Your search keyword '"Abu J.M. Sadeque"' showing total 15 results

1. Discovery of APD371: Identification of a Highly Potent and Selective CB2 Agonist for the Treatment of Chronic Pain

Author

Michelle Solomon, Lars Thoresen, Robert M. Jones, Andrew J. Grottick, David J. Unett, Abu J.M. Sadeque, Chuan Chen, Ibragim Gaidarov, Hussien A. Al-Shamma, Jayant Thatte, Graeme Semple, Jae-Kyu Jung, Amin Usmani, Jeremy Barden, Xiuwen Zhu, Woo Hyun Yoon, Sangdon Han, and Christopher Ronald J

Subjects

0301 basic medicine, Agonist, medicine.drug_class, business.industry, Organic Chemistry, Chronic pain, Osteoarthritis, Tachyphylaxis, Pharmacology, medicine.disease, Biochemistry, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Pharmacokinetics, Oral administration, Drug Discovery, medicine, Morphine, Cannabinoid receptor type 2, business, 030217 neurology & neurosurgery, medicine.drug

Abstract

The discovery of a novel, selective and fully efficacious CB2 agonist with satisfactory pharmacokinetic and pharmaceutical properties is described. Compound 6 was efficacious in a rat model of osteoarthritis pain following oral administration and, in contrast to morphine, maintained its analgesic effect throughout a 5-day subchronic treatment paradigm. These data were consistent with our hypothesis that full agonist efficacy is required for efficient internalization and recycling of the CB2 receptor to avoid tachyphylaxis. Based on its overall favorable preclinical profile, 6 (APD371) was selected for further development for the treatment of pain.

Published

2017

2. Discovery of a novel trans-1,4-dioxycyclohexane GPR119 agonist series

Author

Khawja A. Usmani, Dawei Yue, Zhi-Liang Chu, Abu J.M. Sadeque, Chris Carroll, Chuan Chen, Hsin-Hui Shu, Sanju Narayanan, Hussein Al-Sharmma, Dominic P. Behan, Robert M. Jones, Graeme Semple, James N. Leonard, David J. Unett, Daniel J. Buzard, Michael Morgan, Juerg Lehmann, Imelda Calderon, Shiu-Feng Tung, Woo Hyun Yoon, Xiuwen Zhu, Sangdon Han, Andrew M. Kawasaki, Amy Siu-Ting Wong, and Sun Hee Kim

Subjects

Blood Glucose, Male, medicine.medical_specialty, Clinical Biochemistry, Administration, Oral, Pharmaceutical Science, Pharmacology, Biochemistry, Rats sprague dawley, Receptors, G-Protein-Coupled, Rats, Sprague-Dawley, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Cyclohexanes, Internal medicine, Drug Discovery, medicine, Animals, Humans, Hypoglycemic Agents, Structure–activity relationship, Gpr119 agonist, Molecular Biology, Glycemic, Organic Chemistry, Rats, Zucker, Endocrinology, Diabetes Mellitus, Type 2, chemistry, Molecular Medicine, Lead compound

Abstract

The design and optimization of a novel trans-1,4-dioxycyclohexane GPR119 agonist series is described. A lead compound 21 was found to be a potent and efficacious GPR119 agonist across species, and possessed overall favorable pharmaceutical properties. Compound 21 demonstrated robust acute and chronic regulatory effects on glycemic parameters in the diabetic or non-diabetic rodent models.

Published

2015

3. Discovery of 1a,2,5,5a-tetrahydro-1H-2,3-diaza-cyclopropa[a]pentalen-4-carboxamides as potent and selective CB2 receptor agonists

Author

Hussien A. Al-Shamma, Michael Morgan, Ibragim Gaidarov, Huong T. Dang, Joel Gatlin, Marc Decaire, David J. Unett, Karoline Choi, Jeff Edwards, Dawei Yue, Abu J.M. Sadeque, Kevin Whelan, Yifeng Xiong, Lixia Fu, Jayant Thatte, Graeme Semple, Sonja Strah-Pleynet, Sangdon Han, Michelle Solomon, Dominic P. Behan, Jae-Kyu Jung, Sanju Narayanan, Lars Thoresen, Robert M. Jones, Chuan Chen, Xiuwen Zhu, Khawja A. Usmani, Cameron Pride, and Ruoping Chen

