Your search keyword '"Orexin Receptor Antagonists chemical synthesis"' showing total 15 results

1. Discovery, synthesis and SAR of 2-acyl-1-biarylmethyl pyrazolidines, dual orexin receptor antagonists designed as fast and short-acting sleeping drugs.

Author

Surivet JP, Kessler M, Vaillant C, Aissaoui H, Bezençon O, Busch L, Kiry M, Lüthi U, Marck N, Masse F, Peters JU, Sweatman C, Weigel A, and Kohl C

Subjects

Structure-Activity Relationship, Humans, Animals, Molecular Structure, Hypnotics and Sedatives pharmacology, Hypnotics and Sedatives chemical synthesis, Hypnotics and Sedatives chemistry, Hypnotics and Sedatives pharmacokinetics, Orexin Receptors metabolism, Rats, Dose-Response Relationship, Drug, Male, Orexin Receptor Antagonists pharmacology, Orexin Receptor Antagonists chemistry, Orexin Receptor Antagonists chemical synthesis, Pyrazoles chemistry, Pyrazoles pharmacology, Pyrazoles chemical synthesis, Drug Discovery

Abstract

Dual orexin receptor antagonists (DORAs) are approved for the treatment of sleep onset and/or sleep maintenance insomnia. In the present disclosure, we report the discovery of a new class of DORAs designed to treat sleep disorders requiring a fast onset and a short duration of action (<4 h). We used early human pharmacokinetic-pharmacodynamic (PK-PD) predictions and in vivo experiments to identify DORAs eliciting this specific hypnotic profile. A high-throughput screening campaign revealed hits based on a rarely precedented tricyclic pyrazolidine scaffold. After unsuccessful structure-activity-relationship (SAR) studies on this hit series, a scaffold hopping exercise, aimed at reducing the molecular complexity of the tricyclic scaffold, resulted in the discovery of the 2-acyl-1-biarylmethylpyrazolidine series. SAR studies on this achiral series gave rise to the lead compound DORA 42. In vitro and in vivo parameters of DORA 42, and its PK-PD simulation for human use are detailed., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

2. Structure-guided discovery of orexin receptor-binding PET ligands.

Author

Distler K, Maschauer S, Neu E, Hübner H, Einsiedel J, Prante O, and Gmeiner P

Subjects

Ligands, Humans, Structure-Activity Relationship, Molecular Structure, Radiopharmaceuticals chemistry, Radiopharmaceuticals chemical synthesis, Drug Discovery, Triazoles chemistry, Triazoles chemical synthesis, Triazoles pharmacology, Fluorine Radioisotopes chemistry, Orexin Receptor Antagonists chemistry, Orexin Receptor Antagonists chemical synthesis, Orexin Receptor Antagonists pharmacology, Orexin Receptors metabolism, Positron-Emission Tomography

Abstract

Molecular imaging using positron emission tomography (PET) can serve as a promising tool for visualizing biological targets in the brain. Insights into the expression pattern and the in vivo imaging of the G protein-coupled orexin receptors OX1R and OX2R will further our understanding of the orexin system and its role in various physiological and pathophysiological processes. Guided by crystal structures of our lead compound JH112 and the approved hypnotic drug suvorexant bound to OX1R and OX2R, respectively, we herein describe the design and synthesis of two novel radioligands, [ 18 F]KD23 and [ 18 F]KD10. Key to the success of our structural modifications was a bioisosteric replacement of the triazole moiety with a fluorophenyl group. The 19 F-substituted analog KD23 showed high affinity for the OX1R and selectivity over OX2R, while the high affinity ligand KD10 displayed similar K i values for both subtypes. Radiolabeling starting from the respective pinacol ester precursors resulted in excellent radiochemical yields of 93% and 88% for [ 18 F]KD23 and [ 18 F]KD10, respectively, within 20 min. The new compounds will be useful in PET studies aimed at subtype-selective imaging of orexin receptors in brain tissue., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published

2024

3. Discovery of attenuation effect of orexin 1 receptor to aversion of nalfurafine: Synthesis and evaluation of D-nor-nalfurafine derivatives and analyses of the three active conformations of nalfurafine.

