carlezon Jr., and Bruce M. Cohen

Subjects

Science, Organic chemistry, QD241-441

Abstract

There have been many reports of epimerization of salvinorins at C-8 under basic conditions, but little evidence has been presented to establish the structure of these compounds. We report here the first crystal structure of an 8-epi-salvinorin or derivative: the title compound, 2b. The lactone adopts a boat conformation with the furan equatorial. Several lines of evidence suggest that epimerization proceeds via enolization of the lactone rather than a previously proposed indirect mechanism. Consistent with the general trend in related compounds, the title compound showed lower affinity at the kappa opioid receptor than the natural epimer salvinorin B (2a). The related 8-epi-acid 4b showed no affinity.

Published

2007

3. Effects of the anticonvulsant lacosamide compared to valproate and lamotrigine on cocaine-enhanced reward in rats

Author

Cécile Béguin, William A. Carlezon, Thomas Stöhr, David N. Potter, and Bruce M. Cohen

Subjects

Male, Reinforcement Schedule, Lacosamide, medicine.medical_treatment, Stimulation, Pharmacology, Lamotrigine, Rats, Sprague-Dawley, Self Stimulation, Cocaine, Reward, Acetamides, medicine, Animals, Medial forebrain bundle, Molecular Biology, Valproic Acid, Triazines, General Neuroscience, Rats, Treatment Outcome, Anticonvulsant, Mood, Anticonvulsants, Brain stimulation reward, Neurology (clinical), Psychology, Developmental Biology, medicine.drug

Abstract

Some drugs developed as anticonvulsants (notably, valproate and lamotrigine) have therapeutic effects in bipolar and related disorders. Lacosamide, a recently approved anticonvulsant, has unique effects on sodium channels that may play a role in producing the mood-stabilizing effects of anticonvulsant drugs. We tested whether lacosamide would have effects similar to or different from valproate and lamotrigine in a model of reward and elevated mood. The intracranial self-stimulation (ICSS) test is sensitive to the function of brain reward systems. Changes in ICSS may model aspects of disorders characterized by abnormalities of reward and motivation. Cocaine elevates mood, and reduction of cocaine-induced facilitation of ICSS has been used to predict antimanic-like or mood stabilizing effects of drugs. We tested lacosamide, lamotrigine, and valproate in the rat ICSS test alone or in the presence of cocaine. A high dose of lacosamide (30 mg/kg) significantly elevated ICSS thresholds, indicating that it reduced the rewarding impact of medial forebrain bundle stimulation. Lower doses (3-10 mg/kg) did not alter ICSS, but blocked the cocaine-induced lowering of ICSS thresholds. The highest doses of valproate (300 mg/kg) and lamotrigine (30 mg/kg) also elevated ICSS thresholds, and only these high doses significantly lowered cocaine-induced effects. Of the drugs tested, only lacosamide significantly attenuated the reward-facilitating effects of cocaine at doses that had no effects on ICSS response in the absence of cocaine. Abnormalities of mood and reward are common in psychiatric disorders, and these results suggest that lacosamide deserves further study in models of these disorders.

Published

2012

4. Salvinorin A and derivatives: Protection from metabolism does not prolong short-term, whole-brain residence

Author

Thomas A. Munro, Cécile Béguin, Jacob M. Hooker, David Alexoff, Colleen Shea, Youwen Xu, and Bruce M. Cohen

Subjects

Male, Absorption (skin), Pharmacology, Article, Diterpenes, Clerodane, Rats, Sprague-Dawley, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Pharmacokinetics, Animals, Potency, Carbon Radioisotopes, Chemistry, Brain, Metabolism, Papio anubis, Blood proteins, Salvinorin A, Rats, Kinetics, Salvinorin B ethoxymethyl ether, Positron-Emission Tomography, Injections, Intravenous, Female, Efflux, Diterpenes, Injections, Intraperitoneal, Central Nervous System Agents

Abstract

Salvinorin A (SA) is a potent kappa opioid agonist with a brief duration of action. Consistent with this, our previous positron emission tomography (PET) studies of carbon-11 labeled SA showed that brain levels decrease rapidly after intravenous administration. SA is rapidly metabolized, giving the much less potent salvinorin B (SB), which is presumed to be responsible in part for SA's brief duration of action. To test this, we labeled the metabolically stable methyl ester of SA and SB with carbon-11 and compared their pharmacokinetics by PET imaging after intravenous administration to baboons. Labeling of salvinorin B ethoxymethyl ether (EOM-SB), a derivative with greater potency and resistance to metabolism, provided an additional test of the role of metabolism in brain efflux. Plasma analysis confirmed that SB and EOM-SB exhibited greater metabolic stability than SA. However, the three compounds exhibited very similar pharmacokinetics in brain, entering and exiting rapidly. This suggests that metabolism is not solely responsible for the brief brain residence time of SA. We determined that whole-brain concentrations of EOM-SB declined more slowly than SA after intraperitoneal administration in rodents. This is likely due to a combination in EOM-SB's increased metabolic stability and its decreased plasma protein affinity. Our results suggest that protecting salvinorin A derivatives from metabolism will prolong duration of action, but only when administered by routes giving slow absorption.

