Your search keyword '"Medina, Julio C."' showing total 58 results

1. Novel series of tunable µOR modulators with enhanced brain penetration for the treatment of opioid use disorder, pain and neuropsychiatric indications.

Author

Nerurkar A, Nguyen T, Wang S, Bhatt U, Li K, Li Y, Ding P, Seidl FJ, Holan M, Lee J, Widjaja T, Wei ZL, Sadlowski C, Sperandio D, McGee LR, Youngblood B, Schwartz N, Gehlert D, and Medina JC

Subjects

Rats, Animals, Amides, Brain metabolism, Receptors, Opioid, mu agonists, Analgesics, Opioid pharmacology, Analgesics, Opioid therapeutic use, Pain drug therapy, Opioid-Related Disorders

Abstract

Structural optimization of a previously reported agonist of µOR, PZM21 is described resulting in the discovery of a novel series of amides with at least 4-folds enhanced CNS penetration in rat. Furthermore, these efforts yielded compounds with varying levels of efficacy on the receptor ranging from high efficacy agonists such as compound 20 to antagonists, such as 24. The correlation between in vitro activation of µOR and relative activity in models of analgesia for these compounds is discussed. The compelling results obtained in these studies demonstrate the potential utility of these newly discovered compounds in the treatment of pain and opioid use disorder., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 R2M Pharma. Published by Elsevier Ltd.. All rights reserved.)

Published

2023

2. EPD1504: a novel μ-opioid receptor partial agonist attenuates obsessive-compulsive disorder (OCD)-like behaviors.

Author

Youngblood B, Medina JC, Gehlert DR, and Schwartz N

Abstract

Low doses of μ-opioid receptor (MOR) agonists rapidly ameliorate symptoms in treatment-resistant obsessive-compulsive disorder (OCD) patients (10-50% of OCD patients). However, the utility of MOR agonists is limited by their safety liabilities. We developed a novel MOR partial agonist (EPD1540) that has an improved respiratory safety profile when compared to buprenorphine. Buprenorphine is a MOR partial agonist primarily used in the treatment of opiate-use disorder, which in investigator-led trials, has been shown to rapidly ameliorate symptoms in treatment-resistant OCD patients. In this study, we show that doses of EPD1504 and buprenorphine that occupy small fractions of MORs in the CNS (approximately 20%) are as effective as fluoxetine at ameliorating OCD-like behaviors in two different rat models (an operant probabilistic reversal task and marble burying). Importantly, effective doses of EPD1504 did not impair either locomotor activity, or respiration under normoxic or hypercapnic conditions. Additionally, EPD1504 had effects comparable to buprenorphine in the conditioned place preference assay. These results indicate that EPD1504 may provide a safer alternative to buprenorphine for the treatment of OCD patients., Competing Interests: BY, DG, and NS are employees of and stockholders in Epiodyne, Inc. JM is an Epiodyne stockholder, and a stockholder and employee of R2M., (Copyright © 2023 Youngblood, Medina, Gehlert and Schwartz.)

Published

2023

3. Endogenous µ-opioid receptor activity in the lateral and capsular subdivisions of the right central nucleus of the amygdala prevents chronic postoperative pain.

Author

Cooper AH, Hedden NS, Corder G, Lamerand SR, Donahue RR, Morales-Medina JC, Selan L, Prasoon P, and Taylor BK

Subjects

Animals, Female, Male, Mice, Naloxone pharmacology, Narcotic Antagonists pharmacology, Pain, Postoperative drug therapy, Pain, Postoperative prevention & control, Receptors, Opioid, Receptors, Opioid, mu, Central Amygdaloid Nucleus metabolism, Hyperalgesia drug therapy, Hyperalgesia metabolism, Hyperalgesia prevention & control

Abstract

Tissue injury induces a long-lasting latent sensitization (LS) of spinal nociceptive signaling that is kept in remission by an opposing µ-opioid receptor (MOR) constitutive activity. To test the hypothesis that supraspinal sites become engaged, we induced hindpaw inflammation, waited 3 weeks for mechanical hypersensitivity to resolve, and then injected the opioid receptor inhibitors naltrexone, CTOP or β-funaltrexamine subcutaneously, and/or into the cerebral ventricles. Intracerebroventricular injection of each inhibitor reinstated hypersensitivity and produced somatic signs of withdrawal, indicative of LS and endogenous opioid dependence, respectively. In naïve or sham controls, systemic naloxone (3 mg/kg) produced conditioned place aversion, and systemic naltrexone (3 mg/kg) increased Fos expression in the central nucleus of the amygdala (CeA). In LS animals tested 3 weeks after plantar incision, systemic naltrexone reinstated mechanical hypersensitivity and produced an even greater increase in Fos than in sham controls, particularly in the capsular subdivision of the right CeA. One third of Fos+ profiles co-expressed protein kinase C delta (PKCδ), and 35% of PKCδ neurons co-expressed tdTomato+ in Oprm1 Cre ::tdTomato transgenic mice. CeA microinjection of naltrexone (1 µg) reinstated mechanical hypersensitivity only in male mice and did not produce signs of somatic withdrawal. Intra-CeA injection of the MOR-selective inhibitor CTAP (300 ng) reinstated hypersensitivity in both male and female mice. We conclude that MORs in the capsular subdivision of the right CeA prevent the transition from acute to chronic postoperative pain., (© 2021 Wiley Periodicals LLC.)

Published

2022

4. A Novel Maintenance Therapeutic for Opioid Use Disorder.

Author

Youngblood B, Li K, Gehlert DR, Medina JC, and Schwartz N

Subjects

Animals, Humans, Analgesics, Opioid therapeutic use, Analgesics, Opioid pharmacology, Naltrexone therapeutic use, Naltrexone pharmacology, Narcotic Antagonists therapeutic use, Narcotic Antagonists pharmacology, Opiate Substitution Treatment methods, Receptors, Opioid, mu agonists, Substance Withdrawal Syndrome drug therapy, Buprenorphine therapeutic use, Buprenorphine pharmacology, Opioid-Related Disorders drug therapy

Abstract

Opioid use disorder (OUD) is a major socioeconomic burden. An ideal OUD pharmacotherapy will mitigate the suffering associated with opioid-withdrawal, inhibit the effects of high efficacy opioids, and minimize opioid-cravings while being safe and accessible to a diverse patient population. Although current OUD pharmacotherapies inhibit the euphoric effects of opioids of abuse, the extent to which they safely alleviate withdrawal and opioid-cravings corresponds with their intrinsic µ opioid receptor (MOR) efficacy. In addition to inhibiting the euphoric effects of opioids of abuse, the medium efficacy MOR agonist buprenorphine alleviates withdrawal and opioid-cravings, but its intrinsic MOR efficacy is sufficient such that its utility is limited by abuse and safety liabilities. Although the MOR antagonist naltrexone minimizes euphoria and has no abuse liability, it exacerbates suffering associated with withdrawal and opioid cravings. Therefore, a therapeutic with intrinsic MOR activity between the partial agonist (buprenorphine) and the antagonist (naltrexone) would strike a balance between the benefits and liabilities of these two therapeutics. To address this need, we derived RM1490, an MOR agonist based on a nonmorphinan scaffold that exhibits approximately half the intrinsic MOR efficacy of buprenorphine. In a series of preclinical assays, we compared RM1490 with buprenorphine and naltrexone at doses that achieve therapeutic levels of central nervous system MOR occupancy. RM1490 exhibited a behavioral profile consistent with reduced reward, dependence, and precipitated withdrawal liabilities. RM1490 was also more effective than buprenorphine at reversing the respiratory depressant effects of fentanyl and did not suppress respiration when combined with diazepam. SIGNIFICANCE STATEMENT: In preclinical studies, RM1490 has a physiological and behavioral profile suitable for opioid use disorder maintenance therapy., (Copyright © 2021 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2021

5. Discovery and in Vivo Evaluation of Macrocyclic Mcl-1 Inhibitors Featuring an α-Hydroxy Phenylacetic Acid Pharmacophore or Bioisostere.

Author

Rescourio G, Gonzalez AZ, Jabri S, Belmontes B, Moody G, Whittington D, Huang X, Caenepeel S, Cardozo M, Cheng AC, Chow D, Dou H, Jones A, Kelly RC, Li Y, Lizarzaburu M, Lo MC, Mallari R, Meleza C, Rew Y, Simonovich S, Sun D, Turcotte S, Yan X, Wong SG, Yanez E, Zancanella M, Houze J, Medina JC, Hughes PE, and Brown SP

Subjects

Administration, Oral, Animals, Antineoplastic Agents administration & dosage, Antineoplastic Agents pharmacokinetics, Biological Availability, Cell Line, Tumor, Crystallography, X-Ray, Drug Design, Drug Stability, Female, Humans, Hydrogen Bonding, Mice, Nude, Multiple Myeloma drug therapy, Myeloid Cell Leukemia Sequence 1 Protein chemistry, Myeloid Cell Leukemia Sequence 1 Protein metabolism, Rats, Sprague-Dawley, Structure-Activity Relationship, Sulfonamides chemistry, Xenograft Model Antitumor Assays, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Myeloid Cell Leukemia Sequence 1 Protein antagonists & inhibitors, Phenylacetates chemistry

Abstract

Overexpression of the antiapoptotic protein Mcl-1 provides a survival advantage to some cancer cells, making inhibition of this protein an attractive therapeutic target for the treatment of certain types of tumors. Herein, we report our efforts toward the identification of a novel series of macrocyclic Mcl-1 inhibitors featuring an α-hydroxy phenylacetic acid pharmacophore or bioisostere. This work led to the discovery of 1 , a potent Mcl-1 inhibitor (IC 50 = 19 nM in an OPM-2 cell viability assay) with good pharmacokinetic properties and excellent in vivo efficacy in an OPM-2 multiple myeloma xenograft model.