Author

Nagumo Y, Katoh K, Iio K, Saitoh T, Kutsumura N, Yamamoto N, Ishikawa Y, Irukayama-Tomobe Y, Ogawa Y, Baba T, Tanimura R, Yanagisawa M, and Nagase H

Subjects

Animals, Avoidance Learning drug effects, Binding Sites, Mice, Mice, Knockout, Molecular Conformation, Molecular Docking Simulation, Morphinans metabolism, Morphinans pharmacology, Orexin Receptor Antagonists metabolism, Orexin Receptor Antagonists pharmacology, Orexin Receptors chemistry, Orexin Receptors genetics, Receptors, Opioid, kappa agonists, Receptors, Opioid, kappa metabolism, Spiro Compounds metabolism, Spiro Compounds pharmacology, Morphinans chemistry, Orexin Receptor Antagonists chemical synthesis, Orexin Receptors metabolism, Spiro Compounds chemistry

Abstract

The D-nor-nalfurafine derivatives, which were synthesized by contraction of the six-membered D-ring in nalfurafine (1), had no affinity for orexin 1 receptors (OX 1 Rs). The 17N-lone electron pair in 1 oriented toward the axial direction, while that of D-nor-derivatives was directed in the equatorial configuration. The axial lone electron pair can form a hydrogen bond with the 14-hydroxy group, which could push the 6-amide side chain toward the downward direction with respect to the C-ring. The resulting conformation would be an active conformation for binding with OX 1 R. The dual affinities of 1 for OX 1 R and κ opioid receptor (KOR) led us to elucidate the mechanism by which only 1 showed no aversion but U-50488H. Actually, 1 selectively induced severe aversion in OX 1 R knockout mice, but not in wild-type mice. These results well support that OX 1 R suppresses the aversion of 1. This is the elucidation of long period puzzle which 1 showed no aversion in KOR., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

4. Discovery of ORN0829, a potent dual orexin 1/2 receptor antagonist for the treatment of insomnia.

Author

Futamura A, Suzuki R, Tamura Y, Kawamoto H, Ohmichi M, Hino N, Tokumaru Y, Kirinuki S, Hiyoshi T, Aoki T, Kambe D, and Nozawa D

Subjects

Animals, Dogs, Dose-Response Relationship, Drug, Drug Design, Humans, Male, Molecular Structure, Orexin Receptor Antagonists pharmacokinetics, Orexins pharmacokinetics, Rats, Wistar, Sleep drug effects, Stereoisomerism, Structure-Activity Relationship, Orexin Receptor Antagonists chemical synthesis, Orexin Receptors metabolism, Orexins chemistry, Sleep Initiation and Maintenance Disorders drug therapy

Abstract

Here, we present the design, synthesis, and SAR of dual orexin 1 and 2 receptor antagonists, which were optimized by balancing the antagonistic activity for orexin receptors and lipophilicity. Based on the prototype compound 1, ring construction and the insertion of an additional heteroatom into the resulting ring led to the discovery of orexin 1 and 2 receptor antagonists, which were 3-benzoyl-1,3-oxazinane derivatives. Within these derivatives, (-)-3h enabled a high dual orexin receptor antagonistic activity and a low lipophilicity. Compound (-)-3h exhibited potent sleep-promoting effects at a po dose of 1 mg/kg in a rat polysomnogram study, and optimal PK properties with a rapid T max and short half-lives in rats and dogs were observed, indicating a predicted human half-life of 0.9-2.0 h. Thus, (-)-3h (ORN0829; investigation code name, TS-142) was selected as a viable candidate and is currently in clinical development for the treatment of insomnia., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