Published

2009

5. Modification of the furan ring of salvinorin A: Identification of a selective partial agonist at the kappa opioid receptor

Author

William A. Carlezon, Cécile Béguin, Bruce M. Cohen, Thomas A. Munro, Lee-Yuan Liu-Chen, Wei Xu, Katharine K. Duncan, and Douglas M. Ho

Subjects

Agonist, medicine.drug_class, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Partial agonist, κ-opioid receptor, Article, Diterpenes, Clerodane, Structure-Activity Relationship, chemistry.chemical_compound, 5'-Guanidinonaltrindole, Furan, Drug Discovery, medicine, Furans, Molecular Biology, Salvinorin, Receptors, Opioid, kappa, Organic Chemistry, Salvinorin A, chemistry, Opioid, Molecular Medicine, medicine.drug

Abstract

In an effort to find novel agents which selectively target the kappa opioid receptor (KOPR), we modified the furan ring of the highly potent and selective KOPR agonist salvinorin A. Introduction of small substituents at C-16 was well tolerated. 12-epi-Salvinorin A, synthesized in four steps from salvinorin A, was a selective partial agonist at the KOPR. No clear SAR patterns were observed for C-13 aryl ketones. Introducing a hydroxymethylene group between C-12 and the furan ring was tolerated. Small C-13 esters and ethers gave weak KOPR agonists, while all C-13 amides were inactive. Finally, substitution of oxadiazoles for the furan ring abolished affinity for the KOPR. None of the compounds displayed any KOPR antagonism or any affinity for mu or delta opioid receptors.

Published

2009

6. Standard protecting groups create potent and selective κ opioids: Salvinorin B alkoxymethyl ethers

Author

Katharine K. Duncan, Bruce M. Cohen, Yulin Wang, Thomas A. Munro, Wei Xu, Lee-Yuan Liu-Chen, Cécile Béguin, and William A. Carlezon

Subjects

Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Ether, Alkylation, Methylation, Biochemistry, Chemical synthesis, Article, Diterpenes, Clerodane, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, Structure–activity relationship, Protecting group, Molecular Biology, Molecular Structure, Receptors, Opioid, kappa, Organic Chemistry, Acetal, Salvinorin A, chemistry, Alcohols, Alkoxy group, Molecular Medicine, Diterpenes, Ethers

Abstract

Protection of salvinorin B as standard alkoxyalkyl ethers yielded highly potent kappa opioid receptor agonists. Ethoxymethyl ether 6 is among the most potent and selective kappa agonists reported to date. Fluoroethoxymethyl ether 11 is the first potent, selective fluorinated kappa ligand, with potential use in MRI and PET studies. Further enlargement of the alkoxy group, alkylation of the acetal carbon, or heteroatom substitution all reduced activity. These protecting groups may prove useful in related work not only by enabling the use of harsher synthetic conditions, but potentially by optimizing the potency of the products.

Published

2008

7. N-Methylacetamide Analog of Salvinorin A: A Highly Potent and Selective κ-Opioid Receptor Agonist with Oral Efficacy

Author

Bryan L. Roth, David N. Potter, Tracie A. Paine, Bruce M. Cohen, Cécile Béguin, Loren Berry, Michele R. Richards, William A. Carlezon, Jennifer A. DiNieri, Zhiyang Zhao, Wei Xu, Lee-Yuan Liu-Chen, and Thomas A. Munro

Subjects

Male, Agonist, medicine.medical_specialty, Pyrrolidines, medicine.drug_class, Benzeneacetamides, Administration, Oral, Stimulation, Pharmacology, Diterpenes, Clerodane, Receptors, G-Protein-Coupled, Rats, Sprague-Dawley, Radioligand Assay, chemistry.chemical_compound, Oral administration, In vivo, Internal medicine, Acetamides, medicine, Animals, Humans, Potency, Salvia, Receptor, Psychotropic Drugs, Behavior, Animal, Mood Disorders, Receptors, Opioid, kappa, Membrane Transport Proteins, Salvinorin A, Rats, Analgesics, Opioid, Treatment Outcome, Endocrinology, Opioid, chemistry, Microsomes, Liver, Molecular Medicine, Diterpenes, medicine.drug

Abstract

Several preclinical studies indicate that selective kappa-opioid receptor (KOR) antagonists have antidepressant-like effects, whereas KOR agonists have opposite effects, suggesting that each might be useful in the treatment of mood abnormalities. Salvinorin A (salvA) is a valuable KOR agonist for further study due to its high potency and receptor selectivity. However, it has short lasting effects in vivo and limited oral bioavailability, probably due to acetate metabolism. We compared the in vitro receptor binding selectivity of salvA and four analogs containing an ethyl ether (EE), isopropylamine (IPA), N-methylacetamide (NMA), or N-methylpropionamide (NMP) at C-2. All compounds showed high binding affinity for the KOR (K(i) = 0.11-6.3 nM), although only salvA, EE, and NMA exhibited KOR selectivity. In a liver microsomal assay, salvA was least stable, whereas NMA and IPA displayed slower metabolic transformations. Intraperitoneal (i.p.) administration of salvA, NMA, and NMP dose-dependently elevated brain reward thresholds in the intracranial self-administration (ICSS) test, consistent with prodepressive-like KOR agonist effects. NMA and NMP were equipotent to salvA but displayed longer lasting effects (6- and 10-fold, respectively). A dose of salvA with prominent effects in the ICSS test after i.p. administration (2.0 mg/kg) was inactive after oral administration, whereas the same oral dose of NMA elevated ICSS thresholds. These studies suggest that, although salvA and NMA are similar in potency and selectivity as KOR agonists in vitro, NMA has improved stability and longer lasting actions that might make it more useful for studies of KOR agonist effects in animals and humans.