Published

2019

6. Discovery of a Potent Steroidal Glucocorticoid Receptor Antagonist with Enhanced Selectivity against the Progesterone and Androgen Receptors (OP-3633).

Author

Du X, Eksterowicz J, Zhou H, Rew Y, Zhu L, Yan X, Medina JC, Huang T, Chen X, Sutimantanapi D, Jahchan N, Kong W, Sun J, Zavorotinskaya T, Ye Q, Fantin VR, and Sun D

Subjects

Androgen Receptor Antagonists chemistry, Androgen Receptor Antagonists pharmacology, Drug Discovery, Humans, Models, Molecular, Receptors, Androgen metabolism, Receptors, Glucocorticoid metabolism, Receptors, Progesterone antagonists & inhibitors, Receptors, Progesterone metabolism, Mifepristone analogs & derivatives, Mifepristone pharmacology, Receptors, Glucocorticoid antagonists & inhibitors

Abstract

Structure-based modification of mifepristone ( 1 ) led to the discovery of novel mifepristone derivatives with improved selectivity profile. Addition of a methyl group at the C10 position of the steroid has a significant impact on progesterone receptor (PR) and androgen receptor (AR) activity. Within this series, OP-3633 ( 15 ) emerged as a glucocorticoid receptor (GR) antagonist with increased selectivity against PR and AR, improved cytochrome P450 inhibition profile, and significantly improved pharmacokinetic properties compared to 1 . Furthermore, 15 demonstrated substantial inhibition of GR transcriptional activity in the GR positive HCC1806 triple negative breast cancer xenograft model. Overall, compound 15 is a promising GR antagonist candidate to clinically evaluate the impact of GR inhibition in reversal or prevention of therapy resistance.

Published

2019

7. Cerebrolysin improves peripheral inflammatory pain: Sex differences in two models of acute and chronic mechanical hypersensitivity.

Author

Morales-Medina JC, Flores G, Vallelunga A, Griffiths NH, and Iannitti T

Subjects

Acute Pain immunology, Animals, Carrageenan, Chronic Pain immunology, Disease Models, Animal, Edema immunology, Female, Freund's Adjuvant, Hyperalgesia immunology, Inflammation, Male, Pain Measurement, Rats, Wistar, Time Factors, Acute Pain drug therapy, Amino Acids therapeutic use, Chronic Pain drug therapy, Edema drug therapy, Hyperalgesia drug therapy, Neuroprotective Agents therapeutic use, Sex Characteristics

Abstract

Chronic inflammatory pain is a major health problem worldwide with high prevalence in women. Cerebrolysin is a multimodal neuropeptide preparation that crosses the blood brain barrier and displays neuroprotective properties in aging and disease. Previously, we showed that cerebrolysin reduced mechanical allodynia in a model of persistent inflammation and pain. We aim to build upon the findings of our previous study by investigating the response to acute administration of cerebrolysin in two models of peripheral inflammation and assessing sex differences. We utilized the complete Freund's adjuvant (CFA) that produces maximal oedema and mechanical allodynia within days and carrageenan that produces similar effects within hours. Cerebrolysin reversed the mechanical allodynia in both sexes in CFA-treated rats. On the other hand, in rats treated with carrageenan, cerebrolysin was only effective in reducing mechanical allodynia in female rats. In conclusion, the present study shows that cerebrolysin effects may be sex-specific depending on different mechanisms that are at play in these two models of peripheral inflammatory pain. Further investigations are required to determine the factors contributing to sex differences., (© 2019 Wiley Periodicals, Inc.)

Published

2019

8. Discovery of a Potent and Selective Steroidal Glucocorticoid Receptor Antagonist (ORIC-101).

Author

Rew Y, Du X, Eksterowicz J, Zhou H, Jahchan N, Zhu L, Yan X, Kawai H, McGee LR, Medina JC, Huang T, Chen C, Zavorotinskaya T, Sutimantanapi D, Waszczuk J, Jackson E, Huang E, Ye Q, Fantin VR, and Sun D

Subjects

Animals, Female, Hormone Antagonists chemistry, Hormone Antagonists pharmacokinetics, Humans, Mice, Ovarian Neoplasms metabolism, Ovarian Neoplasms pathology, Rats, Swine, Swine, Miniature, Tissue Distribution, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Drug Discovery, Hormone Antagonists pharmacology, Ovarian Neoplasms drug therapy, Receptors, Glucocorticoid antagonists & inhibitors

Abstract

The glucocorticoid receptor (GR) has been linked to therapy resistance across a wide range of cancer types. Preclinical data suggest that antagonists of this nuclear receptor may enhance the activity of anticancer therapy. The first-generation GR antagonist mifepristone is currently undergoing clinical evaluation in various oncology settings. Structure-based modification of mifepristone led to the discovery of ORIC-101 (28), a highly potent steroidal GR antagonist with reduced androgen receptor (AR) agonistic activity amenable for dosing in androgen receptor positive tumors and with improved CYP2C8 and CYP2C9 inhibition profile to minimize drug-drug interaction potential. Unlike mifepristone, 28 could be codosed with chemotherapeutic agents readily metabolized by CYP2C8 such as paclitaxel. Furthermore, 28 demonstrated in vivo antitumor activity by enhancing response to chemotherapy in the GR + OVCAR5 ovarian cancer xenograft model. Clinical evaluation of safety and therapeutic potential of 28 is underway.

Published

2018

9. Molecular Characterization of Carbapenem-Resistant Acinetobacter baumannii in the Intensive Care Unit of Uruguay's University Hospital Identifies the First rmtC Gene in the Species.

Author

Bado I, Papa-Ezdra R, Delgado-Blas JF, Gaudio M, Gutiérrez C, Cordeiro NF, García-Fulgueiras V, Araújo Pirez L, Seija V, Medina JC, Rieppi G, Gonzalez-Zorn B, and Vignoli R

Subjects

Acinetobacter Infections microbiology, Anti-Bacterial Agents pharmacology, Cross Infection microbiology, Female, Hospitals, University, Humans, Intensive Care Units, Male, Microbial Sensitivity Tests methods, Middle Aged, Multilocus Sequence Typing methods, RNA, Ribosomal, 16S genetics, Uruguay, Acinetobacter baumannii drug effects, Acinetobacter baumannii genetics, Bacterial Proteins genetics, Carbapenems pharmacology, Drug Resistance, Multiple, Bacterial genetics, Genes, Bacterial genetics, beta-Lactamases genetics

Abstract

Carbapenem-resistant Acinetobacter baumannii (CRAB) infections are an increasing concern in intensive care units (ICUs) worldwide. The combination of carbapenemases and 16S rRNA-methyltransferases (16S-RMTases) further reduces the therapeutic options. OXA-carbapenemase/A. baumannii clone tandems in Latin America have already been described; however, no information exists in this region regarding the occurrence of 16S-RMTases in this microorganism. In addition, the epidemiology of A. baumannii in ICUs and its associated resistance profiles are poorly understood. Our objectives were as follows: to study the clonal relationship and antibiotic resistance profiles of clinical and digestive colonizing A. baumannii isolates in an ICU, to characterize the circulating carbapenemases, and to detect 16S-RMTases. Patients admitted between August 2010 and July 2011 with a clinically predicted hospital stay > 48 hr were included. Pharyngeal and rectal swabs were obtained during the first fortnight after hospitalization. Resistance profiles were determined with MicroScan ® and VITEK2 system. Carbapenemases and 16S-RMTases were identified by PCR and sequencing, and clonality was assessed by pulsed-field gel electrophoresis and multilocus sequence typing. Sixty-nine patients were studied and 63 were diagnosed with bacterial infections. Among these, 29 were CRAB isolates; 49 A. baumannii were isolated as digestive colonizers. These 78 isolates were clustered in 7 pulsetypes, mostly belonging to ST79. The only carbapenemase genes detected were bla OXA-51 (n = 78), bla OXA-23 (n = 62), and bla OXA-58 (n = 3). Interestingly, two clinical isolates harbored the rmtC 16S-RMTase gene. To the best of our knowledge, this is the first description of the presence of rmtC in A. baumannii.

Published

2018

10. Discovery and in Vivo Evaluation of the Potent and Selective PI3Kδ Inhibitors 2-((1S)-1-((6-Amino-5-cyano-4-pyrimidinyl)amino)ethyl)-6-fluoro-N-methyl-3-(2-pyridinyl)-4-quinolinecarboxamide (AM-0687) and 2-((1S)-1-((6-Amino-5-cyano-4-pyrimidinyl)amino)ethyl)-5-fluoro-N-methyl-3-(2-pyridinyl)-4-quinolinecarboxamide (AM-1430).

Author

Gonzalez-Lopez de Turiso F, Hao X, Shin Y, Bui M, Campuzano ID, Cardozo M, Dunn MC, Duquette J, Fisher B, Foti RS, Henne K, He X, Hu YL, Kelly RC, Johnson MG, Lucas BS, McCarter J, McGee LR, Medina JC, Metz D, San Miguel T, Mohn D, Tran T, Vissinga C, Wannberg S, Whittington DA, Whoriskey J, Yu G, Zalameda L, Zhang X, and Cushing TD

Subjects

Animals, B-Lymphocytes drug effects, B-Lymphocytes immunology, Class Ia Phosphatidylinositol 3-Kinase metabolism, Dose-Response Relationship, Drug, Humans, Mice, Models, Molecular, Molecular Structure, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors chemistry, Pyridines chemical synthesis, Pyridines chemistry, Quinolines chemical synthesis, Quinolines chemistry, Structure-Activity Relationship, Drug Discovery, Phosphoinositide-3 Kinase Inhibitors, Protein Kinase Inhibitors pharmacology, Pyridines pharmacology, Quinolines pharmacology

Abstract

Optimization of the potency and pharmacokinetic profile of 2,3,4-trisubstituted quinoline, 4, led to the discovery of two potent, selective, and orally bioavailable PI3Kδ inhibitors, 6a (AM-0687) and 7 (AM-1430). On the basis of their improved profile, these analogs were selected for in vivo pharmacodynamic (PD) and efficacy experiments in animal models of inflammation. The in vivo PD studies, which were carried out in a mouse pAKT inhibition animal model, confirmed the observed potency of 6a and 7 in biochemical and cellular assays. Efficacy experiments in a keyhole limpet hemocyanin model in rats demonstrated that administration of either 6a or 7 resulted in a strong dose-dependent reduction of IgG and IgM specific antibodies. The excellent in vitro and in vivo profiles of these analogs make them suitable for further development.

