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44 results on '"Chandrasena, Gamini"'

2. P2X7 receptor‐mediated release of microglial prostanoids and miRNAs correlates with reversal of neuropathic hypersensitivity in rats

Author

Staal, Roland, primary, Khayrullina, Tanzilya, additional, Christensen, Rie, additional, Hestehave, Sara, additional, Zhou, Hua, additional, Cajina, Manuel, additional, Nattini, Megan E., additional, Gandhi, Adarsh, additional, Fallon, Shaun M., additional, Schmidt, Megan, additional, Zorn, Stevin H., additional, Brodbeck, Robbin M., additional, Chandrasena, Gamini, additional, Segerdahl, Märta, additional, Breysse, Nathalie, additional, Hopper, Allen T., additional, Möller, Thomas, additional, and Munro, Gordon, additional

Published
2022
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3. Synthesis and Characterization of the Novel Rodent-Active and CNS-Penetrant P2X7 Receptor Antagonist Lu AF27139

Author

Hopper, Allen T., primary, Juhl, Martin, additional, Hornberg, Jorrit, additional, Badolo, Lassina, additional, Kilburn, John Paul, additional, Thougaard, Annemette, additional, Smagin, Gennady, additional, Song, Dekun, additional, Calice, Londye, additional, Menon, Veena, additional, Dale, Elena, additional, Zhang, Hong, additional, Cajina, Manuel, additional, Nattini, Megan E., additional, Gandhi, Adarsh, additional, Grenon, Michel, additional, Jones, Ken, additional, Khayrullina, Tanzilya, additional, Chandrasena, Gamini, additional, Thomsen, Christian, additional, Zorn, Stevin H., additional, Brodbeck, Robb, additional, Poda, Suresh Babu, additional, Staal, Roland, additional, and Möller, Thomas, additional

Published
2021
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6. Inhibition of the potassium channel K Ca 3.1 by senicapoc reverses tactile allodynia in rats with peripheral nerve injury

Author

Staal, Roland G.W., primary, Khayrullina, Tanzilya, additional, Zhang, Hong, additional, Davis, Scott, additional, Fallon, Shaun M., additional, Cajina, Manuel, additional, Nattini, Megan E., additional, Hu, Andrew, additional, Zhou, Hua, additional, Poda, Suresh Babu, additional, Zorn, Stevin, additional, Chandrasena, Gamini, additional, Dale, Elena, additional, Cambpell, Brian, additional, Biilmann Rønn, Lars Christian, additional, Munro, Gordon, additional, and Mӧller, Thomas, additional

Published
2017
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20. Identification and optimization of a novel series of [2.2.1]-oxabicyclo imide-based androgen receptor antagonists

Author

Salvati, Mark E., Balog, Aaron, Shan, Weifang, Rampulla, Richard, Giese, Soren, Mitt, Tom, Furch, Joseph A., Vite, Gregory D., Attar, Ricardo M., Jure-Kunkel, Maria, Geng, Jieping, Rizzo, Cheryl A., Gottardis, Marco M., Krystek, Stanley R., Gougoutas, Jack, Galella, Michael A., Obermeier, Mary, Fura, Aberra, and Chandrasena, Gamini

Published
2008
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22. 5-(2′-Pyridyl)-2-aminothiazoles: Alkyl amino sulfonamides and sulfamides as potent NPY5 antagonists

Author

Packiarajan, Mathivanan, primary, Coate, Heather, additional, Desai, Mahesh, additional, Jimenez, Hermogenes N., additional, Reinhard, Emily J., additional, Jubian, Vrej J., additional, Marzabadi, Mohammad R., additional, Chandrasena, Gamini, additional, Wolinski, Toni C., additional, Walker, Mary W., additional, and Andersen, Kim, additional

Published
2011
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23. Discovery of tertiary aminoacids as dual PPARα/γ agonists-I

Author

Devasthale, Pratik V., Chen, Sean, Jeon, Yoon, Qu, Fucheng, Ryono, Denis E., Wang, Wei, Zhang, Hao, Cheng, Lin, Farrelly, Dennis, Golla, Rajasree, Grover, Gary, Ma, Zhengping, Moore, Lisa, Seethala, Ramakrishna, Sun, Wei, Doweyko, Arthur M., Chandrasena, Gamini, Sleph, Paul, Hariharan, Narayanan, and Cheng, Peter T.W.

