Your search keyword '"Aberra Fura"' showing total 50 results

1. Discovery of a Partial Glucokinase Activator Clinical Candidate: Diethyl ((3-(3-((5-(Azetidine-1-carbonyl)pyrazin-2-yl)oxy)-5-isopropoxybenzamido)-1H-pyrazol-1-yl)methyl)phosphonate (BMS-820132)

Author

Yan Shi, Ying Wang, Wei Meng, Robert P. Brigance, Denis E. Ryono, Scott Bolton, Hao Zhang, Sean Chen, Rebecca Smirk, Shiwei Tao, Joseph A. Tino, Kristin N. Williams, Richard Sulsky, Laura Nielsen, Bruce Ellsworth, Michael K. Y. Wong, Jung-Hui Sun, Leslie W. Leith, Dawn Sun, Dauh-Rurng Wu, Anuradha Gupta, Richard Rampulla, Arvind Mathur, Bang-Chi Chen, Aiying Wang, Helen G. Fuentes-Catanio, Lori Kunselman, Michael Cap, Jacob Zalaznick, Xiaohui Ma, Heng Liu, Joseph R. Taylor, Rachel Zebo, Beverly Jones, Stephen Kalinowski, Joann Swartz, Ada Staal, Kevin O’Malley, Lisa Kopcho, Jodi K. Muckelbauer, Stanley R. Krystek, Steven A. Spronk, Jovita Marcinkeviciene, Gerry Everlof, Xue-Qing Chen, Carrie Xu, Yi-Xin Li, Robert A. Langish, Yanou Yang, Qi Wang, Kamelia Behnia, Aberra Fura, Evan B. Janovitz, Nicola Pannacciulli, Steven Griffen, Bradley A. Zinker, John Krupinski, Mark Kirby, Jean Whaley, Robert Zahler, Joel C. Barrish, Jeffrey A. Robl, and Peter T. W. Cheng

Subjects

Drug Discovery, Molecular Medicine

Published

2022

2. The discovery of BMS-737 as a potent, CYP17 lyase-selective inhibitor for the treatment of castration-resistant prostate cancer

Author

Chetan Padmakar Darne, Upender Velaparthi, Mark Saulnier, David Frennesson, Peiying Liu, Audris Huang, John Tokarski, Aberra Fura, Thomas Spires, John Newitt, Vanessa M. Spires, Mary T. Obermeier, Paul A. Elzinga, Marco M. Gottardis, Lata Jayaraman, Gregory D. Vite, and Aaron Balog

Subjects

Male, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Lyases, Prostatic Neoplasms, Steroid 17-alpha-Hydroxylase, Androgen Antagonists, Biochemistry, Xenobiotics, Prostatic Neoplasms, Castration-Resistant, Mineralocorticoids, Drug Discovery, Molecular Medicine, Humans, Testosterone, Enzyme Inhibitors, Molecular Biology, Glucocorticoids

Abstract

We report herein, the discovery of BMS-737 (compound 33) as a potent, non-steroidal, reversible small molecule inhibitor demonstrating 11-fold selectivity for CYP17 lyase over CYP17 hydroxylase, as well as a clean xenobiotic CYP profile for the treatment of castration-resistant prostate cancer (CRPC). Extensive SAR studies on the initial lead 1 at three different regions of the molecule resulted in the identification of BMS-737, which demonstrated a robust 83% lowering of testosterone without any significant perturbation of the mineralocorticoid and glucocorticoid levels in cynomologous monkeys in a 1-day PK/PD study.

Published

2022

3. Azatricyclic Inverse Agonists of RORγt That Demonstrate Efficacy in Models of Rheumatoid Arthritis and Psoriasis

Author

Aberra Fura, Shiuhang Yip, Georgia Cornelius, Hai-Yun Xiao, Qingjie Liu, Sha Li, Ning Li, Nicholas A. Meanwell, Shailesh Dudhgaonkar, Max Ruzanov, Jenny Xie, Zili Xiao, Purnima Khandelwal, Carolyn A. Weigelt, David J. Shuster, Dauh-Rurng Wu, T. G. Murali Dhar, Tara Sherry, Yang Michael G, Kevin Stefanski, Jignesh Nagar, Rex Denton, Qihong Zhao, Peng Li, Silvi A. Chacko, Arun Govindarajan, Robert M. Borzilleri, John S. Sack, Yeheng Zhu, Yunling Song, Dawn Sun, Anjuman Rudra, Mary T. Obermeier, Jinhong Wang, Douglas G. Batt, and Venkata Murali

Subjects

Membrane permeability, 010405 organic chemistry, Chemistry, Organic Chemistry, Pharmacology, medicine.disease, 01 natural sciences, Biochemistry, In vitro, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, In vivo, RAR-related orphan receptor gamma, Psoriasis, Rheumatoid arthritis, Drug Discovery, medicine, Potency, Inverse agonist