Published

2016

11. 5-Alkyl-2-urea-Substituted Pyridines: Identification of Efficacious Glucokinase Activators with Improved Properties.

Author

Kohn TJ, Du X, Lai S, Xiong Y, Komorowski R, Veniant M, Fu Z, Jiao X, Pattaropong V, Chow D, Cardozo M, Jin L, Conn M, DeWolf WE Jr, Kraser CF, Hinklin RJ, Boys ML, Medina JC, Houze J, Dransfield P, and Coward P

Abstract

Two 1-(4-aryl-5-alkyl-pyridin-2-yl)-3-methylurea glucokinase activators were identified with robust in vivo efficacy. These two compounds possessed higher solubilities than the previously identified triaryl compounds (i.e., AM-2394). Structure-activity relationship studies are presented along with relevant pharmacokinetic and in vivo data.

Published

2016

12. Novel Series of Potent Glucokinase Activators Leading to the Discovery of AM-2394.

Author

Dransfield PJ, Pattaropong V, Lai S, Fu Z, Kohn TJ, Du X, Cheng A, Xiong Y, Komorowski R, Jin L, Conn M, Tien E, DeWolf WE Jr, Hinklin RJ, Aicher TD, Kraser CF, Boyd SA, Voegtli WC, Condroski KR, Veniant-Ellison M, Medina JC, Houze J, and Coward P

Abstract

Glucokinase (GK) catalyzes the phosphorylation of glucose to glucose-6-phosphate. We present the structure-activity relationships leading to the discovery of AM-2394, a structurally distinct GKA. AM-2394 activates GK with an EC50 of 60 nM, increases the affinity of GK for glucose by approximately 10-fold, exhibits moderate clearance and good oral bioavailability in multiple animal models, and lowers glucose excursion following an oral glucose tolerance test in an ob/ob mouse model of diabetes.

Published

2016

13. Discovery, Optimization, and in Vivo Evaluation of Benzimidazole Derivatives AM-8508 and AM-9635 as Potent and Selective PI3Kδ Inhibitors.

Author

Shin Y, Suchomel J, Cardozo M, Duquette J, He X, Henne K, Hu YL, Kelly RC, McCarter J, McGee LR, Medina JC, Metz D, San Miguel T, Mohn D, Tran T, Vissinga C, Wong S, Wannberg S, Whittington DA, Whoriskey J, Yu G, Zalameda L, Zhang X, and Cushing TD

Subjects

Animals, B-Lymphocytes drug effects, Crystallography, X-Ray, Hemocyanins drug effects, Humans, Immunoglobulin G drug effects, Immunoglobulin M drug effects, Mice, Models, Molecular, Rats, Structure-Activity Relationship, Benzimidazoles chemical synthesis, Benzimidazoles pharmacology, Phosphoinositide-3 Kinase Inhibitors, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors pharmacology

Abstract

Lead optimization efforts resulted in the discovery of two potent, selective, and orally bioavailable PI3Kδ inhibitors, 1 (AM-8508) and 2 (AM-9635), with good pharmacokinetic properties. The compounds inhibit B cell receptor (BCR)-mediated AKT phosphorylation (pAKT) in PI3Kδ-dependent in vitro cell based assays. These compounds which share a benzimidazole bicycle are effective when administered in vivo at unbound concentrations consistent with their in vitro cell potency as a consequence of improved unbound drug concentration with lower unbound clearance. Furthermore, the compounds demonstrated efficacy in a Keyhole Limpet Hemocyanin (KLH) study in rats, where the blockade of PI3Kδ activity by inhibitors 1 and 2 led to effective inhibition of antigen-specific IgG and IgM formation after immunization with KLH.

Published

2016

14. Discovery of the imidazole-derived GPR40 agonist AM-3189.

Author

Ma Z, Lin DC, Sharma R, Liu J, Zhu L, Li AR, Kohn T, Wang Y, Liu JJ, Bartberger MD, Medina JC, Zhuang R, Li F, Zhang J, Luo J, Wong S, Tonn GR, and Houze JB

Subjects

Animals, Dogs, Dose-Response Relationship, Drug, Humans, Imidazoles chemical synthesis, Macaca fascicularis, Mice, Molecular Structure, Rats, Structure-Activity Relationship, Drug Discovery, Imidazoles chemistry, Imidazoles pharmacology, Receptors, G-Protein-Coupled agonists

Abstract

As a follow-up to the GPR40 agonist AMG 837, which was evaluated in clinical trials for the treatment of type II diabetes, further optimization led to the discovery of AM-3189 (13k). AM-3189 is representative of a new class of compounds with minimal CNS penetration, superior pharmacokinetic properties and in vivo efficacy comparable to AMG 837., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2016

15. Synthesis and SAR study of potent and selective PI3Kδ inhibitors.

Author

Bui M, Hao X, Shin Y, Cardozo M, He X, Henne K, Suchomel J, McCarter J, McGee LR, San Miguel T, Medina JC, Mohn D, Tran T, Wannberg S, Wong J, Wong S, Zalameda L, Metz D, and Cushing TD

Subjects

Animals, Class I Phosphatidylinositol 3-Kinases metabolism, Humans, Male, Protein Isoforms antagonists & inhibitors, Protein Isoforms metabolism, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors pharmacokinetics, Quinolines chemical synthesis, Quinolines pharmacokinetics, Rats, Rats, Sprague-Dawley, Structure-Activity Relationship, Class I Phosphatidylinositol 3-Kinases antagonists & inhibitors, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacology, Quinolines chemistry, Quinolines pharmacology

Abstract

2,3,4-Substituted quinolines such as (10a) were found to be potent inhibitors of PI3Kδ in both biochemical and cellular assays with good selectivity over three other class I PI3K isoforms. Some of those analogs showed favorable pharmacokinetic properties., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

16. Discovery and in vivo evaluation of (S)-N-(1-(7-fluoro-2-(pyridin-2-yl)quinolin-3-yl)ethyl)-9H-purin-6-amine (AMG319) and related PI3Kδ inhibitors for inflammation and autoimmune disease.

Author

Cushing TD, Hao X, Shin Y, Andrews K, Brown M, Cardozo M, Chen Y, Duquette J, Fisher B, Gonzalez-Lopez de Turiso F, He X, Henne KR, Hu YL, Hungate R, Johnson MG, Kelly RC, Lucas B, McCarter JD, McGee LR, Medina JC, San Miguel T, Mohn D, Pattaropong V, Pettus LH, Reichelt A, Rzasa RM, Seganish J, Tasker AS, Wahl RC, Wannberg S, Whittington DA, Whoriskey J, Yu G, Zalameda L, Zhang D, and Metz DP

Subjects

Adenosine chemistry, Adenosine metabolism, Animals, Cells, Cultured, Class I Phosphatidylinositol 3-Kinases chemistry, Class I Phosphatidylinositol 3-Kinases metabolism, Crystallography, X-Ray, Disease Models, Animal, Drug Discovery, Female, Humans, Mice, Inbred BALB C, Mice, Transgenic, Models, Chemical, Models, Molecular, Molecular Structure, Protein Binding, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors metabolism, Protein Structure, Tertiary, Quinolines chemistry, Quinolines metabolism, Rats, Inbred Lew, Sf9 Cells, Structure-Activity Relationship, Adenosine pharmacology, Autoimmune Diseases prevention & control, Class I Phosphatidylinositol 3-Kinases antagonists & inhibitors, Inflammation prevention & control, Protein Kinase Inhibitors pharmacology, Quinolines pharmacology

Abstract

The development and optimization of a series of quinolinylpurines as potent and selective PI3Kδ kinase inhibitors with excellent physicochemical properties are described. This medicinal chemistry effort led to the identification of 1 (AMG319), a compound with an IC50 of 16 nM in a human whole blood assay (HWB), excellent selectivity over a large panel of protein kinases, and a high level of in vivo efficacy as measured by two rodent disease models of inflammation.

Published

2015

17. Discovery of AM-7209, a potent and selective 4-amidobenzoic acid inhibitor of the MDM2-p53 interaction.

Author

Rew Y, Sun D, Yan X, Beck HP, Canon J, Chen A, Duquette J, Eksterowicz J, Fox BM, Fu J, Gonzalez AZ, Houze J, Huang X, Jiang M, Jin L, Li Y, Li Z, Ling Y, Lo MC, Long AM, McGee LR, McIntosh J, Oliner JD, Osgood T, Saiki AY, Shaffer P, Wang YC, Wortman S, Yakowec P, Ye Q, Yu D, Zhao X, Zhou J, Medina JC, and Olson SH

Subjects

Animals, Antineoplastic Agents chemistry, Colonic Neoplasms metabolism, Colonic Neoplasms pathology, Female, Humans, Mice, Mice, Nude, Models, Molecular, Molecular Structure, Proto-Oncogene Proteins c-mdm2 metabolism, Structure-Activity Relationship, Tumor Cells, Cultured, Tumor Suppressor Protein p53 metabolism, Antineoplastic Agents pharmacology, Cell Proliferation drug effects, Colonic Neoplasms drug therapy, Drug Discovery, Protein Binding drug effects, Proto-Oncogene Proteins c-mdm2 antagonists & inhibitors, Tumor Suppressor Protein p53 antagonists & inhibitors

Abstract

Structure-based rational design and extensive structure-activity relationship studies led to the discovery of AMG 232 (1), a potent piperidinone inhibitor of the MDM2-p53 association, which is currently being evaluated in human clinical trials for the treatment of cancer. Further modifications of 1, including replacing the carboxylic acid with a 4-amidobenzoic acid, afforded AM-7209 (25), featuring improved potency (KD from ITC competition was 38 pM, SJSA-1 EdU IC50 = 1.6 nM), remarkable pharmacokinetic properties, and in vivo antitumor activity in both the SJSA-1 osteosarcoma xenograft model (ED50 = 2.6 mg/kg QD) and the HCT-116 colorectal carcinoma xenograft model (ED50 = 10 mg/kg QD). In addition, 25 possesses distinct mechanisms of elimination compared to 1.