Subjects

Male, Models, Molecular, Cannabinoid receptor, Clinical Biochemistry, Administration, Oral, Pain, Pharmaceutical Science, Osteoarthritis, Pharmacology, Cb2 agonist, Biochemistry, Rats, Sprague-Dawley, Receptor, Cannabinoid, CB2, Radioligand Assay, Structure-Activity Relationship, Receptor, Cannabinoid, CB1, In vivo, Oral administration, Drug Discovery, Cannabinoid receptor type 2, medicine, Animals, Humans, Potency, Molecular Biology, Inflammation, Molecular Structure, Chemistry, Organic Chemistry, Stereoisomerism, Analgesics, Non-Narcotic, medicine.disease, Arthritis, Experimental, Rats, Microsomes, Liver, Pyrazoles, Molecular Medicine, lipids (amino acids, peptides, and proteins), Selectivity, Heterocyclic Compounds, 3-Ring

Abstract

The design and synthesis of novel 1a,2,5,5a-tetrahydro-1H-2,3-diaza-cyclopropa[a]pentalen-4-carboxamide CB2 selective ligands for the potential treatment of pain is described. Compound (R,R)-25 has good balance between CB2 agonist potency and selectivity over CB1, and possesses overall favorable pharmaceutical properties. It also demonstrated robust in vivo efficacy mediated via CB2 activation in the rodent models of inflammatory and osteoarthritis pain after oral administration.

Published

2015

4. (7-Benzyloxy-2,3-dihydro-1H-pyrrolo[1,2-a]indol-1-yl)acetic Acids as S1P1 Functional Antagonists

Author

Ben Johnson, Tawfik Gharbaoui, Moody Jeanne, David J. Unett, Kevin Whelan, Ibragim Gaidarov, Michael Morgan, Lars Thoresen, Michelle Kasem, Abu J.M. Sadeque, Robert M. Jones, Chuan Chen, Sun Hee Kim, Hussien A. Al-Shamma, Minh Le, Joel Gatlin, Lorene Calvano, Andrew M. Kawasaki, Lixia Fu, Yinghong Gao, Scott Stirn, Weichao Chen, Jeremy Barden, Dominic P. Behan, Krishnan Ashwin M, Xiuwen Zhu, Graeme Semple, Dipanjan Sengupta, Christopher Ronald J, Jeff Edwards, Luis Lopez, Jayant Thatte, Daniel J. Buzard, Anthony C. Blackburn, Michelle Solomon, Todd Anthony, Thomas O. Schrader, and Khawja A. Usmani

Subjects

Autoimmune disease, Chemistry, Stereochemistry, Organic Chemistry, Pharmacology, medicine.disease, Biochemistry, Fingolimod, chemistry.chemical_compound, Pharmacokinetics, Drug Discovery, medicine, Sphingosine-1-phosphate, Direct acting, medicine.drug

Abstract

S1P1 is a validated target for treatment of autoimmune disease, and functional antagonists with superior safety and pharmacokinetic properties are being sought as second generation therapeutics. We describe the discovery and optimization of (7-benzyloxy-2,3-dihydro-1H-pyrrolo[1,2-a]indol-1-yl)acetic acids as potent, centrally available, direct acting S1P1 functional antagonists, with favorable pharmacokinetic and safety properties.