5. Preventing Morphine-Seeking Behavior through the Re-Engineering of Vincamine's Biological Activity.

Author

Norwood VM 4th, Brice-Tutt AC, Eans SO, Stacy HM, Shi G, Ratnayake R, Rocca JR, Abboud KA, Li C, Luesch H, McLaughlin JP, and Huigens RW 3rd

Subjects

Animals, Drug-Seeking Behavior physiology, Injections, Intraperitoneal, Injections, Intraventricular, Male, Mice, Mice, Inbred C57BL, Opioid-Related Disorders drug therapy, Opioid-Related Disorders metabolism, Orexin Receptor Antagonists administration & dosage, Orexin Receptor Antagonists chemical synthesis, Orexin Receptor Antagonists metabolism, Orexin Receptors metabolism, Protein Structure, Secondary, Vincamine metabolism, Chemical Engineering methods, Drug-Seeking Behavior drug effects, Morphine administration & dosage, Vincamine administration & dosage, Vincamine chemical synthesis

Abstract

Innovative discovery strategies are essential to address the ongoing opioid epidemic in the United States. Misuse of prescription and illegal opioids (e.g., morphine, heroin) has led to major problems with addiction and overdose. We used vincamine, an indole alkaloid, as a synthetic starting point for dramatic structural alterations of its complex, fused ring system to synthesize 80 diverse compounds with intricate molecular architectures. A select series of vincamine-derived compounds were screened for both agonistic and antagonistic activities against a panel of 168 G protein-coupled receptor (GPCR) drug targets. Although vincamine was without an effect, the novel compound 4 ( V2a ) demonstrated antagonistic activities against hypocretin (orexin) receptor 2. When advanced to animal studies, 4 ( V2a ) significantly prevented acute morphine-conditioned place preference (CPP) and stress-induced reinstatement of extinguished morphine-CPP in mouse models of opioid reward and relapse. These results demonstrate that the ring distortion of vincamine offers a promising way to explore new chemical space of relevance to opioid addiction.

Published

2020

6. Essential structure of orexin 1 receptor antagonist YNT-707, part V: Structure-activity relationship study of the substituents on the 17-amino group.

Author

Saitoh T, Seki K, Nakajima R, Yamamoto N, Kutsumura N, Nagumo Y, Irukayama-Tomobe Y, Ogawa Y, Ishikawa Y, Yanagisawa M, and Nagase H

Subjects

Amines chemistry, Humans, Kinetics, Morphinans metabolism, Orexin Receptor Antagonists chemical synthesis, Orexin Receptor Antagonists metabolism, Orexin Receptors metabolism, Structure-Activity Relationship, Sulfonamides metabolism, Morphinans chemistry, Orexin Receptor Antagonists chemistry, Orexin Receptors chemistry, Sulfonamides chemistry

Abstract

The morphinan-type orexin 1 receptor (OX 1 R) antagonists such as YNT-707 (2) and YNT-1310 (3) show potent and extremely high selective antagonistic activity against OX 1 R. In the course of our studies of the essential structure of 2, we identified new scaffolds by simplification of the morphinan skeleton. However, the new chemical entities carrying the D-ring removed scaffold showed insufficient activity. To improve the activity of these derivatives, we investigated the effect of substituents mainly focused on the 17-nitrogen group. The 17-N-substituted derivatives, as well as the cyclic derivatives, were synthesized and examined the OX 1 R antagonistic activity. The assay results showed the interesting relationship between the OX 1 R antagonistic activity and the substituents on the 17-nitrogen: the antagonistic activity was increased as the bulkiness of 17-substituents increased. Finally, the 17-N-Boc derivative 14a showed the most potent OX 1 R antagonistic activity (K i  = 14.8 nM)., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2020

7. Essential structure of orexin 1 receptor antagonist YNT-707, Part IV: The role of D-ring in 4,5-epoxymorphinan on the orexin 1 receptor antagonistic activity.