Published
2007
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24. The Novel Neuropeptide Y Y5 Receptor Antagonist Lu AA33810 [N-[[trans-4-[(4,5-Dihydro[1]benzothiepino[5,4-d]thiazol-2-yl)amino]cyclohexyl]methyl]-methanesulfonamide] Exerts Anxiolytic- and Antidepressant-Like Effects in Rat Models of Stress Sensitivity

Author

Walker, Mary W., primary, Wolinsky, Toni D., additional, Jubian, Vrej, additional, Chandrasena, Gamini, additional, Zhong, Huailing, additional, Huang, Xinyan, additional, Miller, Silke, additional, Hegde, Laxminarayan G., additional, Marsteller, Douglas A., additional, Marzabadi, Mohammad R., additional, Papp, Mariusz, additional, Overstreet, David H., additional, Gerald, Christophe P. G., additional, and Craig, Douglas A., additional

Published
2008
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25. Comparative Metabolism of Radiolabeled Muraglitazar in Animals and Humans by Quantitative and Qualitative Metabolite Profiling

Author

Zhang, Donglu, primary, Wang, Lifei, additional, Raghavan, Nirmala, additional, Zhang, Haiying, additional, Li, Wenying, additional, Cheng, Peter T., additional, Yao, Ming, additional, Zhang, Litao, additional, Zhu, Mingshe, additional, Bonacorsi, Samuel, additional, Yeola, Suresh, additional, Mitroka, James, additional, Hariharan, Narayanan, additional, Hosagrahara, Vinayak, additional, Chandrasena, Gamini, additional, Shyu, Wen Chyi, additional, and Humphreys, W. Griffith, additional

Published
2006
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27. Synthesis and biological activity of 5-aryl-4-(4-(5-methyl-1H-imidazol-4-yl)piperidin-1-yl)pyrimidine analogs as potent, highly selective, and orally bioavailable NHE-1 inhibitors

Author

Atwal, Karnail S., primary, O’Neil, Steven V., additional, Ahmad, Saleem, additional, Doweyko, Lidia, additional, Kirby, Mark, additional, Dorso, Charles R., additional, Chandrasena, Gamini, additional, Chen, Bang-Chi, additional, Zhao, Rulin, additional, and Zahler, Robert, additional

Published
2006
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28. 3-Arylimino-2-indolones Are Potent and Selective Galanin GAL3 Receptor Antagonists

Author

Konkel, Michael J., primary, Lagu, Bharat, additional, Boteju, Lakmal W., additional, Jimenez, Hermogenes, additional, Noble, Stewart, additional, Walker, Mary W., additional, Chandrasena, Gamini, additional, Blackburn, Thomas P., additional, Nikam, Sham S., additional, Wright, Jon L., additional, Kornberg, Brian E., additional, Gregory, Tracy, additional, Pugsley, Thomas A., additional, Akunne, Hyacinth, additional, Zoski, Kim, additional, and Wise, Lawrence D., additional

Published
2006
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30. Design and Synthesis of N-[(4-Methoxyphenoxy)carbonyl]-N-[[4-[2-(5- methyl-2-phenyl-4-oxazolyl)ethoxy]phenyl]methyl]glycine [Muraglitazar/BMS-298585], a Novel Peroxisome Proliferator-Activated Receptor α/γ Dual Agonist with Efficacious Glucose and Lipid-Lowering Activities