Published

2014

5. Discovery of APD334: Design of a Clinical Stage Functional Antagonist of the Sphingosine-1-phosphate-1 Receptor

Author

Weichao Chen, Andrew M. Kawasaki, Dominic P. Behan, Jeff Edwards, You-An Ma, Tawfik Gharbaoui, Sun Hee Kim, Jayant Thatte, Hussien A. Al-Shamma, Carleton R. Sage, Jeremy Barden, Anthony C. Blackburn, Michelle Solomon, Xiuwen Zhu, Christopher Ronald J, David Mills, Ibragim Gaidarov, Antonio Garrido Montalban, Sangdon Han, Luis Lopez, Dipanjan Sengupta, Michael Morgan, Juerg Lehmann, Daniel J. Buzard, Graeme Semple, Kevin Whelan, Yinghong Gao, Joel Gatlin, Moody Jeanne, David J. Unett, Imelda Calderon, Lars Thoresen, Robert M. Jones, Brett Ullman, Todd Anthony, Chuan Chen, Minh Le, Khawja A. Usmani, Scott Stirn, Jaimie Karyn Rueter, Lixia Fu, Lorene Calvano, and Abu J.M. Sadeque

Subjects

business.industry, S1p1 receptor, Multiple sclerosis, Lymphocyte, Organic Chemistry, Experimental autoimmune encephalomyelitis, Antagonist, Pharmacology, medicine.disease, Biochemistry, Fingolimod, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Drug Discovery, medicine, Sphingosine-1-phosphate, business, Receptor, medicine.drug

Abstract

APD334 was discovered as part of our internal effort to identify potent, centrally available, functional antagonists of the S1P1 receptor for use as next generation therapeutics for treating multiple sclerosis (MS) and other autoimmune diseases. APD334 is a potent functional antagonist of S1P1 and has a favorable PK/PD profile, producing robust lymphocyte lowering at relatively low plasma concentrations in several preclinical species. This new agent was efficacious in a mouse experimental autoimmune encephalomyelitis (EAE) model of MS and a rat collagen induced arthritis (CIA) model and was found to have appreciable central exposure.

Published

2014

6. Discovery of 2-(((1r,4r)-4-(((4-Chlorophenyl)(phenyl)carbamoyl)oxy)methyl)cyclohexyl)methoxy)acetate (Ralinepag): An Orally Active Prostacyclin Receptor Agonist for the Treatment of Pulmonary Arterial Hypertension

Author

Antonio Garrido Montalban, Steve Chang, Shakya Sagar, P. Douglas Boatman, Weichao Chen, Dominic P. Behan, Thuy-Anh Tran, Yunqing Shi, Young-Jun Shin, Krishnan Ashwin M, Pureza Vallar, John W. Adams, David J. Unett, Michael Morgan, Bryan A. Kramer, Biman B. Pal, Hsin-Hui Shu, Anthony C. Blackburn, Juan Ramirez, Shiu-Feng Tung, Xiaohua Chen, Tina Leakakos, Ning Zou, Abu J.M. Sadeque, Tawfik Gharbaoui, Carleton R. Sage, Anna Shifrina, Graeme Semple, and Ibragim Gaidarov

Subjects

0301 basic medicine, Agonist, medicine.drug_class, Hypertension, Pulmonary, Receptors, Prostaglandin, Administration, Oral, Biological Availability, 030204 cardiovascular system & hematology, Pharmacology, Acetates, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, 0302 clinical medicine, Oral administration, Drug Discovery, medicine, Potency, Animals, Receptor, Prostacyclin receptor, Active metabolite, Prostanoid, In vitro, Rats, 030104 developmental biology, chemistry, Molecular Medicine, Carbamates

Abstract

The design and synthesis of a new series of potent non-prostanoid IP receptor agonists that showed oral efficacy in the rat monocrotaline model of pulmonary arterial hypertension (PAH) are described. Detailed profiling of a number of analogues resulted in the identification of 5c (ralinepag) that has good selectivity in both binding and functional assays with respect to most members of the prostanoid receptor family and a more modest 30- to 50-fold selectivity over the EP3 receptor. In our hands, its potency and efficacy are comparable or superior to MRE269 (the active metabolite of the clinical compound NS-304) with respect to in vitro IP receptor dependent cAMP accumulation assays. 5c had an excellent PK profile across species. Enterohepatic recirculation most probably contributes to a concentration-time profile after oral administration in the cynomolgus monkey that showed a very low peak-to-trough ratio. Following the identification of an acceptable solid form, 5c was selected for further development for the treatment of PAH.