Published

2007

8. Synthesis and in vitro pharmacological studies of C(4) modified salvinorin A analogues

Author

Yulin Wang, Yong Chen, Zhongze Ma, Cécile Béguin, Leelakrishna Kondaveti, Bruce M. Cohen, Lee-Yuan Liu-Chen, William A. Carlezon, Minsheng He, Jian-Guo Li, and David Y.W. Lee

Subjects

Agonist, Stereochemistry, medicine.drug_class, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Biochemistry, Chemical synthesis, Diterpenes, Clerodane, Inhibitory Concentration 50, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, medicine, Humans, Structure–activity relationship, Receptor, Molecular Biology, chemistry.chemical_classification, Receptors, Opioid, kappa, Organic Chemistry, Salvinorin A, Terpenoid, In vitro, Analgesics, Opioid, chemistry, Guanosine 5'-O-(3-Thiotriphosphate), Molecular Medicine, Diterpenes, Lactone

Abstract

Salvinorin A is the most potent naturally occurring opioid agonist with a high selectivity and affinity for kappa-opioid receptor. To explore its structure-activity relationships, modifications at the C(4) position have been studied and a series of salvinorin A derivatives were prepared. These C(4)-modified salvinorin A analogues were screened for binding and functional activities at the human kappa-opioid receptor and several potent new agonists have been identified.

Published

2005

9. Synthesis and in vitro pharmacological studies of new C(2) modified salvinorin A analogues

Author

Cécile Béguin, Vishnu Vardhan R. Karnati, Lee-Yuan Liu-Chen, Minsheng He, Yong Chen, Zhongze Ma, William A. Carlezon, Bruce M. Cohen, David Y.W. Lee, Leelakrishna Kondaveti, and Yulin Wang

Subjects

Agonist, medicine.drug_class, Stereochemistry, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, Biochemistry, Chemical synthesis, Diterpenes, Clerodane, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, medicine, Humans, Structure–activity relationship, Molecular Biology, chemistry.chemical_classification, Salvinorin, Receptors, Opioid, kappa, Organic Chemistry, Salvinorin A, Terpenoid, chemistry, Opioid, Molecular Medicine, Diterpenes, Lactone, medicine.drug

Abstract

Salvinorin A is the most potent naturally occurring opioid agonist yet discovered with high selectivity and affinity for κ-opioid receptor. To explore its structure and activity relationships, a series of salvinorin A derivatives modified at the C(2) position were prepared and studied. These salvinorin A derivatives were screened for binding and functional activities at the human κ-opioid receptor. Compound 4, containing a methoxymethyl group at the 2-position, was a full κ-agonist with an EC50 value at 0.6 nM, which is about 7 times more potent than salvinorin A.

Published

2005

10. Synthesis and in vitro pharmacological evaluation of salvinorin A analogues modified at C(2)

Author

David Y.W. Lee, Cécile Béguin, Yulin Wang, Bruce M. Cohen, Michele R. Richards, William A. Carlezon, Lee-Yuan Liu-Chen, Zhongze Ma, and Yong Chen

Subjects

Agonist, medicine.drug_class, Stereochemistry, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, CHO Cells, Biochemistry, κ-opioid receptor, Chemical synthesis, Partial agonist, Diterpenes, Clerodane, chemistry.chemical_compound, Cricetinae, Drug Discovery, medicine, Animals, Structure–activity relationship, Molecular Biology, Salvinorin, Organic Chemistry, Salvinorin A, Terpenoid, chemistry, Molecular Medicine, Diterpenes

Abstract

Salvinorin A is the only known non-nitrogenous and specific kappa-opioid agonist. A series of salvinorin A derivatives were prepared and tested for in vitro activity at the kappa-opioid receptor. Unsubstituted carbamate 9 was a potent kappa-agonist (EC(50) = 6.2 nM) and should be more stable than salvinorin A toward metabolic transformations. Compound 10, containing an N-methyl carbamate at C(2), showed partial agonist activity with 81% efficacy when compared with the full agonist U50,488H. No antagonist ligands were observed.

Published

2005

11. A quantitative structure-activity relationship study for α-substituted acetamido-N-benzylacetamide derivatives — A novel anticonvulsant drug class

Author

Albert Y. Jin, James P. Stables, Cécile Béguin, Donald F. Weaver, Shridhar V. Andurkar, and Harold Kohn

Subjects

chemistry.chemical_classification, Quantitative structure–activity relationship, Ketone, Chemistry, Stereochemistry, Hydrogen bond, medicine.medical_treatment, Organic Chemistry, Substituent, General Chemistry, Wiener index, Catalysis, Partial charge, chemistry.chemical_compound, Anticonvulsant, medicine, Partition (number theory)

Abstract

A library of 35 benzylacetamide derivatives was evaluated for anticonvulsant activity as reflected in the ED50 (mg/kg) required to suppress seizure activity in the maximal electroshock seizure (MES) test. Using the method of partial least-squares regression in conjunction with cross-validation, the influence of 31 topological, electronic, physico chemical, and structural properties on anticonvulsant activity was investigated. A QSAR model of the logED50 in the MES test was established (R2adj = 0.77) as a function of the following seven properties: the Wiener index on distance code (Wmean), the mean information index on atomic composition (rIac), the partial charge at the C-terminal carbonyl carbon (qCC), the sum of partial charges in the α substituent (qαtotal), the number of hydrogen bond donors and acceptors in the α substituent (Hdα and Haα), and the calculated value of the squared n-octanol/water partition coefficient. Based on this model, two new amido ketone compounds — (R,S)-2-acetamido-5-phenyl-3-pentanone and cis/trans-(R,S)-2-acetamido-5-phenyl-4-penten-3-one — were synthesized and shown to have significant anticonvulsant activity in the MES test.Key words: QSAR, anticonvulsant, benzylacetamide, functionalized amino acid, amido ketones.