Author

Saitoh T, Seki K, Nakajima R, Yamamoto N, Kutsumura N, Nagumo Y, Irukayama-Tomobe Y, Ogawa Y, Ishikawa Y, Tanimura R, Yanagisawa M, and Nagase H

Subjects

Dose-Response Relationship, Drug, Humans, Molecular Structure, Morphinans chemical synthesis, Morphinans chemistry, Orexin Receptor Antagonists chemical synthesis, Orexin Receptor Antagonists chemistry, Structure-Activity Relationship, Sulfonamides chemical synthesis, Sulfonamides chemistry, Morphinans pharmacology, Orexin Receptor Antagonists pharmacology, Orexin Receptors metabolism, Sulfonamides pharmacology

Abstract

The orexin 1 receptor (OX 1 R) antagonists carrying a morphinan skeleton such as YNT-707 (2) and YNT-1310 (3) showed potent and extremely high selective antagonistic activity against OX 1 R. In the course of our study of the essential structure of YNT-707 for high binding affinity against OX 1 R, we prepared derivatives of 2 without the D- and 4,5-epoxy rings to clarify the roles of these structural determinants toward OX 1 R antagonistic activity. The D- and 4,5-epoxy rings played important roles for the active orientation of the 17-sulfonamide and 6-amide side chains. Finally, we identified the simple structure required for selective OX 1 R antagonistic activity in the complex morphinan skeleton, which is expected to be a useful scaffold for further design of OX 1 R ligands., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

8. Oxadiazole Derivatives as Dual Orexin Receptor Antagonists: Synthesis, Structure-Activity Relationships, and Sleep-Promoting Properties in Rats.

Author

Brotschi C, Roch C, Gatfield J, Treiber A, Williams JT, Sifferlen T, Heidmann B, Jenck F, Bolli MH, and Boss C

Subjects

Animals, Azepines pharmacology, Cytochrome P-450 CYP3A chemistry, Cytochrome P-450 CYP3A metabolism, Dogs, Half-Life, Humans, Inhibitory Concentration 50, Orexin Receptor Antagonists metabolism, Orexin Receptor Antagonists pharmacology, Orexin Receptors chemistry, Oxadiazoles metabolism, Oxadiazoles pharmacology, Rats, Sleep drug effects, Structure-Activity Relationship, Triazoles pharmacology, Orexin Receptor Antagonists chemical synthesis, Orexin Receptors metabolism, Oxadiazoles chemistry

Abstract

The orexin system plays an important role in the regulation of wakefulness. Suvorexant, a dual orexin receptor antagonist (DORA) is approved for the treatment of primary insomnia. Herein, we outline our optimization efforts toward a novel DORA. We started our investigation with rac-[3-(5-chloro-benzooxazol-2-ylamino)piperidin-1-yl]-(5-methyl-2-[1,2,3]triazol-2-ylphenyl)methanone (3), a structural hybrid of suvorexant and a piperidine-containing DORA. During the optimization, we resolved liabilities such as chemical instability, CYP3A4 inhibition, and low brain penetration potential. Furthermore, structural modification of the piperidine scaffold was essential to improve potency at the orexin 2 receptor. This work led to the identification of (5-methoxy-4-methyl-2-[1,2,3]triazol-2-ylphenyl)-{(S)-2-[5-(2-trifluoromethoxyphenyl)-[1,2,4]oxadiazol-3-yl]pyrrolidin-1-yl}methanone (51), a potent, brain-penetrating DORA with in vivo efficacy similar to that of suvorexant in rats., (© 2019 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2019

9. Essential structure of orexin 1 receptor antagonist YNT-707, Part II: Drastic effect of the 14-hydroxy group on the orexin 1 receptor antagonistic activity.