Published

2017

7. Fused tricyclic indoles as S1P1 agonists with robust efficacy in animal models of autoimmune disease

Author

Joel Gatlin, Kevin Whelan, Michael Morgan, Juerg Lehmann, Lixia Fu, Yinghong Gao, Moody Jeanne, Minh Le, Hussien A. Al-Shamma, Jeremy Barden, Khawja A. Usmani, Jeff Edwards, Chuan Chen, Jayant Thatte, Dipanjan Sengupta, Xiuwen Zhu, Abu J.M. Sadeque, Imelda Calderon, Michelle Solomon, Lars Thoresen, Tawfik Gharbaoui, Robert M. Jones, Ling Liu, Luis Lopez, Daniel J. Buzard, Brett Ullman, Krishnan Ashwin M, Sheryll Espinola, Charles Xing, Sangdon Han, and Andrew M. Kawasaki

Subjects

Autoimmune disease, chemistry.chemical_classification, Chemistry, Sphingosine-1-phosphate receptor, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Pharmacology, medicine.disease, Biochemistry, In vitro, Sprague dawley, In vivo, Drug Discovery, medicine, Molecular Medicine, Structure–activity relationship, lipids (amino acids, peptides, and proteins), Receptor, Molecular Biology, Tricyclic

Abstract

Two series of fused tricyclic indoles were identified as potent and selective S1P(1) agonists. In vivo these agonists produced a significant reduction in circulating lymphocytes which translated into robust efficacy in several rodent models of autoimmune disease. Importantly, these agonists were devoid of any activity at the S1P(3) receptor in vitro, and correspondingly did not produce S1P(3) mediated bradycardia in telemeterized rat.

Published

2012

8. Identification of Human Sulfotransferases Involved in Lorcaserin N-Sulfamate Formation

Author

Weichao G. Chen, Khawja A. Usmani, Chuan Chen, Safet Palamar, Abu J.M. Sadeque, and Matthew A. Cerny

Subjects

0301 basic medicine, Agonist, Male, medicine.drug_class, Metabolite, Pharmaceutical Science, Pharmacology, Lorcaserin, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Therapeutic index, medicine, Humans, Receptor, chemistry.chemical_classification, Dose-Response Relationship, Drug, Metabolism, Benzazepines, Cytosol, 030104 developmental biology, Enzyme, chemistry, 030220 oncology & carcinogenesis, Microsomes, Liver, Female, Sulfonic Acids, Sulfotransferases, medicine.drug, Protein Binding

Abstract

Lorcaserin [(R)-8-chloro-1-methyl-2,3,4,5-tetrahydro-1H-3-benzazepine] hydrochloride hemihydrate, a selective serotonin 5-hydroxytryptamine (5-HT) 5-HT(2C) receptor agonist, is approved by the U.S. Food and Drug Administration for chronic weight management. Lorcaserin is primarily cleared by metabolism, which involves multiple enzyme systems with various metabolic pathways in humans. The major circulating metabolite is lorcaserin N-sulfamate. Both human liver and renal cytosols catalyze the formation of lorcaserin N-sulfamate, where the liver cytosol showed a higher catalytic efficiency than renal cytosol. Human sulfotransferases (SULTs) SULT1A1, SULT1A2, SULT1E1, and SULT2A1 are involved in the formation of lorcaserin N-sulfamate. The catalytic efficiency of these SULTs for lorcaserin N-sulfamate formation is widely variable, and among the SULT isoforms SULT1A1 was the most efficient. The order of intrinsic clearance for lorcaserin N-sulfamate is SULT1A1 > SULT2A1 > SULT1A2 > SULT1E1. Inhibitory effects of lorcaserin N-sulfamate on major human cytochrome P450 (P450) enzymes were not observed or minimal. Lorcaserin N-sulfamate binds to human plasma protein with high affinity (i.e., >99%). Thus, despite being the major circulating metabolite, the level of free lorcaserin N-sulfamate would be minimal at a lorcaserin therapeutic dose and unlikely be sufficient to cause drug-drug interactions. Considering its formation kinetic parameters, high plasma protein binding affinity, minimal P450 inhibition or induction potential, and stability, the potential for metabolic drug-drug interaction or toxicological effects of lorcaserin N-sulfamate is remote in a normal patient population.