Author

Devasthale, Pratik V., primary, Chen, Sean, additional, Jeon, Yoon, additional, Qu, Fucheng, additional, Shao, Chunning, additional, Wang, Wei, additional, Zhang, Hao, additional, Cap, Michael, additional, Farrelly, Dennis, additional, Golla, Rajasree, additional, Grover, Gary, additional, Harrity, Thomas, additional, Ma, Zhengping, additional, Moore, Lisa, additional, Ren, Jimmy, additional, Seethala, Ramakrishna, additional, Cheng, Lin, additional, Sleph, Paul, additional, Sun, Wei, additional, Tieman, Aaron, additional, Wetterau, John R., additional, Doweyko, Arthur, additional, Chandrasena, Gamini, additional, Chang, Shu Y., additional, Humphreys, W. Griffith, additional, Sasseville, Vito G., additional, Biller, Scott A., additional, Ryono, Denis E., additional, Selan, Fred, additional, Hariharan, Narayanan, additional, and Cheng, Peter T. W., additional

Published
2004
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31. Aminoimidazoles as bioisosteres of acylguanidines: novel, potent, selective and orally bioavailable inhibitors of the sodium hydrogen exchanger isoform-1

Author

Ahmad, Saleem, primary, Ngu, Khehyong, additional, Combs, Donald W, additional, Wu, Shung C, additional, Weinstein, David S, additional, Liu, Wen, additional, Chen, Bang-Chi, additional, Chandrasena, Gamini, additional, Dorso, Charles R, additional, Kirby, Mark, additional, and Atwal, Karnail S, additional

Published
2004
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32. Lack of Exposure in a First-in-Man Study Due to Aldehyde Oxidase Metabolism: Investigated by Use of 14C-microdose, Humanized Mice, Monkey Pharmacokinetics, and In Vitro Methods

Author

Jensen, Klaus Gjervig, Jacobsen, Anne-Marie, Bundgaard, Christoffer, Nilausen, Dorrit Østergaard, Thale, Zia, Chandrasena, Gamini, and Jørgensen, Martin

Abstract

Inclusion of a microdose of 14C-labeled drug in the first-in-man study of new investigational drugs and subsequent analysis by accelerator mass spectrometry has become an integrated part of drug development at Lundbeck. It has been found to be highly informative with regard to investigations of the routes and rates of excretion of the drug and the human metabolite profiles according to metabolites in safety testing guidance and also when additional metabolism-related issues needed to be addressed. In the first-in-man study with the NCE Lu AF09535, contrary to anticipated, surprisingly low exposure was observed when measuring the parent compound using conventional bioanalysis. Parallel accelerator mass spectrometry analysis revealed that the low exposure was almost exclusively attributable to extensive metabolism. The metabolism observed in humans was mediated via a human specific metabolic pathway, whereas an equivalent extent of metabolism was not observed in preclinical species. In vitro, incubation studies in human liver cytosol revealed involvement of aldehyde oxidase (AO) in the biotransformation of Lu AF09535. In vivo, substantially lower plasma exposure of Lu AF09535 was observed in chimeric mice with humanized livers compared with control animals. In addition, Lu AF09535 exhibited very low oral bioavailability in monkeys despite relatively low clearance after intravenous administration in contrast to the pharmacokinetics in rats and dogs, both showing low clearance and high bioavailability. The in vitro and in vivo methods applied were proved useful for identifying and evaluating AO-dependent metabolism. Different strategies to integrate these methods for prediction of in vivo human clearance of AO substrates were evaluated.

Published
2017
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35. The Novel Neuropeptide Y Y5Receptor Antagonist Lu AA33810 [N-[[trans-4-[(4,5-Dihydro[1]benzothiepino[5,4-d]thiazol-2-yl)amino]cyclohexyl]methyl]-methanesulfonamide] Exerts Anxiolytic- and Antidepressant-Like Effects in Rat Models of Stress Sensitivity

Author

Walker, Mary W., Wolinsky, Toni D., Jubian, Vrej, Chandrasena, Gamini, Zhong, Huailing, Huang, Xinyan, Miller, Silke, Hegde, Laxminarayan G., Marsteller, Douglas A., Marzabadi, Mohammad R., Papp, Mariusz, Overstreet, David H., Gerald, Christophe P.G., and Craig, Douglas A.