Published

2014

18. C5-Alkyl-2-methylurea-Substituted Pyridines as a New Class of Glucokinase Activators.

Author

Du X, Hinklin RJ, Xiong Y, Dransfield P, Park J, Kohn TJ, Pattaropong V, Lai S, Fu Z, Jiao X, Chow D, Jin L, Davda J, Veniant MM, Anderson DA, Baer BR, Bencsik JR, Boyd SA, Chicarelli MJ, Mohr PJ, Wang B, Condroski KR, DeWolf WE, Conn M, Tran T, Yang J, Aicher TD, Medina JC, Coward P, and Houze JB

Abstract

Glucokinase (GK) activators represent a class of type 2 diabetes therapeutics actively pursued due to the central role that GK plays in regulating glucose homeostasis. Herein we report a novel C5-alkyl-2-methylurea-substituted pyridine series of GK activators derived from our previously reported thiazolylamino pyridine series. Our efforts in optimizing potency, enzyme kinetic properties, and metabolic stability led to the identification of compound 26 (AM-9514). This analogue showed a favorable combination of in vitro potency, enzyme kinetic properties, acceptable pharmacokinetic profiles in preclinical species, and robust efficacy in a rodent PD model.

Published

2014

19. Optimization beyond AMG 232: discovery and SAR of sulfonamides on a piperidinone scaffold as potent inhibitors of the MDM2-p53 protein-protein interaction.

Author

Wang Y, Zhu J, Liu JJ, Chen X, Mihalic J, Deignan J, Yu M, Sun D, Kayser F, McGee LR, Lo MC, Chen A, Zhou J, Ye Q, Huang X, Long AM, Yakowec P, Oliner JD, Olson SH, and Medina JC

Subjects

Acetates chemistry, Animals, Crystallography, X-Ray, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Models, Molecular, Molecular Conformation, Piperidones chemistry, Protein Binding drug effects, Proto-Oncogene Proteins c-mdm2 chemistry, Rats, Structure-Activity Relationship, Tumor Suppressor Protein p53 chemistry, Acetates pharmacology, Drug Discovery, Piperidones pharmacology, Proto-Oncogene Proteins c-mdm2 antagonists & inhibitors, Sulfonamides chemistry, Tumor Suppressor Protein p53 antagonists & inhibitors

Abstract

We recently reported on the discovery of AMG 232, a potent and selective piperidinone inhibitor of the MDM2-p53 interaction. AMG 232 is being evaluated in human clinical trials for cancer. Continued exploration of the N-alkyl substituent of this series, in an effort to optimize interactions with the MDM2 glycine-58 shelf region, led to the discovery of sulfonamides such as compounds 31 and 38 that have similar potency, hepatocyte stability and rat pharmacokinetic properties to AMG 232., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

20. Solving time-dependent CYP3A4 inhibition for a series of indole-phenylacetic acid dual antagonists of the PGD(2) receptors CRTH2 and DP.

Author

Johnson MG, Liu JJ, Li AR, van Lengerich B, Wang S, Medina JC, Collins TL, Danao J, Seitz L, Willee A, D'Souza W, Budelsky AL, Fan PW, and Wong SG

Subjects

Dose-Response Relationship, Drug, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Humans, Indoles chemistry, Molecular Structure, Phenylacetates chemistry, Structure-Activity Relationship, Time Factors, Cytochrome P-450 CYP3A metabolism, Enzyme Inhibitors pharmacology, Indoles pharmacology, Phenylacetates pharmacology, Receptors, Immunologic antagonists & inhibitors, Receptors, Prostaglandin antagonists & inhibitors

Abstract

Based on their structural similarity to previously described compound AMG 009, indole-phenyl acetic acids were proposed to be potent dual inhibitors of chemoattractant receptor-homologous molecule expressed on Th2 cells (CRTH2 or DP2) and prostanoid D receptor (DP or DP1). This series was equipotent to AMG 009 in binding assays against both receptors but exhibited decreased serum shift. We discovered early in the optimization of these indole-phenylacetic acid compounds that they demonstrated CYP3A4 time-dependent inhibition (TDI). Hypothesizing that the source of TDI was the indole core we modified the 1,2,3-substitution to eventually afford a highly potent modulator of CRTH2 and DP which did not exhibit TDI., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

21. Structure-assisted discovery of the first non-retinoid ligands for Retinol-Binding Protein 4.

Author

Wang Y, Connors R, Fan P, Wang X, Wang Z, Liu J, Kayser F, Medina JC, Johnstone S, Xu H, Thibault S, Walker N, Conn M, Zhang Y, Liu Q, Grillo MP, Motani A, Coward P, and Wang Z

Subjects

Animals, Crystallography, X-Ray, Dose-Response Relationship, Drug, Humans, Ligands, Male, Mice, Models, Molecular, Molecular Structure, Rats, Retinol-Binding Proteins, Plasma metabolism, Small Molecule Libraries chemical synthesis, Small Molecule Libraries chemistry, Structure-Activity Relationship, Vitamin A blood, Drug Discovery, Retinol-Binding Proteins, Plasma antagonists & inhibitors, Small Molecule Libraries pharmacology

Abstract

Retinol-Binding Protein 4 (RBP4) is a plasma protein that transports retinol (vitamin A) from the liver to peripheral tissues. This Letter highlights our efforts in discovering the first, to our knowledge, non-retinoid small molecules that bind to RBP4 at the retinol site and reduce serum RBP4 levels in mice, by disrupting the interaction between RBP4 and transthyretin (TTR), a plasma protein that binds RBP4 and protects it from renal excretion. Potent compounds were discovered and optimized quickly from high-throughput screen (HTS) hits utilizing a structure-based approach. Inhibitor co-crystal X-ray structures revealed unique disruptions of RBP4-TTR interactions by our compounds through induced loop conformational changes instead of steric hindrance exemplified by fenretinide. When administered to mice, A1120, a representative compound in the series, showed concentration-dependent retinol and RBP4 lowering., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

22. Discovery of Potent and Simplified Piperidinone-Based Inhibitors of the MDM2-p53 Interaction.

Author

Yu M, Wang Y, Zhu J, Bartberger MD, Canon J, Chen A, Chow D, Eksterowicz J, Fox B, Fu J, Gribble M, Huang X, Li Z, Liu JJ, Lo MC, McMinn D, Oliner JD, Osgood T, Rew Y, Saiki AY, Shaffer P, Yan X, Ye Q, Yu D, Zhao X, Zhou J, Olson SH, Medina JC, and Sun D

Abstract

Continued optimization of the N-substituent in the piperidinone series provided potent piperidinone-pyridine inhibitors 6, 7, 14, and 15 with improved pharmacokinetic properties in rats. Reducing structure complexity of the N-alkyl substituent led to the discovery of 23, a potent and simplified inhibitor of MDM2. Compound 23 exhibits excellent pharmacokinetic properties and substantial in vivo antitumor activity in the SJSA-1 osteosarcoma xenograft mouse model.

Published

2014

23. Discovery of AMG 925, a FLT3 and CDK4 dual kinase inhibitor with preferential affinity for the activated state of FLT3.

Author

Li Z, Wang X, Eksterowicz J, Gribble MW Jr, Alba GQ, Ayres M, Carlson TJ, Chen A, Chen X, Cho R, Connors RV, DeGraffenreid M, Deignan JT, Duquette J, Fan P, Fisher B, Fu J, Huard JN, Kaizerman J, Keegan KS, Li C, Li K, Li Y, Liang L, Liu W, Lively SE, Lo MC, Ma J, McMinn DL, Mihalic JT, Modi K, Ngo R, Pattabiraman K, Piper DE, Queva C, Ragains ML, Suchomel J, Thibault S, Walker N, Wang X, Wang Z, Wanska M, Wehn PM, Weidner MF, Zhang AJ, Zhao X, Kamb A, Wickramasinghe D, Dai K, McGee LR, and Medina JC

Subjects

Animals, Cyclin-Dependent Kinase 6 antagonists & inhibitors, Cytochrome P-450 CYP3A, Cytochrome P-450 CYP3A Inhibitors, Dogs, Drug Discovery, Heterocyclic Compounds, 3-Ring pharmacology, Humans, Macaca fascicularis, Naphthyridines pharmacology, Protein Kinase Inhibitors pharmacokinetics, Protein Kinase Inhibitors pharmacology, Rats, Structure-Activity Relationship, U937 Cells, fms-Like Tyrosine Kinase 3 genetics, Cyclin-Dependent Kinase 4 antagonists & inhibitors, Heterocyclic Compounds, 3-Ring chemical synthesis, Naphthyridines chemical synthesis, Protein Kinase Inhibitors chemical synthesis, fms-Like Tyrosine Kinase 3 antagonists & inhibitors

Abstract

We describe the structural optimization of a lead compound 1 that exhibits dual inhibitory activities against FLT3 and CDK4. A series of pyrido[4',3':4,5]pyrrolo[2,3-d]pyrimidine derivatives was synthesized, and SAR analysis, using cell-based assays, led to the discovery of 28 (AMG 925), a potent and orally bioavailable dual inhibitor of CDK4 and FLT3, including many FLT3 mutants reported to date. Compound 28 inhibits the proliferation of a panel of human tumor cell lines including Colo205 (Rb(+)) and U937 (FLT3(WT)) and induced cell death in MOLM13 (FLT3(ITD)) and even in MOLM13 (FLT3(ITD, D835Y)), which exhibits resistance to a number of FLT3 inhibitors currently under clinical development. At well-tolerated doses, compound 28 leads to significant growth inhibition of MOLM13 xenografts in nude mice, and the activity correlates with inhibition of STAT5 and Rb phosphorylation.