Published

2015

9. Discovery and optimization of 5-fluoro-4,6-dialkoxypyrimidine GPR119 agonists

Author

Luis Lopez, Daniel J. Buzard, Abu J.M. Sadeque, David J. Unett, Ching-Fen Chuang, Hsin-Hui Shu, Rohit Bhat, James N. Leonard, Sanju Narayanan, Dawei Yue, Robert M. Jones, Amy Siu-Ting Wong, Michael Morgan, Zhi-Liang Chu, Juerg Lehmann, Sun Hee Kim, Hussien A. Al-Shamma, Imelda Calderon, Kevin Whelan, Steve Chang, Shiu-Feng Tung, Tawfik Gharbaoui, Andrew M. Kawasaki, and Sangdon Han

Subjects

Agonist, Inhibitory potential, Glucose control, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, medicine.drug_class, Pyridines, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Pharmacology, Biochemistry, In vitro, Receptors, G-Protein-Coupled, Structure-Activity Relationship, GPR119, Piperidines, Drug Discovery, medicine, Molecular Medicine, Humans, Molecular Biology, CYP2C9

Abstract

A series of 5-fluoro-4,6-dialkoxypyrimidine GPR119 modulators were discovered and optimized for in vitro agonist activity. A lead molecule was identified that has improved agonist efficacy relative to our clinical compound (APD597) and possesses reduced CYP2C9 inhibitory potential. This optimized lead was found to be efficacious in rodent models of glucose control both alone and in combination with a Dipeptidyl peptidase-4 (DPP-4) inhibitor.

Published

2014

10. Biopharmaceutics permeability classification of lorcaserin, a selective 5-hydroxytryptamine 2C agonist: method suitability and permeability class membership

Author

Michael G. Ma, Cody L. Fullenwider, Weichao G. Chen, Abu J.M. Sadeque, and Chuan Chen

Subjects

Agonist, Serotonin, medicine.drug_class, Pharmaceutical Science, Pharmacology, Permeability, Lorcaserin, Biopharmaceutics, Drug Discovery, medicine, Humans, ATP Binding Cassette Transporter, Subfamily B, Member 1, Class membership, Chemistry, United States Food and Drug Administration, Benzazepines, Hydrogen-Ion Concentration, Biopharmaceutics Classification System, United States, Permeability (earth sciences), Intestinal Absorption, Solubility, Molecular Medicine, Serotonin Antagonists, Caco-2 Cells, medicine.drug

Abstract

The objectives of the study were (1) to demonstrate that a Caco-2 cell-based permeability assay, developed in our laboratory, is suitable to identify the permeability classification according to the US Food and Drug Administration Biopharmaceutics Classification System guidance, and (2) to use the validated Caco-2 method to determine permeability class membership of lorcaserin. Lorcaserin, marketed in United States as Belviq, is a selective human 5-hydroxytryptamine 2C agonist used for weight management. First, the permeability of twenty commercially available drugs was determined in the apical-to-basolateral direction at a final concentration of 10 μM, with the pH of transporter buffer in the apical and basolateral compartments being 6.8 and 7.4, respectively. A rank-order relationship between in vitro permeability results and the extent of human intestinal absorption for the drugs tested was observed. Second, the apparent permeability coefficient values of lorcaserin at 2, 20, and 200 μM and apical pH values of 6.8 and 7.4 in the apical-to-basolateral direction were determined using the validated method and found to be comparable to those of the high-permeability internal standard metoprolol. Lorcaserin permeability across Caco-2 cell monolayers was not dependent on the variation of apical pH. Furthermore, lorcaserin was not a substrate for efflux transporters such as P-glycoprotein. In conclusion, using the validated Caco-2 permeability assay, it was shown that lorcaserin is a highly permeable compound.