Abstract

Neuropeptide Y (NPY) regulates physiological processes via receptor subtypes (Y1, Y2, Y4, Y5, and y6). The Y5receptor is well known for its role in appetite. Based on expression in the limbic system, we hypothesized that the Y5receptor might also modulate stress sensitivity. We identified a novel Y5receptor-selective antagonist, Lu AA33810 [N-[[trans-4-[(4,5-dihydro[1]-benzothiepino[5,4-d]thiazol-2-yl)amino]cyclohexyl]methyl]-methanesulfonamide], that bound to cloned rat Y5receptors (Ki= 1.5 nM) and antagonized NPY-evoked cAMP and calcium mobilization in vitro. Lu AA33810 (3-30 mg/kg p.o.) blocked feeding elicited by intracerebroventricular injection of the Y5receptor-selective agonist [cPP1-7,NPY19-23,Ala31,Aib32,Gln34]-hPancreatic Polypeptide in Sprague-Dawley rats. In vivo effects of Lu AA33810 were correlated with brain exposure ≥ 50 ng/g and ex vivo Y5receptor occupancy of 22 to 95%. Lu AA33810 was subsequently evaluated in models of stress sensitivity. In Fischer 344 rats, Lu AA33810 (30 mg/kg p.o.) attenuated increases in plasma ACTH and corticosterone elicited by intracerebroventricular injection of [cPP1-7,NPY19-23,Ala31,Aib32,Gln34]-hPancreatic Polypeptide. In Sprague-Dawley rats subjected to the social interaction test, Lu AA33810 (3-30 mg/kg p.o.) produced anxiolytic-like effects after acute or chronic treatment. In Flinders sensitive line rats, chronic dosing of Lu AA33810 (10 mg/kg/day i.p.) produced anxiolytic-like effects in the social interaction test, plus antidepressant-like effects in the forced swim test. In Wistar rats exposed to chronic mild stress, chronic dosing of Lu AA33810 (3 and 10 mg/kg/day i.p.) produced antidepressant-like activity, i.e., normalization of stress-induced decrease in sucrose consumption. We propose that Y5receptors may function as part of an endogenous stress-sensing system to mediate social anxiety and reward or motivational deficits in selected rodent models.

Published
2009
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36. The novel neuropeptide Y Y5 receptor antagonist Lu AA33810 [N-[[trans-4-[(4,5-dihydro[1]benzothiepino[5,4-d]thiazol-2-yl)amino]cyclohexyl]methyl]-methanesulfonamide] exerts anxiolytic- and antidepressant-like effects in rat models of stress sensitivity.

Author

Walker, Mary W, Wolinsky, Toni D, Jubian, Vrej, Chandrasena, Gamini, Zhong, Huailing, Huang, Xinyan, Miller, Silke, Hegde, Laxminarayan G, Marsteller, Douglas A, Marzabadi, Mohammad R, Papp, Mariusz, Overstreet, David H, Gerald, Christophe P G, and Craig, Douglas A

Abstract

Neuropeptide Y (NPY) regulates physiological processes via receptor subtypes (Y(1), Y(2), Y(4), Y(5), and y(6)). The Y(5) receptor is well known for its role in appetite. Based on expression in the limbic system, we hypothesized that the Y(5) receptor might also modulate stress sensitivity. We identified a novel Y(5) receptor-selective antagonist, Lu AA33810 [N-[[trans-4-[(4,5-dihydro[1]-benzothiepino[5,4-d]thiazol-2-yl)amino]cyclohexyl]methyl]-methanesulfonamide], that bound to cloned rat Y(5) receptors (K(i) = 1.5 nM) and antagonized NPY-evoked cAMP and calcium mobilization in vitro. Lu AA33810 (3-30 mg/kg p.o.) blocked feeding elicited by intracerebroventricular injection of the Y(5) receptor-selective agonist [cPP(1-7),NPY(19-23),Ala(31),Aib(32),Gln(34)]-hPancreatic Polypeptide in Sprague-Dawley rats. In vivo effects of Lu AA33810 were correlated with brain exposure > or = 50 ng/g and ex vivo Y(5) receptor occupancy of 22 to 95%. Lu AA33810 was subsequently evaluated in models of stress sensitivity. In Fischer 344 rats, Lu AA33810 (30 mg/kg p.o.) attenuated increases in plasma ACTH and corticosterone elicited by intracerebroventricular injection of [cPP(1-7),NPY(19-23),Ala(31),Aib(32),Gln(34)]-hPancreatic Polypeptide. In Sprague-Dawley rats subjected to the social interaction test, Lu AA33810 (3-30 mg/kg p.o.) produced anxiolytic-like effects after acute or chronic treatment. In Flinders sensitive line rats, chronic dosing of Lu AA33810 (10 mg/kg/day i.p.) produced anxiolytic-like effects in the social interaction test, plus antidepressant-like effects in the forced swim test. In Wistar rats exposed to chronic mild stress, chronic dosing of Lu AA33810 (3 and 10 mg/kg/day i.p.) produced antidepressant-like activity, i.e., normalization of stress-induced decrease in sucrose consumption. We propose that Y(5) receptors may function as part of an endogenous stress-sensing system to mediate social anxiety and reward or motivational deficits in selected rodent models.