Published

2014

24. Novel inhibitors of the MDM2-p53 interaction featuring hydrogen bond acceptors as carboxylic acid isosteres.

Author

Gonzalez AZ, Li Z, Beck HP, Canon J, Chen A, Chow D, Duquette J, Eksterowicz J, Fox BM, Fu J, Huang X, Houze J, Jin L, Li Y, Ling Y, Lo MC, Long AM, McGee LR, McIntosh J, Oliner JD, Osgood T, Rew Y, Saiki AY, Shaffer P, Wortman S, Yakowec P, Yan X, Ye Q, Yu D, Zhao X, Zhou J, Olson SH, Sun D, and Medina JC

Subjects

Acetates chemistry, Animals, Bone Neoplasms drug therapy, Carboxylic Acids chemistry, Cells, Cultured, Crystallography, X-Ray, Drug Design, Female, Humans, Hydrogen Bonding, Mice, Mice, Nude, Models, Molecular, Molecular Structure, Osteosarcoma drug therapy, Piperidones chemistry, Protein Binding, Proto-Oncogene Proteins c-mdm2 metabolism, Stereoisomerism, Structure-Activity Relationship, Tumor Cells, Cultured, Tumor Suppressor Protein p53 metabolism, Xenograft Model Antitumor Assays, Acetates pharmacology, Antineoplastic Agents pharmacology, Carboxylic Acids pharmacology, Cell Proliferation drug effects, Myocytes, Smooth Muscle drug effects, Piperidones pharmacology, Protein Interaction Domains and Motifs drug effects, Proto-Oncogene Proteins c-mdm2 antagonists & inhibitors, Tumor Suppressor Protein p53 antagonists & inhibitors

Abstract

We previously reported the discovery of potent and selective morpholinone and piperidinone inhibitors of the MDM2-p53 interaction. These inhibitors have in common a carboxylic acid moiety that engages in an electrostatic interaction with MDM2-His96. Our continued search for potent and diverse inhibitors led to the discovery of novel replacements for these acids uncovering new interactions with the MDM2 protein. In particular, using pyridine or thiazole as isosteres of the carboxylic acid moiety resulted in very potent analogues. From these, AM-6761 (4) emerged as a potent inhibitor with remarkable biochemical (HTRF IC50 = 0.1 nM) and cellular potency (SJSA-1 EdU IC50 = 16 nM), as well as favorable pharmacokinetic properties. Compound 4 also shows excellent antitumor activity in the SJSA-1 osteosarcoma xenograft model with an ED50 of 11 mg/kg. Optimization efforts toward the discovery of these inhibitors as well as the new interactions observed with the MDM2 protein are described herein.

Published

2014

25. Selective and potent morpholinone inhibitors of the MDM2-p53 protein-protein interaction.

Author

Gonzalez AZ, Eksterowicz J, Bartberger MD, Beck HP, Canon J, Chen A, Chow D, Duquette J, Fox BM, Fu J, Huang X, Houze JB, Jin L, Li Y, Li Z, Ling Y, Lo MC, Long AM, McGee LR, McIntosh J, McMinn DL, Oliner JD, Osgood T, Rew Y, Saiki AY, Shaffer P, Wortman S, Yakowec P, Yan X, Ye Q, Yu D, Zhao X, Zhou J, Olson SH, Medina JC, and Sun D

Subjects

Animals, Cell Line, Tumor, Crystallography, X-Ray, Drug Discovery, Humans, Indicators and Reagents, Mice, Models, Molecular, Molecular Conformation, Morpholines pharmacokinetics, Rats, Structure-Activity Relationship, Xenograft Model Antitumor Assays, Acetates chemical synthesis, Acetates pharmacology, Antineoplastic Agents chemical synthesis, Antineoplastic Agents pharmacology, Morpholines chemical synthesis, Morpholines pharmacology, Proto-Oncogene Proteins c-mdm2 antagonists & inhibitors, Proto-Oncogene Proteins c-mdm2 chemistry, Tumor Suppressor Protein p53 antagonists & inhibitors, Tumor Suppressor Protein p53 chemistry

Abstract

We previously reported the discovery of AMG 232, a highly potent and selective piperidinone inhibitor of the MDM2-p53 interaction. Our continued search for potent and diverse analogues led to the discovery of novel morpholinone MDM2 inhibitors. This change to a morpholinone core has a significant impact on both potency and metabolic stability compared to the piperidinone series. Within this morpholinone series, AM-8735 emerged as an inhibitor with remarkable biochemical potency (HTRF IC50 = 0.4 nM) and cellular potency (SJSA-1 EdU IC50 = 25 nM), as well as pharmacokinetic properties. Compound 4 also shows excellent antitumor activity in the SJSA-1 osteosarcoma xenograft model with an ED50 of 41 mg/kg. Lead optimization toward the discovery of this inhibitor as well as key differences between the morpholinone and the piperidinone series will be described herein.

Published

2014

26. Discovery of AMG 232, a potent, selective, and orally bioavailable MDM2-p53 inhibitor in clinical development.

Author

Sun D, Li Z, Rew Y, Gribble M, Bartberger MD, Beck HP, Canon J, Chen A, Chen X, Chow D, Deignan J, Duquette J, Eksterowicz J, Fisher B, Fox BM, Fu J, Gonzalez AZ, Gonzalez-Lopez De Turiso F, Houze JB, Huang X, Jiang M, Jin L, Kayser F, Liu JJ, Lo MC, Long AM, Lucas B, McGee LR, McIntosh J, Mihalic J, Oliner JD, Osgood T, Peterson ML, Roveto P, Saiki AY, Shaffer P, Toteva M, Wang Y, Wang YC, Wortman S, Yakowec P, Yan X, Ye Q, Yu D, Yu M, Zhao X, Zhou J, Zhu J, Olson SH, and Medina JC

Subjects

Acetates chemistry, Administration, Oral, Antineoplastic Agents chemistry, Biological Availability, Crystallography, X-Ray, Drug Discovery, Humans, Piperidones chemistry, Protein Conformation, Acetates pharmacology, Antineoplastic Agents pharmacology, Piperidones pharmacology, Proto-Oncogene Proteins c-mdm2 antagonists & inhibitors, Tumor Suppressor Protein p53 antagonists & inhibitors

Abstract

We recently reported the discovery of AM-8553 (1), a potent and selective piperidinone inhibitor of the MDM2-p53 interaction. Continued research investigation of the N-alkyl substituent of this series, focused in particular on a previously underutilized interaction in a shallow cleft on the MDM2 surface, led to the discovery of a one-carbon tethered sulfone which gave rise to substantial improvements in biochemical and cellular potency. Further investigation produced AMG 232 (2), which is currently being evaluated in human clinical trials for the treatment of cancer. Compound 2 is an extremely potent MDM2 inhibitor (SPR KD = 0.045 nM, SJSA-1 EdU IC50 = 9.1 nM), with remarkable pharmacokinetic properties and in vivo antitumor activity in the SJSA-1 osteosarcoma xenograft model (ED50 = 9.1 mg/kg).

Published

2014

27. Discovery and optimization of 5-(2-((1-(phenylsulfonyl)-1,2,3,4-tetrahydroquinolin-7-yl)oxy)pyridin-4-yl)-1,2,4-oxadiazoles as novel gpr119 agonists.

Author

Wang Y, Yu M, Zhu J, Zhang JK, Kayser F, Medina JC, Siegler K, Conn M, Shan B, Grillo MP, Liu JJ, and Coward P

Subjects

Animals, Dose-Response Relationship, Drug, Humans, Macaca fascicularis, Molecular Structure, Oxadiazoles chemical synthesis, Oxadiazoles chemistry, Quinolines chemical synthesis, Quinolines chemistry, Rats, Structure-Activity Relationship, Drug Discovery, Oxadiazoles pharmacology, Quinolines pharmacology, Receptors, G-Protein-Coupled agonists

Abstract

We describe the discovery and optimization of 5-(2-((1-(phenylsulfonyl)-1,2,3,4-tetrahydroquinolin-7-yl)oxy)pyridin-4-yl)-1,2,4-oxadiazoles as novel agonists of GPR119. Previously described aniline 2 had suboptimal efficacy in signaling assays using cynomolgus monkey (cyno) GPR119 making evaluation of the target in preclinical models difficult. Replacement of the aniline ring with a tetrahydroquinoline ring constrained the rotation of the aniline C-N bond and gave compounds with increased efficacy on human and cyno receptors. Additional optimization led to the discovery of 10, which possesses higher free fraction in plasma and improved pharmacokinetic properties in rat and cyno compared to 2., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

28. Optimization of GPR40 Agonists for Type 2 Diabetes.

Author

Liu JJ, Wang Y, Ma Z, Schmitt M, Zhu L, Brown SP, Dransfield PJ, Sun Y, Sharma R, Guo Q, Zhuang R, Zhang J, Luo J, Tonn GR, Wong S, Swaminath G, Medina JC, Lin DC, and Houze JB

Abstract

GPR40 (FFA1 and FFAR1) has gained significant interest as a target for the treatment of type 2 diabetes. TAK-875 (1), a GPR40 agonist, lowered hemoglobin A1c (HbA1c) and lowered both postprandial and fasting blood glucose levels in type 2 diabetic patients in phase II clinical trials. We optimized phenylpropanoic acid derivatives as GPR40 agonists and identified AMG 837 (2) as a clinical candidate. Here we report our efforts in searching for structurally distinct back-ups for AMG 837. These efforts led to the identification of more polar GPR40 agonists, such as AM-4668 (10), that have improved potency, excellent pharmacokinetic properties across species, and minimum central nervous system (CNS) penetration.