Published

2013

11. Kinetics of 5-HT2B receptor signaling: profound agonist-dependent effects on signaling onset and duration

Author

Chuan Chen, Charles Xing, Todd Anthony, John Frazer, Abu J.M. Sadeque, Daniel J. Buzard, Huong T. Dang, Joel Gatlin, Ibragim Gaidarov, Xiaohua Chen, Minh Le, David J. Unett, and Steve Chang

Subjects

Agonist, Ergot Alkaloids, medicine.drug_class, Arrestins, Pharmacology, Radioligand Assay, In vivo, Calcium flux, Receptor, Serotonin, 5-HT2B, medicine, Humans, Phosphorylation, Inositol phosphate, Receptor, Extracellular Signal-Regulated MAP Kinases, Adrenergic alpha-Antagonists, beta-Arrestins, chemistry.chemical_classification, Dose-Response Relationship, Drug, Phenoxybenzamine, Chemistry, Beta-Arrestins, Amphetamines, Serotonin Receptor Agonists, HEK293 Cells, Biophysics, Molecular Medicine, Calcium, Signal transduction, Ex vivo, Signal Transduction

Abstract

The kinetics of drug-receptor interactions can profoundly influence in vivo and in vitro pharmacology. In vitro, the potencies of slowly associating agonists may be underestimated in assays capturing transient signaling events. When divergent receptor-mediated signaling pathways are evaluated using combinations of equilibrium and transient assays, potency differences driven by kinetics may be erroneously interpreted as biased signaling. In vivo, drugs with slow dissociation rates may display prolonged physiologic effects inconsistent with their pharmacokinetic profiles. We evaluated a panel of 5-hydroxytryptamine2B (5-HT2B) receptor agonists in kinetic radioligand binding assays and in transient, calcium flux assays, and inositol phosphate accumulation assays; two functional readouts emanating from Gαq-mediated activation of phospholipase C. In binding studies, ergot derivatives demonstrated slow receptor association and dissociation rates, resulting in significantly reduced potency in calcium assays relative to inositol phosphate accumulation assays. Ergot potencies for activation of extracellular signal-regulated kinases 1 and 2 were also highly time-dependent. A number of ergots produced wash-resistant 5-HT2B signaling that persisted for many hours without appreciable loss of potency, which was not explained simply by slow receptor-dissociation kinetics. Mechanistic studies indicated that persistent signaling originated from internalized or sequestered receptors. This study provides a mechanistic basis for the long durations of action in vivo and wash-resistant effects in ex vivo tissue models often observed for ergots. The 5-HT2B agonist activity of a number of ergot-derived therapeutics has been implicated in development of cardiac valvulopathy in man. The novel, sustained nature of ergot signaling reported here may represent an additional mechanism contributing to the valvulopathic potential of these compounds.

Published

2013

12. Identification of human cytochrome P450 and flavin-containing monooxygenase enzymes involved in the metabolism of lorcaserin, a novel selective human 5-hydroxytryptamine 2C agonist

Author

Khawja A. Usmani, Weichao G. Chen, and Abu J.M. Sadeque

Subjects

Furafylline, CYP2B6, Pharmaceutical Science, Flavin-containing monooxygenase, Biology, Pharmacology, In Vitro Techniques, Catalysis, Lorcaserin, chemistry.chemical_compound, Cytochrome P-450 Enzyme System, medicine, Receptor, Serotonin, 5-HT2C, Humans, CYP2A6, Biotransformation, CYP3A4, CYP1A2, Monooxygenase, Benzazepines, chemistry, Biochemistry, Microsomes, Liver, Oxygenases, Metabolic Detoxication, Phase I, Serotonin 5-HT2 Receptor Agonists, medicine.drug