Published
2009
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37. Comparative Metabolism of Radiolabeled Muraglitazar in Animals and Humans by Quantitative and Qualitative Metabolite Profiling

Author

Zhang, Donglu, Wang, Lifei, Raghavan, Nirmala, Zhang, Haiying, Li, Wenying, Cheng, Peter T., Yao, Ming, Zhang, Litao, Zhu, Mingshe, Bonacorsi, Samuel, Yeola, Suresh, Mitroka, James, Hariharan, Narayanan, Hosagrahara, Vinayak, Chandrasena, Gamini, Shyu, Wen Chyi, and Humphreys, W. Griffith

Abstract

Muraglitazar (Pargluva), a dual α/γ peroxisome proliferator-activated receptor (PPAR) activator, has both glucose- and lipid-lowering effects in animal models and in patients with diabetes. This study describes the in vivo and in vitro comparative metabolism of [14C]muraglitazar in rats, dogs, monkeys, and humans by quantitative and qualitative metabolite profiling. Metabolite identification and quantification methods used in these studies included liquid chromatography/mass spectrometry (LC/MS), LC/tandem MS, LC/radiodetection, LC/UV, and a newly described mass defect filtering technique in conjunction with high resolution MS. After oral administration of [14C]muraglitazar, absorption was rapid in all species, reaching a concentration peak for parent and total radioactivity in plasma within 1 h. The most abundant component in plasma at all times in all species was the parent drug, and no metabolite was present in greater than 2.5% of the muraglitazar concentrations at 1 h postdose in rats, dogs, and humans. All metabolites observed in human plasma were also present in rats, dogs, or monkeys. Urinary excretion of radioactivity was low (<5% of the dose) in all intact species, and the primary route of elimination was via biliary excretion in rats, monkeys, and humans. Based on recovered doses in urine and bile, muraglitazar showed a very good absorption in rats, monkeys, and humans. The major drug-related components in bile of rats, monkeys, and humans were glucuronides of muraglitazar and its oxidative metabolites. The parent compound was a minor component in bile, suggesting extensive metabolism of the drug. In contrast, the parent drug and oxidative metabolites were the major components in feces, and no glucuronide conjugates were found, suggesting that glucuronide metabolites were excreted in bile and hydrolyzed in the gastrointestinal tract. The metabolites of muraglitazar resulted from both glucuronidation and oxidation. The metabolites in general had greatly reduced activity as PPARα/γ activators relative to muraglitazar. In conclusion, muraglitazar was rapidly absorbed, extensively metabolized through glucuronidation and oxidation, and mainly eliminated in the feces via biliary excretion of glucuronide metabolites in all species studied. Disposition and metabolic pathways were qualitatively similar in rats, dogs, monkeys, and humans.