Published

2014

29. Improving the Pharmacokinetics of GPR40/FFA1 Full Agonists.

Author

Du X, Dransfield PJ, Lin DC, Wong S, Wang Y, Wang Z, Kohn T, Yu M, Brown SP, Vimolratana M, Zhu L, Li AR, Su Y, Jiao X, Liu JJ, Swaminath G, Tran T, Luo J, Zhuang R, Zhang J, Guo Q, Li F, Connors R, Medina JC, and Houze JB

Abstract

We recently reported the discovery of a potent GPR40 full agonist AM-1638 (1). Herein, we describe our efforts in improving the drug-like properties of the full agonists through the systematic introduction of polar groups in the C-, D-, and A-rings. This led to the discovery of new GPR40 full agonists with significantly improved pharmacokinetic propeties. Compound 8 and 20 also showed potent in vivo efficacy in oral glucose tolerance tests in mice in addition to the improvement in properties.

Published

2014

30. Discovery and optimization of N-(3-(1,3-dioxo-2,3-dihydro-1H-pyrrolo[3,4-c]pyridin-4-yloxy)phenyl)benzenesulfonamides as novel GPR119 agonists.

Author

Yu M, Ken Zhang J, Wang Y, Zhu J, Kayser F, Medina JC, Siegler K, Conn M, Shan B, Grillo MP, Coward P, and Jim Liu J

Subjects

Animals, Dose-Response Relationship, Drug, Humans, Microsomes, Liver chemistry, Microsomes, Liver metabolism, Molecular Structure, Pyridines chemistry, Pyridines metabolism, Rats, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides metabolism, Drug Discovery, Pyridines pharmacology, Receptors, G-Protein-Coupled agonists, Sulfonamides pharmacology

Abstract

The discovery and optimization of novel N-(3-(1,3-dioxo-2,3-dihydro-1H-pyrrolo[3,4-c]pyridin-4-yloxy)phenyl)benzenesulfonamide GPR119 agonists is described. Modification of the pyridylphthalimide motif of the molecule with R(1)=-Me and R(2)=-(i)Pr substituents, incorporated with a 6-fluoro substitution on the central phenyl ring offered a potent and metabolically stable tool compound 22., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2014

31. Discovery and optimization of arylsulfonyl 3-(pyridin-2-yloxy)anilines as novel GPR119 agonists.

Author

Zhang JK, Li AR, Yu M, Wang Y, Zhu J, Kayser F, Medina JC, Siegler K, Conn M, Shan B, Grillo MP, Eksterowicz J, Coward P, and Liu JJ

Subjects

Aniline Compounds chemical synthesis, Animals, Diabetes Mellitus, Type 2 drug therapy, Drug Discovery, Humans, Mice, Models, Molecular, Receptors, G-Protein-Coupled chemistry, Structure-Activity Relationship, Aniline Compounds chemistry, Aniline Compounds pharmacology, Receptors, G-Protein-Coupled agonists

Abstract

We describe the discovery of a series of arylsulfonyl 3-(pyridin-2-yloxy)anilines as GPR119 agonists derived from compound 1. Replacement of the three methyl groups in 1 with metabolically stable moieties led to the identification of compound 34, a potent and efficacious GPR119 agonist with improved pharmacokinetic (PK) properties., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

32. Rational design and binding mode duality of MDM2-p53 inhibitors.

Author

Gonzalez-Lopez de Turiso F, Sun D, Rew Y, Bartberger MD, Beck HP, Canon J, Chen A, Chow D, Correll TL, Huang X, Julian LD, Kayser F, Lo MC, Long AM, McMinn D, Oliner JD, Osgood T, Powers JP, Saiki AY, Schneider S, Shaffer P, Xiao SH, Yakowec P, Yan X, Ye Q, Yu D, Zhao X, Zhou J, Medina JC, and Olson SH

Subjects

Animals, Circular Dichroism, Crystallography, Crystallography, X-Ray, Drug Design, Female, Humans, Indicators and Reagents, Mice, Mice, Nude, Models, Molecular, Morpholines chemical synthesis, Morpholines pharmacology, Piperidines chemical synthesis, Piperidines pharmacology, Stereoisomerism, Structure-Activity Relationship, Xenograft Model Antitumor Assays, Antineoplastic Agents chemical synthesis, Antineoplastic Agents pharmacology, Proto-Oncogene Proteins c-mdm2 antagonists & inhibitors, Tumor Suppressor Protein p53 antagonists & inhibitors

Abstract

Structural analysis of both the MDM2-p53 protein-protein interaction and several small molecules bound to MDM2 led to the design and synthesis of tetrasubstituted morpholinone 10, an MDM2 inhibitor with a biochemical IC50 of 1.0 μM. The cocrystal structure of 10 with MDM2 inspired two independent optimization strategies and resulted in the discovery of morpholinones 16 and 27 possessing distinct binding modes. Both analogues were potent MDM2 inhibitors in biochemical and cellular assays, and morpholinone 27 (IC50 = 0.10 μM) also displayed suitable PK profile for in vivo animal experiments. A pharmacodynamic (PD) experiment in mice implanted with human SJSA-1 tumors showed p21(WAF1) mRNA induction (2.7-fold over vehicle) upon oral dosing of 27 at 300 mg/kg.

Published

2013

33. Discovery and Optimization of Potent GPR40 Full Agonists Containing Tricyclic Spirocycles.

Author

Wang Y, Liu JJ, Dransfield PJ, Zhu L, Wang Z, Du X, Jiao X, Su Y, Li AR, Brown SP, Kasparian A, Vimolratana M, Yu M, Pattaropong V, Houze JB, Swaminath G, Tran T, Nguyen K, Guo Q, Zhang J, Zhuang R, Li F, Miao L, Bartberger MD, Correll TL, Chow D, Wong S, Luo J, Lin DC, and Medina JC

Abstract

GPR40 (FFAR1 or FFA1) is a target of high interest being pursued to treat type II diabetes due to its unique mechanism leading to little risk of hypoglycemia. We recently reported the discovery of AM-1638 (2), a potent full agonist of GPR40. In this report, we present the discovery of GPR40 full agonists containing conformationally constrained tricyclic spirocycles and their structure-activity relationships leading to more potent agonists such as AM-5262 (26) with improved rat PK profile and general selectivity profile. AM-5262 enhanced glucose stimulated insulin secretion (mouse and human islets) and improved glucose homeostasis in vivo (OGTT in HF/STZ mice) when compared to AM-1638.

Published

2013

34. Aminopyrazole-Phenylalanine Based GPR142 Agonists: Discovery of Tool Compound and in Vivo Efficacy Studies.

Author

Yu M, Lizarzaburu M, Motani A, Fu Z, Du X, Liu JJ, Jiao X, Lai S, Fan P, Fu A, Liu Q, Murakoshi M, Nara F, Oda K, Okuyama R, Reagan JD, Watanabe N, Yamazaki M, Xiong Y, Zhang Y, Zhuang R, Lin DC, Houze JB, Medina JC, and Li L

Abstract

Herein, we report the lead optimization of amrinone-phenylalanine based GPR142 agonists. Structure-activity relationship studies led to the discovery of aminopyrazole-phenylalanine carboxylic acid 22, which exhibited good agonistic activity, high target selectivity, desirable pharmacokinetic properties, and no cytochrome P450 or hERG liability. Compound 22, together with its orally bioavailable ethyl ester prodrug 23, were found to be suitable for in vivo proof-of-concept studies. Compound 23 displayed good efficacy in a mouse oral glucose tolerance test (OGTT). Compound 22 showed GPR142 dependent stimulation of insulin secretion in isolated mouse islets and demonstrated a statistically significant glucose lowering effect in a mouse model bearing transplanted human islets.

Published

2013

35. Phenylalanine derivatives as GPR142 agonists for the treatment of type II diabetes.

Author

Du X, Kim YJ, Lai S, Chen X, Lizarzaburu M, Turcotte S, Fu Z, Liu Q, Zhang Y, Motani A, Oda K, Okuyama R, Nara F, Murakoshi M, Fu A, Reagan JD, Fan P, Xiong Y, Shen W, Li L, Houze J, and Medina JC

Subjects

Animals, Blood Glucose analysis, Dose-Response Relationship, Drug, Drug Stability, Glucose Tolerance Test, HEK293 Cells, Humans, Hypoglycemic Agents administration & dosage, Hypoglycemic Agents chemistry, Insulin blood, Insulin metabolism, Insulin Secretion, Male, Mice, Mice, Inbred Strains, Microsomes chemistry, Phenylalanine administration & dosage, Phenylalanine chemistry, Rats, Receptors, G-Protein-Coupled metabolism, Structure-Activity Relationship, Diabetes Mellitus, Type 2 drug therapy, Hypoglycemic Agents pharmacology, Phenylalanine pharmacology, Receptors, G-Protein-Coupled agonists

Abstract

GPR142 is a novel GPCR that is predominantly expressed in pancreatic β-cells. GPR142 agonists potentiate glucose-dependent insulin secretion, and therefore can reduce the risk of hypoglycemia. Optimization of our lead pyridinone-phenylalanine series led to a proof-of-concept compound 22, which showed in vivo efficacy in mice with dose-dependent increase in insulin secretion and a decrease in glucose levels., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

36. Discovery and optimization of a novel series of GPR142 agonists for the treatment of type 2 diabetes mellitus.

Author

Lizarzaburu M, Turcotte S, Du X, Duquette J, Fu A, Houze J, Li L, Liu J, Murakoshi M, Oda K, Okuyama R, Nara F, Reagan J, Yu M, and Medina JC

Subjects

Animals, Dose-Response Relationship, Drug, Humans, Hypoglycemic Agents chemical synthesis, Hypoglycemic Agents chemistry, Microsomes, Liver chemistry, Microsomes, Liver metabolism, Molecular Structure, Phenylalanine chemical synthesis, Phenylalanine chemistry, Rats, Structure-Activity Relationship, Diabetes Mellitus, Type 2 drug therapy, Drug Discovery, Hypoglycemic Agents pharmacology, Phenylalanine pharmacology, Receptors, G-Protein-Coupled agonists

Abstract

The discovery and initial optimization of a series of phenylalanine based agonists for GPR142 is described. The structure-activity-relationship around the major areas of the molecule was explored to give agonists 90 times more potent than the initial HTS hit in a human GPR142 inositol phosphate accumulation assay. Removal of CYP inhibition by exploration of the pyridine A-ring is also described., (Copyright © 2012. Published by Elsevier Ltd.)