Author

Ohrui S, Yamamoto N, Saitoh T, Kutsumura N, Nagumo Y, Irukayama-Tomobe Y, Ogawa Y, Ishikawa Y, Watanabe Y, Hayakawa D, Gouda H, Yanagisawa M, and Nagase H

Subjects

Molecular Conformation, Molecular Dynamics Simulation, Molecular Structure, Morphinans chemical synthesis, Orexin Receptor Antagonists chemical synthesis, Stereoisomerism, Sulfonamides chemical synthesis, Morphinans chemistry, Orexin Receptor Antagonists chemistry, Sulfonamides chemistry

Abstract

The 14-dehydration- and 14-H derivatives of the orexin 1 receptor (OX 1 R) antagonist YNT-707 (2) were synthesized. The obtained derivatives showed higher affinities for OX 1 R than the corresponding 14-hydroxy derivatives. The conformational analysis suggested that the 17-sulfonamide groups in the derivatives without the 14-hydroxy group have a greater tendency to be oriented toward the upper side of the D-ring compared with the 14-hydroxy derivatives. Additionally, the 14-dehydration-derivative with 6α-amide side chain showed significantly higher affinity than the 14-hydroxy derivative, while the corresponding 14-H derivative showed only slightly higher affinity. Thus, the 14-hydroxy group strongly affects the affinity of the antagonist for the OX 1 R., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

10. Essential structure of orexin 1 receptor antagonist YNT-707, Part I: Role of the 4,5-epoxy ring for binding with orexin 1 receptor.

Author

Yamamoto N, Ohrui S, Okada T, Yata M, Saitoh T, Kutsumura N, Nagumo Y, Irukayama-Tomobe Y, Ogawa Y, Ishikawa Y, Watanabe Y, Hayakawa D, Gouda H, Yanagisawa M, and Nagase H

Subjects

Binding Sites drug effects, Dose-Response Relationship, Drug, Epoxy Compounds chemistry, Humans, Molecular Structure, Morphinans chemical synthesis, Morphinans chemistry, Orexin Receptor Antagonists chemical synthesis, Orexin Receptor Antagonists chemistry, Structure-Activity Relationship, Sulfonamides chemical synthesis, Sulfonamides chemistry, Epoxy Compounds pharmacology, Morphinans pharmacology, Orexin Receptor Antagonists pharmacology, Orexin Receptors metabolism, Sulfonamides pharmacology

Abstract

The essential structure of the orexin 1 receptor (OX 1 R) antagonist YNT-707 (2) was clarified, particularly the roles to OX 1 R antagonist activities of the 3-OMe, the 4,5-epoxy ring, the 14-hydroxy group, and the orientation of the 6-amide side chain. The 3-OMe and 17-sulfonamide group were shown to be essential for the OX 1 R antagonistic activity. The 4,5-epoxy ring plays an important role for the active orientation of the 6-amide group. The 14-hydroxy group could lower the activity of the 6β-amide isomer by the interaction of the 14-hydroxy group with the 6-amide group, which could orient the 6-amide group toward the upper side of the C-ring. Finally, we proposed the difference in the active conformation between OX 1 R and κ opioid receptor (KOR), especially in the orientation of the 6-amide group which is expected to be a useful guide for medicinal chemists to design OX 1 R ligands., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

11. Discovery of Highly Potent Dual Orexin Receptor Antagonists via a Scaffold-Hopping Approach.

Author

Heidmann B, Gatfield J, Roch C, Treiber A, Tortoioli S, Brotschi C, Williams JT, Bolli MH, Abele S, Sifferlen T, Jenck F, and Boss C

Subjects

Animals, Cytochrome P-450 CYP3A metabolism, Cytochrome P-450 CYP3A Inhibitors chemical synthesis, Cytochrome P-450 CYP3A Inhibitors chemistry, Dogs, Dose-Response Relationship, Drug, Humans, Male, Microsomes, Liver chemistry, Microsomes, Liver metabolism, Molecular Structure, Orexin Receptor Antagonists chemical synthesis, Orexin Receptor Antagonists chemistry, Rats, Rats, Wistar, Sleep drug effects, Structure-Activity Relationship, Cytochrome P-450 CYP3A Inhibitors pharmacology, Drug Discovery, Orexin Receptor Antagonists pharmacology, Orexin Receptors metabolism