Published
2007
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38. Involvement of Multiple Cytochrome P450 and UDP-Glucuronosyltransferase Enzymes in the in Vitro Metabolism of Muraglitazar

Author

Zhang, Donglu, Wang, Lifei, Chandrasena, Gamini, Ma, Li, Zhu, Mingshe, Zhang, Hongjian, Davis, Carl D., and Humphreys, W. Griffith

Abstract

Muraglitazar (Pargluva), a dual α/γ peroxisome proliferator-activated receptor activator, has both glucose- and lipid-lowering effects in animal models and in patients with diabetes. The human major primary metabolic pathways of muraglitazar include acylglucuronidation, aliphatic/aryl hydroxylation, and O-demethylation. This study describes the identification of human cytochrome P450 (P450) and UDP-glucuronosyltransferase (UGT) enzymes involved in the in vitro metabolism of muraglitazar. [14C]Muraglitazar was metabolized by cDNA-expressed CYP2C8, 2C9, 2C19, 2D6, and 3A4, but to a very minimal extent by CYP1A2, 2A6, 2B6, 2C18, 2E1, and 3A5. Inhibition of the in vitro metabolism of muraglitazar in human liver microsomes, at a clinically efficacious concentration, by chemical inhibitors and monoclonal antibodies further supported involvement of CYP2C8, 2C9, 2C19, 2D6, and 3A4 in its oxidation. A combination of intrinsic clearance (Vmax/Km) and relative concentrations of each P450 enzyme in the human liver was used to predict the contribution of CYP2C8, 2C9, 2C19, 2D6, and 3A4 to the formation of each primary oxidative metabolite and to the overall oxidative metabolism of muraglitazar. Glucuronidation of [14C]muraglitazar was catalyzed by cDNA-expressed UGT1A1, 1A3, and 1A9, but not by UGT1A6, 1A8, 1A10, 2B4, 2B7, and 2B15. The Kmvalues for muraglitazar glucuronidation by the three active UGT enzymes were similar (2–4 μM). In summary, muraglitazar was metabolized by multiple P450 and UGT enzymes to form multiple metabolites. This characteristic predicts a low potential for the alteration of the pharmacokinetic parameters of muraglitazar via polymorphic drug metabolism enzymes responsible for clearance of the compound or by coadministration of drugs that inhibit or induce relevant metabolic enzymes.

Published
2007
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40. 3-Arylimino-2-indolones Are Potent and Selective Galanin GAL3 Receptor Antagonists

Author

J. Konkel, Michael, Lagu, Bharat, W. Boteju, Lakmal, Jimenez, Hermogenes, Noble, Stewart, W. Walker, Mary, Chandrasena, Gamini, P. Blackburn, Thomas, S. Nikam, Sham, L. Wright, Jon, E. Kornberg, Brian, Gregory, Tracy, A. Pugsley, Thomas, Akunne, Hyacinth, Zoski, Kim, and D. Wise, Lawrence

Abstract

A series of 3-imino-2-indolones are the first published, high-affinity antagonists of the galanin GAL3 receptor. One example, 1,3-dihydro-1-phenyl-3-[[3-(trifluoromethyl)phenyl]imino]-2H-indol-2-one (9), was shown to have high affinity for the human GAL3 receptor (Ki = 17 nM) and to be highly selective for GAL3 over a broad panel of targets, including GAL1 and GAL2. Compound 9 was also shown to be an antagonist in a human GAL3 receptor functional assay (Kb = 29 nM).

Published
2006

42. Fused thiazolyl alkynes as potent mGlu5 receptor positive allosteric modulators.

Author

Packiarajan, Mathivanan, Grenon, Michel, Zorn, Samuel, Hopper, Allen T., White, Andrew D., Chandrasena, Gamini, Pu, Xiaosui, Brodbeck, Robbin M., and Robichaud, Albert J.