Abstract

Lorcaserin, a selective serotonin 5-hydroxytryptamine 2C receptor agonist, is being developed for weight management. The oxidative metabolism of lorcaserin, mediated by recombinant human cytochrome P450 (P450) and flavin-containing monooxygenase (FMO) enzymes, was examined in vitro to identify the enzymes involved in the generation of its primary oxidative metabolites, N-hydroxylorcaserin, 7-hydroxylorcaserin, 5-hydroxylorcaserin, and 1-hydroxylorcaserin. Human CYP1A2, CYP2A6, CYP2B6, CYP2C19, CYP2D6, CYP3A4, and FMO1 are major enzymes involved in N-hydroxylorcaserin; CYP2D6 and CYP3A4 are enzymes involved in 7-hydroxylorcaserin; CYP1A1, CYP1A2, CYP2D6, and CYP3A4 are enzymes involved in 5-hydroxylorcaserin; and CYP3A4 is an enzyme involved in 1-hydroxylorcaserin formation. In 16 individual human liver microsomal preparations (HLM), formation of N-hydroxylorcaserin was correlated with CYP2B6, 7-hydroxylorcaserin was correlated with CYP2D6, 5-hydroxylorcaserin was correlated with CYP1A2 and CYP3A4, and 1-hydroxylorcaserin was correlated with CYP3A4 activity at 10.0 μM lorcaserin. No correlation was observed for N-hydroxylorcaserin with any P450 marker substrate activity at 1.0 μM lorcaserin. N-Hydroxylorcaserin formation was not inhibited by CYP1A2, CYP2A6, CYP2B6, CYP2C19, CYP2D6, and CYP3A4 inhibitors at the highest concentration tested. Furafylline, quinidine, and ketoconazole, selective inhibitors of CYP1A2, CYP2D6, and CYP3A4, respectively, inhibited 5-hydroxylorcaserin (IC(50) = 1.914 μM), 7-hydroxylorcaserin (IC(50) = 0.213 μM), and 1-hydroxylorcaserin formation (IC(50) = 0.281 μM), respectively. N-Hydroxylorcaserin showed low and high K(m) components in HLM and 7-hydroxylorcaserin showed lower K(m) than 5-hydroxylorcaserin and 1-hydroxylorcaserin in HLM. The highest intrinsic clearance was observed for N-hydroxylorcaserin, followed by 7-hydroxylorcaserin, 5-hydroxylorcaserin, and 1-hydroxylorcaserin in HLM. Multiple human P450 and FMO enzymes catalyze the formation of four primary oxidative metabolites of lorcaserin, suggesting that lorcaserin has a low probability of drug-drug interactions by concomitant medications.

Published

2012

13. Identification of human UDP-glucuronosyltransferases involved in N-carbamoyl glucuronidation of lorcaserin

Author

Abu J.M. Sadeque, Matthew A. Cerny, Khawja A. Usmani, Safet Palamar, and Weichao G. Chen

Subjects

UGT1A6, Glucuronosyltransferase, Glucuronidation, Pharmaceutical Science, Pharmacology, Glucuronidation Pathway, In Vitro Techniques, Kidney, Lorcaserin, Glucuronides, Microsomes, medicine, Receptor, Serotonin, 5-HT2C, Humans, Enzyme Inhibitors, Intestinal Mucosa, biology, Molecular Structure, Chemistry, Benzazepines, UGT2B7, Intestines, Kinetics, Liver, Microsome, biology.protein, Glucuronide, Serotonin 5-HT2 Receptor Agonists, medicine.drug

Abstract

Lorcaserin, a selective serotonin 5-HT(2C) receptor agonist, is a weight management agent in clinical development. Lorcaserin N-carbamoyl glucuronidation governs the predominant excretory pathway of lorcaserin in humans. Human UDP-glucuronosyltransferases (UGTs) responsible for lorcaserin N-carbamoyl glucuronidation are identified herein. Lorcaserin N-carbamoyl glucuronide formation was characterized by the following approaches: metabolic screening using human tissues (liver, kidney, intestine, and lung) and recombinant enzymes, kinetic analyses, and inhibition studies. Whereas microsomes from all human tissues studied herein were found to be catalytically active for lorcaserin N-carbamoyl glucuronidation, liver microsomes were the most efficient. With recombinant UGT enzymes, lorcaserin N-carbamoyl glucuronidation was predominantly catalyzed by three UGT2Bs (UGT2B7, UGT2B15, and UGT2B17), whereas two UGT1As (UGT1A6 and UGT1A9) played a minor role. UGT2B15 was most efficient, with an apparent K(m) value of 51.6 ± 1.9 μM and V(max) value of 237.4 ± 2.8 pmol/mg protein/min. The rank order of catalytic efficiency of human UGT enzymes for lorcaserin N-carbamoyl glucuronidation was UGT2B15 > UGT2B7 > UGT2B17 > UGT1A9 > UGT1A6. Inhibition of lorcaserin N-carbamoyl glucuronidation activities of UGT2B7, UGT2B15, and UGT2B17 in human liver microsomes by mefenamic acid, bisphenol A, and eugenol further substantiated the involvement of these UGT2B isoforms. In conclusion, multiple human UGT enzymes catalyze N-carbamoyl glucuronidation of lorcaserin; therefore, it is unlikely that inhibition of any one of these UGT activities will lead to significant inhibition of the lorcaserin N-carbamoyl glucuronidation pathway. Thus, the potential for drug-drug interaction by concomitant administration of a drug(s) that is metabolized by any of these UGTs is remote.