Published

2012

37. Discovery and in vivo evaluation of dual PI3Kβ/δ inhibitors.

Author

Gonzalez-Lopez de Turiso F, Shin Y, Brown M, Cardozo M, Chen Y, Fong D, Hao X, He X, Henne K, Hu YL, Johnson MG, Kohn T, Lohman J, McBride HJ, McGee LR, Medina JC, Metz D, Miner K, Mohn D, Pattaropong V, Seganish J, Simard JL, Wannberg S, Whittington DA, Yu G, and Cushing TD

Subjects

Models, Molecular, Drug Discovery, Drug Evaluation, Preclinical, Phosphoinositide-3 Kinase Inhibitors, Protein Kinase Inhibitors pharmacology

Abstract

Structure-based rational design led to the synthesis of a novel series of potent PI3K inhibitors. The optimized pyrrolopyridine analogue 63 was a potent and selective PI3Kβ/δ dual inhibitor that displayed suitable physicochemical properties and pharmacokinetic profile for animal studies. Analogue 63 was found to be efficacious in animal models of inflammation including a keyhole limpet hemocyanin (KLH) study and a collagen-induced arthritis (CIA) disease model of rheumatoid arthritis. These studies highlight the potential therapeutic value of inhibiting both the PI3Kβ and δ isoforms in the treatment of a number of inflammatory diseases.

Published

2012

38. Discovery of AM-1638: A Potent and Orally Bioavailable GPR40/FFA1 Full Agonist.

Author

Brown SP, Dransfield PJ, Vimolratana M, Jiao X, Zhu L, Pattaropong V, Sun Y, Liu J, Luo J, Zhang J, Wong S, Zhuang R, Guo Q, Li F, Medina JC, Swaminath G, Lin DC, and Houze JB

Abstract

GPR40 (FFA1) is a G-protein-coupled receptor, primarily expressed in pancreatic islets, the activation of which elicits increased insulin secretion only in the presence of elevated glucose levels. A potent, orally bioavailable small molecule GPR40 agonist is hypothesized to be an effective antidiabetic posing little or no risk of hypoglycemia. We recently reported the discovery of AMG 837 (1), a potent partial agonist of GPR40. Herein, we present the optimization from the GPR40 partial agonist 1 to the structurally and pharmacologically distinct GPR40 full agonist AM-1638 (21). Moreover, we demonstrate the improved in vivo efficacy that GPR40 full agonist 21 exhibits in BDF/DIO mice as compared to partial agonist 1.

Published

2012

39. An expeditious synthesis of the MDM2-p53 inhibitor AM-8553.

Author

Lucas BS, Fisher B, McGee LR, Olson SH, Medina JC, and Cheung E

Subjects

Acetates chemistry, Amino Alcohols chemical synthesis, Amino Alcohols chemistry, Antineoplastic Agents chemistry, Cyclization, Humans, Lactones chemical synthesis, Lactones chemistry, Models, Molecular, Oxazoles chemical synthesis, Oxazoles chemistry, Piperidones chemistry, Stereoisomerism, Acetates chemical synthesis, Antineoplastic Agents chemical synthesis, Piperidones chemical synthesis, Proto-Oncogene Proteins c-mdm2 antagonists & inhibitors, Tumor Suppressor Protein p53 antagonists & inhibitors

Abstract

The development of the structurally complex MDM2/p53 inhibitor AM-8553 was impeded by the low yield of the initial synthesis. A second generation synthesis is described that features a Noyori dynamic kinetic resolution, a highly diastereoselective allylation, and a novel oxazoline-assisted piperidinone forming reaction to provide AM-8553 in 35.6% yield and 11 steps.

Published

2012

40. Structure-based design of novel inhibitors of the MDM2-p53 interaction.

Author

Rew Y, Sun D, Gonzalez-Lopez De Turiso F, Bartberger MD, Beck HP, Canon J, Chen A, Chow D, Deignan J, Fox BM, Gustin D, Huang X, Jiang M, Jiao X, Jin L, Kayser F, Kopecky DJ, Li Y, Lo MC, Long AM, Michelsen K, Oliner JD, Osgood T, Ragains M, Saiki AY, Schneider S, Toteva M, Yakowec P, Yan X, Ye Q, Yu D, Zhao X, Zhou J, Medina JC, and Olson SH

Subjects

Acetates pharmacokinetics, Acetates pharmacology, Animals, Antineoplastic Agents pharmacokinetics, Antineoplastic Agents pharmacology, Cell Line, Tumor, Cell Proliferation drug effects, Crystallography, X-Ray, Drug Screening Assays, Antitumor, Hepatocytes metabolism, Humans, Macaca fascicularis, Mice, Mice, Nude, Models, Molecular, Molecular Conformation, Neoplasm Transplantation, Piperidones pharmacokinetics, Piperidones pharmacology, Protein Binding, Rats, Stereoisomerism, Structure-Activity Relationship, Transplantation, Heterologous, rho GTP-Binding Proteins biosynthesis, Acetates chemical synthesis, Antineoplastic Agents chemical synthesis, Piperidones chemical synthesis, Proto-Oncogene Proteins c-mdm2 metabolism, Tumor Suppressor Protein p53 metabolism

Abstract

Structure-based rational design led to the discovery of novel inhibitors of the MDM2-p53 protein-protein interaction. The affinity of these compounds for MDM2 was improved through conformational control of both the piperidinone ring and the appended N-alkyl substituent. Optimization afforded 29 (AM-8553), a potent and selective MDM2 inhibitor with excellent pharmacokinetic properties and in vivo efficacy.

Published

2012

41. Optimization of phenylacetic acid derivatives for balanced CRTH2 and DP dual antagonists.

Author

Liu JJ, Wang Y, Johnson MG, Li AR, Shen W, Wang X, Su Y, Brown M, Van Lengerich B, Rickel E, Martin T, Budelsky A, Seitz L, Danao J, Tang HL, Collins T, and Medina JC

Subjects

HEK293 Cells, Humans, Inhibitory Concentration 50, Molecular Structure, Phenylacetates chemistry, Phenylacetates pharmacology, Protein Binding drug effects, Drug Design, Phenylacetates chemical synthesis, Receptors, Immunologic antagonists & inhibitors, Receptors, Prostaglandin antagonists & inhibitors

Abstract

Our first generation CRTH2 and DP dual antagonists, represented by AMG 009, are more potent toward the CRTH2 receptor than to the DP receptor. Here we report our efforts in the discovery of CRTH2 and DP dual antagonists with more balanced potencies to both receptors, such as compound 15., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2012

42. AMG 837: a potent, orally bioavailable GPR40 agonist.

Author

Houze JB, Zhu L, Sun Y, Akerman M, Qiu W, Zhang AJ, Sharma R, Schmitt M, Wang Y, Liu J, Liu J, Medina JC, Reagan JD, Luo J, Tonn G, Zhang J, Lu JY, Chen M, Lopez E, Nguyen K, Yang L, Tang L, Tian H, Shuttleworth SJ, and Lin DC

Subjects

Administration, Oral, Animals, Biological Availability, Biphenyl Compounds administration & dosage, Biphenyl Compounds chemistry, Dose-Response Relationship, Drug, Mice, Mice, Knockout, Molecular Structure, Receptors, G-Protein-Coupled deficiency, Receptors, G-Protein-Coupled metabolism, Stereoisomerism, Structure-Activity Relationship, Biphenyl Compounds pharmacology, Receptors, G-Protein-Coupled agonists

Abstract

The discovery that certain long chain fatty acids potentiate glucose stimulated insulin secretion through the previously orphan receptor GPR40 sparked interest in GPR40 agonists as potential antidiabetic agents. Optimization of a series of β-substituted phenylpropanoic acids led to the identification of (S)-3-(4-((4'-(trifluoromethyl)biphenyl-3-yl)methoxy)phenyl)hex-4-ynoic acid (AMG 837) as a potent GPR40 agonist with a superior pharmacokinetic profile and robust glucose-dependent stimulation of insulin secretion in rodents., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2012

43. Optimization of phenylacetic acid derivatives for CRTH2 and DP selective antagonism.

Author

Wang Y, Fu Z, Schmitt M, Wang X, Shen W, Rickel E, Martin T, Budelsky A, Marshall D, Collins T, Tang HL, Medina JC, and Liu JJ

Subjects

Asthma therapy, Chemistry, Pharmaceutical methods, Drug Design, Humans, Hypersensitivity drug therapy, Inhibitory Concentration 50, Kinetics, Models, Chemical, Phenylacetates chemistry, Phenylacetates pharmacology, Prostaglandin D2 metabolism, Receptors, G-Protein-Coupled metabolism, Sulfonamides chemistry, Sulfonamides pharmacology, Receptors, Immunologic antagonists & inhibitors, Receptors, Prostaglandin antagonists & inhibitors