Abstract

Starting from suvorexant (trade name Belsomra), we successfully identified interesting templates leading to potent dual orexin receptor antagonists (DORAs) via a scaffold-hopping approach. Structure-activity relationship optimization allowed us not only to improve the antagonistic potency on both orexin 1 and orexin 2 receptors (Ox1 and Ox2, respectively), but also to increase metabolic stability in human liver microsomes (HLM), decrease time-dependent inhibition of cytochrome P450 (CYP) 3A4, and decrease P-glycoprotein (Pgp)-mediated efflux. Compound 80 c [{(1S,6R)-3-(6,7-difluoroquinoxalin-2-yl)-3,8-diazabicyclo[4.2.0]octan-8-yl}(4-methyl-[1,1'-biphenyl]-2-yl)methanone] is a potent and selective DORA that inhibits the stimulating effects of orexin peptides OXA and OXB at both Ox1 and Ox2. In calcium-release assays, 80 c was found to exhibit an insurmountable antagonistic profile at both Ox1 and Ox2, while displaying a sleep-promoting effect in rat and dog models, similar to that of the benchmark compound suvorexant., (© 2016 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2016

12. Discovery of 1H-pyrazolo[3,4-b]pyridines as potent dual orexin receptor antagonists (DORAs).

Author

Behnke D, Cotesta S, Hintermann S, Fendt M, Gee CE, Jacobson LH, Laue G, Meyer A, Wagner T, Badiger S, Chaudhari V, Chebrolu M, Pandit C, Hoyer D, and Betschart C

Subjects

Administration, Intravenous, Administration, Oral, Animals, Crystallography, X-Ray, Mice, Molecular Structure, Orexin Receptor Antagonists chemical synthesis, Protein Binding drug effects, Pyrazoles chemical synthesis, Pyrazoles pharmacology, Pyridines chemical synthesis, Drug Discovery, Orexin Receptor Antagonists chemistry, Orexin Receptor Antagonists pharmacology, Pyrazoles chemistry, Pyridines chemistry, Pyridines pharmacology

Abstract

Compound rac-1 was identified by high throughput screening. Here we report SAR studies and MedChem optimization towards the highly potent dual orexin receptor antagonists (S)-2 and (S)-3. Furthermore, strategies to overcome the suboptimal physicochemical properties are highlighted and the pharmacokinetic profiles of representative compounds is presented., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

13. Discovery of diazepane amide DORAs and 2-SORAs enabled by exploration of isosteric quinazoline replacements.

Author

Roecker AJ, Mercer SP, Bergman JM, Gilbert KF, Kuduk SD, Harrell CM, Garson SL, Fox SV, Gotter AL, Tannenbaum PL, Prueksaritanont T, Cabalu TD, Cui D, Lemaire W, Winrow CJ, Renger JJ, and Coleman PJ

Subjects

Animals, Disease Models, Animal, Dogs, Dose-Response Relationship, Drug, Humans, Mice, Microsomes, Liver drug effects, Models, Molecular, Molecular Structure, Orexin Receptor Antagonists chemical synthesis, Orexin Receptor Antagonists chemistry, Pyrimidines chemical synthesis, Pyrimidines chemistry, Quinazolines chemical synthesis, Quinazolines chemistry, Rats, Structure-Activity Relationship, Drug Discovery, Orexin Receptor Antagonists pharmacology, Orexin Receptors metabolism, Pyrimidines pharmacology, Quinazolines pharmacology, Sleep Initiation and Maintenance Disorders drug therapy