Published

2012

14. Discovery and structure-activity relationship of 3-methoxy-N-(3-(1-methyl-1H-pyrazol-5-yl)-4-(2-morpholinoethoxy)phenyl)benzamide (APD791): a highly selective 5-hydroxytryptamine2A receptor inverse agonist for the treatment of arterial thrombosis

Author

Abu J.M. Sadeque, Michael Morgan, Marc Decaire, Honnappa Jayakumar, Lan Pham, John W. Adams, Graeme Semple, Jin-Sun Karoline Choi, Konrad Feichtinger, Yifeng Xiong, Bradley Teegarden, John Frazer, Diane Yuskin, Sonja Strah-Pleynet, Weichao Chen, Brett Ullman, Robert R. Webb, Hussien A. Al-Shamma, Martin Casper, Peter I. Dosa, and Daniel T. Connolly

Subjects

Male, Drug Inverse Agonism, Platelet Aggregation, Stereochemistry, Morpholines, hERG, Pharmacology, Pyrazole, Substrate Specificity, chemistry.chemical_compound, Inhibitory Concentration 50, Structure-Activity Relationship, Dogs, Drug Discovery, Structure–activity relationship, Inverse agonist, Animals, Humans, Platelet, Receptor, Serotonin, 5-HT2A, Receptor, Benzamide, biology, Thrombosis, Arteries, Rats, chemistry, Benzamides, biology.protein, Molecular Medicine, Pyrazoles, Female, Serotonin 5-HT2 Receptor Agonists

Abstract

Serotonin, which is stored in platelets and is released during thrombosis, activates platelets via the 5-HT(2A) receptor. 5-HT(2A) receptor inverse agonists thus represent a potential new class of antithrombotic agents. Our medicinal program began with known compounds that displayed binding affinity for the recombinant 5-HT(2A) receptor, but which had poor activity when tested in human plasma platelet inhibition assays. We herein describe a series of phenyl pyrazole inverse agonists optimized for selectivity, aqueous solubility, antiplatelet activity, low hERG activity, and good pharmacokinetic properties, resulting in the discovery of 10k (APD791). 10k inhibited serotonin-amplified human platelet aggregation with an IC(50) = 8.7 nM and had negligible binding affinity for the closely related 5-HT(2B) and 5-HT(2C) receptors. 10k was orally bioavailable in rats, dogs, and monkeys and had an acceptable safety profile. As a result, 10k was selected further evaluation and advanced into clinical development as a potential treatment for arterial thrombosis.

Published

2010

15. Pharmaceutical Excipients in Drug-Drug Interaction

Author

Chuan Chen and Abu J.M. Sadeque

Subjects

Drug, Interaction potential, Drug development, Chemistry, business.industry, media_common.quotation_subject, Drug-drug interaction, Medicine, Drug interaction, Pharmacology, Pharmaceutical formulation, business, media_common

Abstract

During the development of a given drug formulation, the interactions between the drug and excipients need to be carefully studied to ensure that the drug is stable in the formulation. Enzyme-based drug interaction involving excipients appears to occur predominantly in preclinical studies. The article discusses drug-drug interaction potential of pharmaceutical excipients, with a focus on solubilizing excipients. Keywords: drug-drug interactions; enzyme-based drug interaction; drug development; drug formulation; pharmaceutical excipients

Published

2009