Published

2005

12. N-Substituted amino acid N′-benzylamides: synthesis, anticonvulsant, and metabolic activities

Author

Robert D. Voyksner, Cécile Béguin, Arnaud LeTiran, Harold Kohn, and James P. Stables

Subjects

Stereochemistry, medicine.medical_treatment, Clinical Biochemistry, Substituent, Pharmaceutical Science, Biochemistry, Chemical synthesis, Structure-Activity Relationship, chemistry.chemical_compound, In vivo, Benzyl Compounds, Drug Discovery, medicine, Animals, Amino Acids, Molecular Biology, chemistry.chemical_classification, Organic Chemistry, Stereoisomerism, Metabolism, Amides, In vitro, Rats, Amino acid, Anticonvulsant, chemistry, Molecular Medicine, Anticonvulsants, Amine gas treating

Abstract

Amino acid amides (AAA) were prepared and evaluated in seizure models. The AAA displayed moderate-to-excellent activity in the maximal electroshock seizure (MES) test and were devoid of activity in the subcutaneous Metrazol-induced (scMet) seizure test. The AAA anticonvulsant activity was neither strongly influenced by the C(2) substituent nor by the degree of terminal amine substitution. An in vitro metabolism study suggested that the structure-activity relationship pattern was due, in part, to metabolic processes that occurred at the N-terminal amine unit.

Published

2004

13. Functionalized amido ketones: new anticonvulsant agents

Author

Donald F. Weaver, Albert Y. Jin, Shridhar V. Andurkar, Cécile Béguin, Harold Kohn, and James P. Stables

Subjects

Male, medicine.drug_class, Stereochemistry, medicine.medical_treatment, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Carboxamide, Biochemistry, Chemical synthesis, Aminoketone, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Seizures, Amide, Drug Discovery, medicine, Animals, Amino Acids, Molecular Biology, chemistry.chemical_classification, Electroshock, Organic Chemistry, Ketones, Amides, Rats, Amino acid, Anticonvulsant Agent, Anticonvulsant, chemistry, Models, Animal, Molecular Medicine, Anticonvulsants, biological phenomena, cell phenomena, and immunity, Enone

Abstract

We have reported that functionalized amino acids (FAA) are potent anticonvulsants. Replacing the N-terminal amide group in FAA with phenethyl, styryl, and phenylethynyl units provided a series of functionalized amido ketones (FAK). We show that select FAK exhibit significant anticonvulsant activities thereby providing information about the structural requirements for FAA and FAK bioactivity.

Published

2003

14. Duration of Action of a Broad Range of Selective κ-Opioid Receptor Antagonists Is Positively Correlated with c-Jun N-Terminal Kinase-1 Activation

Author

Charles H. Mitch, Erica J. Melief, Mayumi Miyatake, Sarah Grimwood, Linda M. Rorick-Kehn, Bruce M. Cohen, William A. Carlezon, Cécile Béguin, F. Ivy Carroll, and Charles Chavkin

Subjects

Pharmacology, Trifluoromethyl, medicine.drug_class, Stereochemistry, Receptors, Opioid, kappa, c-jun, Antagonist, (+)-Naloxone, Articles, JDTic, Cell Line, Enzyme Activation, Isoenzymes, Mice, Inbred C57BL, chemistry.chemical_compound, Mice, chemistry, Opioid receptor, medicine, Molecular Medicine, Animals, Humans, Mitogen-Activated Protein Kinase 8, Benzamide, Receptor