Abstract

Dual orexin receptor antagonists (DORAs), or orexin 1 (OX1) and orexin 2 (OX2) receptor antagonists, have demonstrated clinical utility for the treatment of insomnia. Medicinal chemistry efforts focused on the reduction of bioactivation potential of diazepane amide 1 through the modification of the Western heterocycle resulted in the discovery of suvorexant, a DORA recently approved by the FDA for the treatment of insomnia. A second strategy towards reducing bioactivation risk is presented herein through the exploration of monocyclic quinazoline isosteres, namely substituted pyrimidines. These studies afforded potent DORAs with significantly reduced bioactivation risk and efficacy in rodent sleep models. Surprisingly, side products from the chemistry used to produce these DORAs yielded isomeric pyrimidine-containing diazepane amides possessing selective OX2R antagonist (2-SORA) profiles. Additional exploration of these isomeric pyrimidines uncovered potent 2-SORA diazepane amides with sleep efficacy in mouse EEG studies., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

14. Substituted pyrrolidin-2-ones: Centrally acting orexin receptor antagonists promoting sleep. Part 2.

Author

Sifferlen T, Boller A, Chardonneau A, Cottreel E, Gatfield J, Treiber A, Roch C, Jenck F, Aissaoui H, Williams JT, Brotschi C, Heidmann B, Siegrist R, and Boss C

Subjects

Administration, Oral, Animals, Dose-Response Relationship, Drug, Humans, Lactams administration & dosage, Lactams pharmacology, Molecular Structure, Orexin Receptor Antagonists chemical synthesis, Orexin Receptor Antagonists chemistry, Pyrrolidinones chemical synthesis, Pyrrolidinones chemistry, Rats, Structure-Activity Relationship, Orexin Receptor Antagonists pharmacology, Orexin Receptors metabolism, Pyrrolidinones pharmacology, Sleep drug effects

Abstract

Starting from advanced pyrrolidin-2-one lead compounds, this novel series of small-molecule orexin receptor antagonists was further optimized by fine-tuning of the C-3 substitution at the γ-lactam ring. We discuss our design to align in vitro potency with metabolic stability and improved physicochemical/pharmacokinetic properties while avoiding P-glycoprotein-mediated efflux. These investigations led to the identification of the orally active 3-hydroxypyrrolidin-2-one 46, a potent and selective orexin-2 receptor antagonist, that achieved good brain exposure and promoted physiological sleep in rats., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

15. Effect of 1-substitution on tetrahydroisoquinolines as selective antagonists for the orexin-1 receptor.

Author

Perrey DA, German NA, Decker AM, Thorn D, Li JX, Gilmour BP, Thomas BF, Harris DL, Runyon SP, and Zhang Y

Subjects

Animals, CHO Cells, Calcium metabolism, Cocaine pharmacology, Cricetulus, Dopamine Uptake Inhibitors pharmacology, Dose-Response Relationship, Drug, Humans, Locomotion drug effects, Locomotion physiology, Male, Molecular Structure, Orexin Receptor Antagonists chemical synthesis, Orexin Receptors chemistry, Orexin Receptors genetics, Orexin Receptors metabolism, Rats, Sprague-Dawley, Tetrahydroisoquinolines chemical synthesis, Orexin Receptor Antagonists chemistry, Orexin Receptor Antagonists pharmacology, Tetrahydroisoquinolines chemistry, Tetrahydroisoquinolines pharmacology

Abstract

Selective blockade of the orexin-1 receptor (OX1) has been suggested as a potential approach to drug addiction therapy because of its role in modulating the brain's reward system. We have recently reported a series of tetrahydroisoquinoline-based OX1 selective antagonists. Aimed at elucidating structure-activity relationship requirements in other regions of the molecule and further enhancing OX1 potency and selectivity, we have designed and synthesized a series of analogues bearing a variety of substituents at the 1-position of the tetrahydroisoquinoline. The results show that an optimally substituted benzyl group is required for activity at the OX1 receptor. Several compounds with improved potency and/or selectivity have been identified. When combined with structural modifications that were previously found to improve selectivity, we have identified compound 73 (RTIOX-251) with an apparent dissociation constant (Ke) of 16.1 nM at the OX1 receptor and >620-fold selectivity over the OX2 receptor. In vivo, compound 73 was shown to block the development of locomotor sensitization to cocaine in rats.

Published

2015