Abstract

We have previously reported that optimization of a series of phenylacetic acid derivatives led to the discovery of CRTH2 and DP dual antagonists, such as AMG 009 and AMG 853. During the optimization process, we discovered that minor structural modifications also afforded potent and selective CRTH2 or DP antagonists. Here we report the structure-activity relationship that led to the discovery of selective CRTH2 antagonists such as 2 and 17, and selective DP antagonists, such as 4 and 5., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2012

44. Discovery of potent and specific CXCR3 antagonists.

Author

Chen X, Mihalic J, Deignan J, Gustin DJ, Duquette J, Du X, Chan J, Fu Z, Johnson M, Li AR, Henne K, Sullivan T, Lemon B, Ma J, Miao S, Tonn G, Collins T, and Medina JC

Subjects

Animals, Bleomycin toxicity, Chromosome Aberrations, Cytochrome P-450 CYP3A, Cytochrome P-450 CYP3A Inhibitors, Dogs, Dose-Response Relationship, Drug, Drug Design, Humans, Inflammation, Inhibitory Concentration 50, Leukocytes drug effects, Macaca fascicularis, Mice, Models, Chemical, Quinazolines pharmacology, Quinazolinones pharmacology, Time Factors, Quinazolines chemical synthesis, Quinazolinones chemical synthesis, Receptors, CXCR3 antagonists & inhibitors

Abstract

The optimization of a series of 8-aza-quinazolinone analogs for antagonist activity against the CXCR3 receptor is reported. Compounds were optimized to avoid the formation of active metabolites and time-dependent-inhibitors of CYP3A4. In addition, antagonists showed potent against CXCR3 activity in whole blood and optimized to avoid activity in the chromosomal aberration assay. Compound 25 was identified as having the optimal balance of CXCR3 activity and pharmacokinetic properties across multiple pre-clinical species, which are reported herein., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2012

45. Optimization of triazoles as novel and potent nonphlorizin SGLT2 inhibitors.

Author

Du X, Lizarzaburu M, Turcotte S, Lee T, Greenberg J, Shan B, Fan P, Ling Y, Medina JC, and Houze J

Subjects

Drug Stability, Molecular Structure, Phlorhizin chemistry, Solubility, Structure-Activity Relationship, Triazoles chemistry, Triazoles chemical synthesis

Abstract

Previous efforts have led to the identification of a potent, selective, and nonphlorizin based SGLT2 inhibitor 1. This Letter describes efforts to further optimize the potency, microsomal stability, solubility and pharmacokinetic properties of this series of SGLT2 inhibitors. From these efforts, compounds 28 and 32 have improved solubility and pharmacokinetic properties compared to compound 1., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

46. Benzodiazepinone Derivatives as CRTH2 Antagonists.

Author

Liu JJ, Cheng AC, Tang HL, and Medina JC

Abstract

Multiple CRTH2 antagonists are currently evaluated in human clinical trials for asthma and chronic obstructive pulmonary disease (COPD). During our lead optimization for CRTH2 antagonists, an observation of an intramolecular hydrogen bond in ortho-phenylsulfonamido benzophenone derivatives led to the design and synthesis of conformationally constrained benzodiazepinones as potent CRTH2 antagonists. The benzodiazepinones are 2 orders of magnitude more potent than the original flexible bisaryl ethers in our binding assay. Selected benzodiazepinones, such as compound 6, were also potent in the human eosinophil shape change assay. Analysis of the rigid conformations of these benzodiazepinones and ortho-phenylsulfonamido benzophenones provided an explanation for the structure-activity relationship and revealed the possible bound conformations to CRTH2, which may be useful for building a pharmacophore model of CRTH2 antagonists.

Published

2011

47. Discovery of AMG 853, a CRTH2 and DP Dual Antagonist.

Author

Liu J, Li AR, Wang Y, Johnson MG, Su Y, Shen W, Wang X, Lively S, Brown M, Lai S, Gonzalez Lopez De Turiso F, Xu Q, Van Lengerich B, Schmitt M, Fu Z, Sun Y, Lawlis S, Seitz L, Danao J, Wait J, Ye Q, Tang HL, Grillo M, Collins TL, Sullivan TJ, and Medina JC

Abstract

Prostaglandin D2 (PGD2) plays a key role in mediating allergic reactions seen in asthma, allergic rhinitis, and atopic dermatitis. PGD2 exerts its activity through two G protein-coupled receptors (GPCRs), prostanoid D receptor (DP or DP1), and chemoattractant receptor-homologous molecule expressed on Th2 cells (CRTH2 or DP2). We report the optimization of a series of phenylacetic acid derivatives in an effort to improve the dual activity of AMG 009 against DP and CRTH2. These efforts led to the discovery of AMG 853 (2-(4-(4-(tert-butylcarbamoyl)-2-(2-chloro-4-cyclopropylphenyl sulfonamido)phenoxy)-5-chloro-2-fluorophenyl)acetic acid), which is being evaluated in human clinical trials for asthma.

Published

2011

48. Identification of piperazine-bisamide GHSR antagonists for the treatment of obesity.

Author

Yu M, Lizarzaburu M, Beckmann H, Connors R, Dai K, Haller K, Li C, Liang L, Lindstrom M, Ma J, Motani A, Wanska M, Zhang A, Li L, and Medina JC

Subjects

Amides chemical synthesis, Amides therapeutic use, Animals, Anti-Obesity Agents chemical synthesis, Anti-Obesity Agents therapeutic use, High-Throughput Screening Assays, Humans, Indoles chemical synthesis, Indoles therapeutic use, Obesity drug therapy, Piperazines chemical synthesis, Piperazines therapeutic use, Rats, Receptors, Ghrelin metabolism, Structure-Activity Relationship, Amides chemistry, Anti-Obesity Agents chemistry, Indoles chemistry, Piperazines chemistry, Receptors, Ghrelin antagonists & inhibitors

Abstract

Piperazine-bisamide analogs were discovered as partial agonists of human growth hormone secretagogue receptor (GHSR) in a high throughput screen. The partial agonists were optimized for potency and converted into antagonists through structure-activity relationship (SAR) studies. The efforts also led to the identification of potent antagonist with favorable PK profile suitable as a tool compound for in vivo studies., (Copyright 2010 Elsevier Ltd. All rights reserved.)

Published

2010

49. Antagonism of chemokine receptor CXCR3 inhibits osteosarcoma metastasis to lungs.

Author

Pradelli E, Karimdjee-Soilihi B, Michiels JF, Ricci JE, Millet MA, Vandenbos F, Sullivan TJ, Collins TL, Johnson MG, Medina JC, Kleinerman ES, Schmid-Alliana A, and Schmid-Antomarchi H

Subjects

Acetamides pharmacology, Animals, Apoptosis, Blotting, Western, Calcium metabolism, Caspases metabolism, Cell Movement, Female, Humans, Lung Neoplasms metabolism, Lung Neoplasms secondary, Mice, Mice, Inbred BALB C, Mice, Nude, Neoplasm Invasiveness, Osteosarcoma metabolism, Osteosarcoma pathology, Pyrimidinones pharmacology, Receptors, CXCR3 genetics, Receptors, CXCR3 metabolism, Signal Transduction, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Lung Neoplasms prevention & control, Osteosarcoma prevention & control, Receptors, CXCR3 antagonists & inhibitors

Abstract

Metastasis continues to be the leading cause of mortality for patients with cancer. Several years ago, it became clear that chemokines and their receptors could control the tumor progress. CXCR3 has now been identified in many cancers including osteosarcoma and CXCR3 ligands were expressed by lungs that are the primary sites to which this tumor metastasize. This study tested the hypothesis that disruption of the CXCR3/CXCR3 ligands complexes could lead to a decrease in lungs metastasis. The experimental design involved the use of the CXCR3 antagonist, AMG487 and 2 murine models of osteosarcoma lung metastases. After tail vein injection of osteosarcoma cells, mice that were systematically treated with AMG487 according to preventive or curative protocols had a significant reduction in metastatic disease. Treatment of osteosarcoma cells in vitro with AMG487 led to decreased migration, decreased matrix metalloproteinase activity, decreased proliferation/survival and increased caspase-independent death. Taken together, our results support the hypothesis that CXCR3 and their ligands intervene in the initial dissemination of the osteosarcoma cells to the lungs and stimulate the growth and expansion of the metastatic foci in later stages. Moreover, these studies indicate that targeting CXCR3 may specifically inhibit tumor metastasis without adversely affecting antitumoral host response.

Published

2009

50. Imidazo-pyrazine derivatives as potent CXCR3 antagonists.

Author

Du X, Gustin DJ, Chen X, Duquette J, McGee LR, Wang Z, Ebsworth K, Henne K, Lemon B, Ma J, Miao S, Sabalan E, Sullivan TJ, Tonn G, Collins TL, and Medina JC

Subjects

Animals, Anti-Inflammatory Agents chemical synthesis, Anti-Inflammatory Agents pharmacokinetics, Benzeneacetamides chemical synthesis, Benzeneacetamides pharmacokinetics, Cyclic S-Oxides chemical synthesis, Cyclic S-Oxides pharmacokinetics, Humans, Imidazoles chemical synthesis, Imidazoles pharmacokinetics, Mice, Molecular Conformation, Pyrazines chemical synthesis, Pyrazines pharmacokinetics, Rats, Receptors, CXCR3 metabolism, Anti-Inflammatory Agents chemistry, Benzeneacetamides chemistry, Cyclic S-Oxides chemistry, Imidazoles chemistry, Pyrazines chemistry, Receptors, CXCR3 antagonists & inhibitors

Abstract

A general way of improving the potency of CXCR3 antagonists with fused hetero-bicyclic cores was identified. Optimization efforts led to the discovery of a series of imidazo-pyrazine derivatives with improved pharmacokinetic properties in addition to increased potency. The efficacy of the lead compound 21 is evaluated in a mouse lung inflammation model.

Published

2009