Abstract

The κ-opioid receptor is a widely expressed G-protein-coupled receptor that has been implicated in biological responses to pain, stress, anxiety, and depression, and its potential as a therapeutic target in these syndromes is becoming increasingly apparent. However, the prototypical selective κ-opioid antagonists have very long durations of action that have been attributed to c-Jun N-terminal kinase (JNK) 1 activation in vivo. To test generality of this proposed noncompetitive mechanism, we used C57BL/6 wild type mice to determine the durations of antagonist action of novel κ-opioid receptor ligands and examined their efficacies for JNK1 activation compared with conventional competitive antagonists. Of the 12 compounds tested, 5 had long durations of action that positively correlated with JNK activation: RTI-5989-97 [(3S)-7-hydroxy-N-[(1S)-1-[(3R,4R)-4-(3-hydroxyphenyl)-3,4-dimethyl-1-piperidinyl]methyl}-(2-methylpropyl]-2-methyl-1,2,3,4-tetrahydro-3-isoquinolinecarboxamide], RTI-5989-194 [(3R)-7-hydroxy-N-[(1S)-1-[(3R,4R)-4-(3-hydroxyphenyl)-3,4-dimethyl-1-piperidinyl]methyl}-(2-methylbutyl]-1,2,3,4-tetrahydro-3-isoquinolinecarboxamide], RTI-5989-241 [(3R)-7-hydroxy-N-[(1S)-1-{[(3R,4R)-4-(3-methoxyphenyl)-3,4-dimethyl-1-piperidinyl]methyl}-2-methylpropyl]-1,2,3,4-tetrahydroisoquinoline-3-carboxamide)], nor-binaltorphimine (nor-BNI); and (3R)-7-hydroxy-N-((1S)-1-{[(3R,4R)-4-(3-hydroxyphenyl)-3,4-dimethyl-1-piperidinyl]methyl}-2-methylpropyl)-1,2,3,4-tetrahydro-3-isoquinolinecarboxamide (JDTic). Seven had short durations of action and did not increase phospho-JNK-ir: RTI-5989-212[(3R)-N-[(1S)-1-[(3R,4R)-4-(3-hydroxyphenyl)-3,4-dimethyl-1-piperidinyl]methyl}-(2-methylpropyl]-7-methoxy-1,2,3,4-tetrahydroisoquinoline-3-carboxamide], RTI-5989-240 [(3R)-7-hydroxy-N-[(1S)-1-[(3R,4R)-4-(3-hydroxyphenyl)-3,4-dimethylpiperidin-1-yl]methyl}-(2-methylpropyl]-3-methyl-1,2,3,4-tetrahydroisoquinoline-3-carboxamide], JSPA0658 [(S)-3-fluoro-4-(4-((2-(3,5-dimethylphenyl)pyrrolidin-1-yl)methyl)phenoxy)benzamide], JSPA071B [(S)-3-fluoro-4-(4-((2-(3,5-bis(trifluoromethyl)phenyl)pyrrolidin-1-yl)methyl)phenoxy)benzamide]. PF-4455242 [2-methyl-N-((2′-(pyrrolidin-1-ylsulfonyl)biphenyl-4-yl)methyl)propan-1-amine], PF-4455242 [2-methyl-N-((2′-(pyrrolidin-1-ylsulfonyl)biphenyl-4-yl)methyl)propan-1-amine], FP3FBZ [(S)-3-fluoro-4-(4-((2-(3-fluorophenyl)pyrrolidin-1-yl)methyl)phenoxy)benzamide], and naloxone. After long-acting antagonist treatment, pJNK-ir did not increase in mice lacking the κ-opioid receptor; increased pJNK-ir returned to baseline by 48 h after treatment; and a second challenge with nor-BNI 72 h after the first did not increase pJNK-ir. Long-lasting antagonism and increased phospho-JNK-ir were not seen in animals lacking the JNK1 isoform. These results support the hypothesis that the duration of action of small molecule κ-opioid receptor antagonists in vivo is determined by their efficacy in activating JNK1 and that persistent inactivation of the κ-receptor does not require sustained JNK activation.

Published

2011

15. Differential signaling properties at the kappa opioid receptor of 12-epi-salvinorin A and its analogues

Author

John M. Streicher, William A. Carlezon, Bruce M. Cohen, Lee-Yuan Liu-Chen, Laura M. Bohn, Justin S. Potuzak, Chad E. Groer, Cécile Béguin, and Wei Xu

Subjects

Agonist, medicine.drug_class, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, Pharmacology, Biochemistry, κ-opioid receptor, Partial agonist, Article, Diterpenes, Clerodane, chemistry.chemical_compound, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, medicine, Humans, Receptor, Molecular Biology, Dose-Response Relationship, Drug, Salvinorin, Receptors, Opioid, kappa, Organic Chemistry, Ligand (biochemistry), Salvinorin A, chemistry, Opioid, Molecular Medicine, medicine.drug, Signal Transduction

Abstract

The kappa opioid receptor (KOPR) has been identified as a potential drug target to prevent or alter the course of mood, anxiety and addictive disorders or reduce response to stress. In a search for highly potent and selective KOPR partial agonists as pharmacological tools, we have modified 12-epi-salvinorin A, a compound which we have previously observed to be a KOPR partial agonist. Five analogues of 12-epi-salvinorin A were synthesized and their effects on G protein activation as well as β-arrestin2 recruitment were evaluated. Only 12-epi-salvinorin A (1) partially activated signaling through G proteins, yet acted as a full agonist in the β-arrestin 2 DiscoveRx assay. Other salvinorin analogues tested in these functional assays were full agonists in both assays of KOPR activation. By comparison, the non-selective opioid ligand nalbuphine, known to be a partial agonist for G-protein activation, was also a partial agonist for the β-arrestin mediated signaling pathway activated through KOPR.

Published

2011

16. 6′‐Guanidinonaltrindole (6′‐GNTI) is a potent and functionally unique kappa opioid agonist that displays bias against beta‐arrestin recruitment and receptor internalization

Author

John M. Streicher, Chad E. Groer, Thomas A. Munro, Laura M. Bohn, Cécile Béguin, and Bruce M. Cohen

Subjects

chemistry.chemical_compound, Opioid Agonist, Chemistry, 6'-Guanidinonaltrindole, Genetics, Arrestin beta 2, Pharmacology, Molecular Biology, Biochemistry, Receptor internalization, Kappa, Biotechnology

Published

2011

17. Role of kappa-opioid receptors in the effects of salvinorin A and ketamine on attention in rats

Author

Bruce M. Cohen, Bryan L. Roth, Christina L. Nemeth, Tracie A. Paine, Joseph E. Rittiner, Cécile Béguin, William A. Carlezon, and F. Ivy Carroll