Subjects
*GLUTAMATE receptors, *ALKYNES, *THIAZOLES, *ALLOSTERIC regulation, *STRUCTURE-activity relationships, *STRUCTURAL optimization, *CARBOXAMIDES
Abstract

Abstract: A new series of potent fused thiazole mGlu5 receptor positive allosteric modulators (PAMs) (10, 11 and 27–31) are disclosed and details of the SAR and optimization are described. Optimization of alkynyl thiazole 9 (Lu AF11205) led to the identification of potent fused thiazole analogs 10b, 27a, 28j and 31d. In general, substituted cycloalkyl, aryl and heteroaryl carboxamides, and carbamate analogs are mGlu5 PAMs, whereas smaller alkyl carboxamide, sulfonamide and sulfamide analogs tend to be mGlu5 negative allosteric modulators (NAMs). [Copyright &y& Elsevier]

Published
2013
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43. 5-(2′-Pyridyl)-2-aminothiazoles: Alkyl amino sulfonamides and sulfamides as potent NPY5 antagonists

Author

Packiarajan, Mathivanan, Coate, Heather, Desai, Mahesh, Jimenez, Hermogenes N., Reinhard, Emily J., Jubian, Vrej J., Marzabadi, Mohammad R., Chandrasena, Gamini, Wolinski, Toni C., Walker, Mary W., and Andersen, Kim

Subjects
*AZOLES, *AMIDES, *ORGANIC synthesis, *POLYPEPTIDES, *NEUROPEPTIDE Y, *SOLUBILITY, *PHARMACEUTICAL chemistry, *THERAPEUTICS, SULFONAMIDE drugs
Abstract

Abstract: Synthesis, SAR and physico-chemical properties of an alkyl aminothiazole series 8 and 16 are described. 2-Pyridylaminothiazole based compounds such as 8c and 16a exhibit high affinity at the NPY5 receptor with desirable c Log Ps and solubilities. However, they also suffer from high in vitro and in vivo clearance. Compound 16a partially inhibits the feeding behavior elicited by i.c.v. injection of the selective NPY5 agonist [cPP1–7, NPY19–23, Ala31, Aib32, Gln34]-human pancreatic polypeptide polypeptide (cPP). [Copyright &y& Elsevier]

Published
2011
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44. Design and synthesis of N-[(4-methoxyphenoxy)carbonyl]-N-[[4-[2-(5- methyl-2-phenyl-4-oxazolyl)ethoxy]phenyl]methyl]glycine [Muraglitazar/BMS-298585], a novel peroxisome proliferator-activated receptor alpha/gamma dual agonist with efficacious glucose and lipid-lowering activities.

Author

Devasthale PV, Chen S, Jeon Y, Qu F, Shao C, Wang W, Zhang H, Cap M, Farrelly D, Golla R, Grover G, Harrity T, Ma Z, Moore L, Ren J, Seethala R, Cheng L, Sleph P, Sun W, Tieman A, Wetterau JR, Doweyko A, Chandrasena G, Chang SY, Humphreys WG, Sasseville VG, Biller SA, Ryono DE, Selan F, Hariharan N, and Cheng PT

Subjects
Adipocytes cytology, Animals, Blood Glucose drug effects, Cell Line, Diabetes Mellitus, Type 2 drug therapy, Fatty Acids blood, Glycine chemistry, Glycine pharmacology, Humans, Hyperlipidemias drug therapy, Hypoglycemic Agents pharmacokinetics, Hypoglycemic Agents pharmacology, Hypolipidemic Agents pharmacokinetics, Hypolipidemic Agents pharmacology, Insulin blood, Male, Mice, Mice, Obese, Oxazoles chemistry, Oxazoles pharmacology, Transcriptional Activation, Triglycerides blood, Glycine analogs & derivatives, Glycine chemical synthesis, Hypoglycemic Agents chemical synthesis, Hypolipidemic Agents chemical synthesis, Oxazoles chemical synthesis, PPAR alpha agonists, PPAR gamma agonists
Abstract

Muraglitazar/BMS-298585 (2) has been identified as a non-thiazolidinedione PPAR alpha/gamma dual agonist that shows potent activity in vitro at human PPARalpha (EC(50) = 320 nM) and PPARgamma(EC(50) = 110 nM). Compound 2 shows excellent efficacy for lowering glucose, insulin, triglycerides, and free fatty acids in genetically obese, severely diabetic db/db mice and has a favorable ADME profile. Compound 2 is currently in clinical development for the treatment of type 2 diabetes and dyslipidemia.

Published
2005
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