Subjects

Male, Visual perception, genetic structures, media_common.quotation_subject, κ-opioid receptor, behavioral disciplines and activities, Receptors, N-Methyl-D-Aspartate, Article, Diterpenes, Clerodane, Rats, Sprague-Dawley, chemistry.chemical_compound, Perception, medicine, Reaction Time, Animals, Ketamine, Attention, media_common, Pharmacology, Dose-Response Relationship, Drug, Receptors, Opioid, kappa, Cognition, medicine.disease, Salvinorin A, Rats, chemistry, Schizophrenia, NMDA receptor, sense organs, Psychology, Neuroscience, psychological phenomena and processes, medicine.drug

Abstract

Disruptions in perception and cognition are characteristic of psychiatric conditions such as schizophrenia. Studies of pharmacological agents that alter perception and cognition in humans might provide a better understanding of the brain substrates of these complex processes. One way to study these states in rodents is with tests that require attention and visual perception for correct performance.We examined the effects of two drugs that cause disruptions in perception and cognition in humans-the kappa-opioid receptor (KOR) agonist salvinorin A (salvA; 0.125-4.0 mg/kg) and the non-competitive NMDA receptor antagonist ketamine (0.63-20 mg/kg)-on behavior in rats using the 5-choice serial reaction time task (5CSRTT), a food-motivated test that quantifies attention. We also compared the binding profiles of salvA and ketamine at KORs and NMDA receptors.SalvA and ketamine produced the same pattern of disruptive effects in the 5CSRTT, characterized by increases in signs often associated with reduced motivation (omission errors) and deficits in processing (elevated latencies to respond correctly). Sessions in which rats were fed before testing suggest that reduced motivation produces a subtly different pattern of behavior. Pretreatment with the KOR antagonist JDTic (10 mg/kg) blocked all salvA effects and some ketamine effects. Binding and function studies revealed that ketamine is a full agonist at KORs, although not as potent or selective as salvA.SalvA and ketamine have previously under-appreciated similarities in their behavioral effects and pharmacological profiles. By implication, KORs might be involved in some of the cognitive abnormalities observed in psychiatric disorders such as schizophrenia.

Published

2010

18. Kappa-opioid ligands in the study and treatment of mood disorders

Author

William A. Carlezon, Allison T. Knoll, Cécile Béguin, and Bruce M. Cohen

Subjects

Bipolar Disorder, Pharmacology, Bioinformatics, Ligands, Partial agonist, Article, chemistry.chemical_compound, Drug Delivery Systems, Medicine, Animals, Humans, Pharmacology (medical), Bipolar disorder, Endogenous opioid, business.industry, Depression, Mood Disorders, Receptors, Opioid, kappa, JDTic, medicine.disease, Mood, chemistry, Mood disorders, Drug Design, Antidepressant, medicine.symptom, business, Mania

Abstract

The biological basis of mood is not understood. Most research on mood and affective states has focused on the roles of brain systems containing monoamines (e.g., dopamine, norepinephrine, serotonin). However, it is becoming clear that endogenous opioid systems in the brain may also be involved in the regulation of mood. In this review, we focus on the potential utility of kappa-opioid receptor (KOR) ligands in the study and treatment of psychiatric disorders. Research from our group and others suggests that KOR antagonists might be useful for depression, KOR agonists might be useful for mania, and KOR partial agonists might be useful for mood stabilization. Currently available KOR agents have some unfavorable properties that might be addressed through medicinal chemistry. The development of KOR-selective agents with improved drug-like characteristics would facilitate preclinical and clinical studies designed to evaluate the possibility that KORs are a feasible target for new medications.

Published

2009

19. Medicinal Chemistry of Kappa Opioid Receptor Antagonists

Author

Bruce M. Cohen and Cécile Béguin

Subjects

business.industry, medicine.drug_class, fungi, Pharmacology, JDTic, κ-opioid receptor, body regions, chemistry.chemical_compound, chemistry, Opioid receptor, Medicine, Structure–activity relationship, skin and connective tissue diseases, business, Norbinaltorphimine, Short duration, medicine.drug

Abstract

The kappa opioid receptor (KOR), a member of the opioid receptor family, was initially studied for its involvement in the mediation of pain. More recently, there has been growing interest in selective KOR agents for their potential effects on mood and reward. In particular, selective KOR antagonists may offer a novel approach to relieve symptoms of depression. In this chapter, we describe the structure–activity relationships (SAR) of nonpeptidic KOR antagonists. Specifically, we review the SAR of norbinaltorphimine (norBNI) and its structur ally simplified derivative GNTI. We present the SAR of JDTic and the recently developed MTHQ. The SAR patterns of norBNI have been extensively studied, but there have been relatively fewer studies on the SAR of JDTic and MTHQ. While the overall SAR trends of these structurally distinct agents differ, there appears to be a common requirement for KOR inhibition: the presence of a phenol unit and a basic nitrogen. In the second part of this chapter, we discuss the unusually long duration of action of the available KOR antagonists and make suggestions on pos sibilities for the design of additional KOR antagonists.

Published

2009

20. 8-epi-Salvinorin B: crystal structure and affinity at the kappa opioid receptor

Author

Richard J. Staples, Lee-Yuan Liu-Chen, Katharine K. Duncan, Thomas A. Munro, Wei Xu, Bruce M. Cohen, William A. Carlezon, and Cécile Béguin

Subjects

chemistry.chemical_classification, medicine.drug_class, Stereochemistry, Organic Chemistry, Cyclohexane conformation, Crystal structure, κ-opioid receptor, Full Research Paper, lcsh:QD241-441, chemistry.chemical_compound, chemistry, lcsh:Organic chemistry, Opioid receptor, Furan, medicine, Epimer, lcsh:Q, lcsh:Science, Derivative (chemistry), Lactone

Abstract

There have been many reports of epimerization of salvinorins at C-8 under basic conditions, but little evidence has been presented to establish the structure of these compounds. We report here the first crystal structure of an 8-epi-salvinorin or derivative: the title compound, 2b. The lactone adopts a boat conformation with the furan equatorial. Several lines of evidence suggest that epimerization proceeds via enolization of the lactone rather than a previously proposed indirect mechanism. Consistent with the general trend in related compounds, the title compound showed lower affinity at the kappa opioid receptor than the natural epimer salvinorin B (2a). The related 8-epi-acid 4b showed no affinity.

Published

2006

21. Depressive-like effects of the kappa-opioid receptor agonist salvinorin A on behavior and neurochemistry in rats

Author

David Y.W. Lee, Michael H. Baumann, Michele R. Richards, Jennifer A. DiNieri, Zhongze Ma, Cécile Béguin, Bruce M. Cohen, Mark S. Todtenkopf, William A. Carlezon, and Richard B. Rothman

Subjects

Agonist, Male, Serotonin, medicine.drug_class, Dopamine, Microdialysis, Stimulation, Dynorphin, Pharmacology, Motor Activity, Open field, Diterpenes, Clerodane, Rats, Sprague-Dawley, chemistry.chemical_compound, medicine, Animals, Swimming, Endogenous opioid, Brain Chemistry, Psychotropic Drugs, Behavior, Animal, Salvinorin, Receptors, Opioid, kappa, Salvinorin A, Rats, chemistry, Depression, Chemical, Molecular Medicine, Brain stimulation reward, Diterpenes, Psychology, Extracellular Space

Abstract

Endogenous opioids seem to play a critical role in the regulation of mood states. For example, there is accumulating evidence that stimulation of kappa-opioid receptors, upon which the endogenous opioid dynorphin acts, can produce depressive-like behaviors in laboratory animals. Here we examined whether systemic administration of salvinorin A (SalvA), a potent and highly selective kappa-opioid agonist, would produce depressive-like effects in the forced swim test (FST) and intracranial self-stimulation (ICSS) test, which are behavioral models often used to study depression in rats. We extracted, isolated, and purified SalvA from Salvia divinorum plant leaves and examined its effects on behavior in the FST and ICSS test across a range of doses (0.125-2.0 mg/kg) after systemic (intraperitoneal) administration. SalvA dose dependently increased immobility in the FST, an effect opposite to that of standard antidepressant drugs. Doses of SalvA that produced these effects in the FST did not affect locomotor activity in an open field. Furthermore, SalvA dose dependently elevated ICSS thresholds, an effect similar to that produced by treatments that cause depressive symptoms in humans. At a dose that caused the depressive-like effects in both the FST and ICSS assays, SalvA decreased extracellular concentrations of dopamine (DA) within the nucleus accumbens (NAc), a critical component of brain reward circuitry, without affecting extracellular concentrations of serotonin (5-HT). These data provide additional support for the hypothesis that stimulation of brain kappa-opioid receptors triggers depressive-like signs in rats and raise the possibility that decreases in extracellular concentrations of DA within the NAc contribute to these effects.

Published

2005

22. Selective κ Opioid Antagonists nor-BNI, GNTI and JDTic Have Low Affinities for Non-Opioid Receptors and Transporters

Author

William A. Carlezon, Xi Ping Huang, Nicola Antonio Colabufo, Ashlee Van't Veer, Carmela Inglese, Bryan L. Roth, Cécile Béguin, Maria Grazia Perrone, Bruce M. Cohen, F. Ivy Carroll, and Thomas A. Munro

Subjects

Narcotic Antagonists, NOP, Receptors, Opioid, mu, lcsh:Medicine, Pharmacology, Biochemistry, Guanidines, Ion Channels, Naltrexone, Transmembrane Transport Proteins, Norepinephrine, chemistry.chemical_compound, Piperidines, Receptors, Opioid, delta, Tetrahydroisoquinolines, Molecular Cell Biology, Membrane Receptor Signaling, lcsh:Science, Receptor, Multidisciplinary, Neurotransmitter Receptor Signaling, Muscarinic acetylcholine receptor M1, JDTic, Morphinans, Cytochemistry, Medicine, Research Article, Signal Transduction, Protein Binding, medicine.drug, Drugs and Devices, Allosteric regulation, Signaling Pathways, Neuropharmacology, Allosteric Regulation, medicine, Humans, Biology, Norepinephrine Plasma Membrane Transport Proteins, Receptors, Opioid, kappa, lcsh:R, Cell Membrane, Antagonist, Membrane Proteins, Proteins, Biological Transport, Receptors, Adrenergic, alpha, Transmembrane Proteins, Kinetics, chemistry, Opioid, Small Molecules, Acetylcholine Receptors, Cellular Neuroscience, Muscarinic Acetylcholine Receptors, lcsh:Q, Calcium, Caco-2 Cells, Adrenergic Signal Transduction, Neuroscience

Abstract

Background Nor-BNI, GNTI and JDTic induce selective κ opioid antagonism that is delayed and extremely prolonged, but some other effects are of rapid onset and brief duration. The transient effects of these compounds differ, suggesting that some of them may be mediated by other targets. Results In binding assays, the three antagonists showed no detectable affinity (K i≥10 µM) for most non-opioid receptors and transporters (26 of 43 tested). There was no non-opioid target for which all three compounds shared detectable affinity, or for which any two shared sub-micromolar affinity. All three compounds showed low nanomolar affinity for κ opioid receptors, with moderate selectivity over μ and δ (3 to 44-fold). Nor-BNI bound weakly to the α2C-adrenoceptor (K i = 630 nM). GNTI enhanced calcium mobilization by noradrenaline at the α1A-adrenoceptor (EC50 = 41 nM), but did not activate the receptor, displace radioligands, or enhance PI hydrolysis. This suggests that it is a functionally-selective allosteric enhancer. GNTI was also a weak M1 receptor antagonist (K B = 3.7 µM). JDTic bound to the noradrenaline transporter (K i = 54 nM), but only weakly inhibited transport (IC50 = 1.1 µM). JDTic also bound to the opioid-like receptor NOP (K i = 12 nM), but gave little antagonism even at 30 µM. All three compounds exhibited rapid permeation and active efflux across Caco-2 cell monolayers. Conclusions Across 43 non-opioid CNS targets, only GNTI exhibited a potent functional effect (allosteric enhancement of α1A-adrenoceptors). This may contribute to GNTI's severe transient effects. Plasma concentrations of nor-BNI and GNTI may be high enough to affect some peripheral non-opioid targets. Nonetheless, κ opioid antagonism persists for weeks or months after these transient effects dissipate. With an adequate pre-administration interval, our results therefore strengthen the evidence that nor-BNI, GNTI and JDTic are highly selective κ opioid antagonists.

Published

2013

23. Corrigendum to 'Synthesis and in vitro evaluation of salvinorin A analogues: Effect of configuration at C(2) and substitution at C(18)' [Bioorg. Med. Chem. Lett. 16 (2006) 4679–4685]

Author

Cécile Béguin, Jian-Guo Li, William A. Carlezon, Lee-Yuan Liu-Chen, Bruce M. Cohen, Michele R. Richards, Wei Xu, and Yulin Wang

Subjects

chemistry.chemical_compound, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Drug Discovery, Substitution (logic), Pharmaceutical Science, Molecular Medicine, Molecular Biology, Biochemistry, In vitro, Salvinorin A

Published

2008

24. Long-acting κ opioid antagonists nor-BNI, GNTI and JDTic: pharmacokinetics in mice and lipophilicity

Author

Ashlee Van't Veer, Cécile Béguin, F. Ivy Carroll, Bruce M. Cohen, Zhiyang Zhao, Thomas A. Munro, William A. Carlezon, and Loren Berry

Subjects

Male, Swine, medicine.drug_class, Narcotic Antagonists, Nor-BNI, 5’-GNTI, Norbinaltorphimine, Pharmacology, Guanidines, Permeability, Naltrexone, Mice, chemistry.chemical_compound, Piperidines, Pharmacokinetics, Desensitization (telecommunications), Opioid receptor, Tetrahydroisoquinolines, 5'-Guanidinonaltrindole, Lipophilicity, medicine, Animals, Pharmacology (medical), Chemistry, Receptors, Opioid, kappa, JNK1, Brain, Biological Transport, MAPK8, JDTic, Morphinans, Opioid, LLC-PK1 Cells, P-gp, 5’-guanidinonaltrindole, Hydrophobic and Hydrophilic Interactions, Injections, Intraperitoneal, Research Article, medicine.drug

Abstract

Background Nor-BNI, GNTI and JDTic induce κ opioid antagonism that is delayed by hours and can persist for months. Other effects are transient. It has been proposed that these drugs may be slowly absorbed or distributed, and may dissolve in cell membranes, thus slowing elimination and prolonging their effects. Recent evidence suggests, instead, that they induce prolonged desensitization of the κ opioid receptor. Methods To evaluate these hypotheses, we measured relevant physicochemical properties of nor-BNI, GNTI and JDTic, and the timecourse of brain and plasma concentrations in mice after intraperitoneal administration (using LC-MS-MS). Results In each case, plasma levels were maximal within 30 min and declined by >80% within four hours, correlating well with previously reported transient effects. A strong negative correlation was observed between plasma levels and the delayed, prolonged timecourse of κ antagonism. Brain levels of nor-BNI and JDTic peaked within 30 min, but while nor-BNI was largely eliminated within hours, JDTic declined gradually over a week. Brain uptake of GNTI was too low to measure accurately, and higher doses proved lethal. None of the drugs were highly lipophilic, showing high water solubility (> 45 mM) and low distribution into octanol (log D7.4 < 2). Brain homogenate binding was within the range of many shorter-acting drugs (>7% unbound). JDTic showed P-gp-mediated efflux; nor- BNI and GNTI did not, but their low unbound brain uptake suggests efflux by another mechanism. Conclusions The negative plasma concentration-effect relationship we observed is difficult to reconcile with simple competitive antagonism, but is consistent with desensitization. The very slow elimination of JDTic from brain is surprising given that it undergoes active efflux, has modest affinity for homogenate, and has a shorter duration of action than nor-BNI under these conditions. We propose that this persistence may result from entrapment in cellular compartments such as lysosomes.