Abstract

[Image: see text] Structure–activity relationship studies directed toward the replacement of the fused phenyl ring of the lead hexahydrobenzoindole RORγt inverse agonist series represented by 1 with heterocyclic moieties led to the identification of three novel aza analogs 5–7. The hexahydropyrrolo[3,2-f]quinoline series 5 (X = N, Y = Z=CH) showed potency and metabolic stability comparable to series 1 but with improved in vitro membrane permeability and serum free fraction. This structural modification was applied to the hexahydrocyclopentanaphthalene series 3, culminating in the discovery of 8e as a potent and selective RORγt inverse agonist with an excellent in vitro profile, good pharmacokinetic properties, and biologic-like in vivo efficacy in preclinical models of rheumatoid arthritis and psoriasis.

Published

2021

4. Novel Tricyclic Pyroglutamide Derivatives as Potent RORγt Inverse Agonists Identified using a Virtual Screening Approach

Author

Tara Sherry, John E. Macor, Jinhong Wang, Georgia Cornelius, Shiuhang Yip, Luisa Salter-Cid, Qingjie Liu, Purnima Khandelwal, Carolyn A. Weigelt, Max Ruzanov, John S. Sack, Kevin Stefanski, Jenny Xie, T. G. Murali Dhar, Sha Li, Melissa Yarde, Joseph A. Tino, Qihong Zhao, Dauh-Rurng Wu, Mary T. Obermeier, David J. Shuster, Aberra Fura, Douglas G. Batt, and Rex Denton

Subjects

chemistry.chemical_classification, Virtual screening, 010405 organic chemistry, Stereochemistry, Organic Chemistry, Prodrug, Cyclohexanecarboxylic acid, 01 natural sciences, Biochemistry, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, chemistry.chemical_compound, chemistry, RAR-related orphan receptor gamma, Drug Discovery, Moiety, Inverse agonist, Solubility, Tricyclic

Abstract

[Image: see text] Employing a virtual screening approach, we identified the pyroglutamide moiety as a nonacid replacement for the cyclohexanecarboxylic acid group which, when coupled to our previously reported conformationally locked tricyclic core, provided potent and selective RORγt inverse agonists. Structure–activity relationship optimization of the pyroglutamide moiety led to the identification of compound 18 as a potent and selective RORγt inverse agonist, albeit with poor aqueous solubility. We took advantage of the tertiary carbinol group in 18 to synthesize a phosphate prodrug, which provided good solubility, excellent exposures in mouse PK studies, and significant efficacy in a mouse model of psoriasis.

Published

2020

5. Discovery of a Partial Glucokinase Activator Clinical Candidate: Diethyl ((3-(3-((5-(Azetidine-1-carbonyl)pyrazin-2-yl)oxy)-5-isopropoxybenzamido)-1

Author

Yan, Shi, Ying, Wang, Wei, Meng, Robert P, Brigance, Denis E, Ryono, Scott, Bolton, Hao, Zhang, Sean, Chen, Rebecca, Smirk, Shiwei, Tao, Joseph A, Tino, Kristin N, Williams, Richard, Sulsky, Laura, Nielsen, Bruce, Ellsworth, Michael K Y, Wong, Jung-Hui, Sun, Leslie W, Leith, Dawn, Sun, Dauh-Rurng, Wu, Anuradha, Gupta, Richard, Rampulla, Arvind, Mathur, Bang-Chi, Chen, Aiying, Wang, Helen G, Fuentes-Catanio, Lori, Kunselman, Michael, Cap, Jacob, Zalaznick, Xiaohui, Ma, Heng, Liu, Joseph R, Taylor, Rachel, Zebo, Beverly, Jones, Stephen, Kalinowski, Joann, Swartz, Ada, Staal, Kevin, O'Malley, Lisa, Kopcho, Jodi K, Muckelbauer, Stanley R, Krystek, Steven A, Spronk, Jovita, Marcinkeviciene, Gerry, Everlof, Xue-Qing, Chen, Carrie, Xu, Yi-Xin, Li, Robert A, Langish, Yanou, Yang, Qi, Wang, Kamelia, Behnia, Aberra, Fura, Evan B, Janovitz, Nicola, Pannacciulli, Steven, Griffen, Bradley A, Zinker, John, Krupinski, Mark, Kirby, Jean, Whaley, Robert, Zahler, Joel C, Barrish, Jeffrey A, Robl, and Peter T W, Cheng

Subjects

Diabetes Mellitus, Type 2, Glucokinase, Organophosphonates, Azetidines, Humans, Hypoglycemic Agents, Hypoglycemia

Abstract

Glucokinase (GK) is a key regulator of glucose homeostasis, and its small-molecule activators represent a promising opportunity for the treatment of type 2 diabetes. Several GK activators have been advanced into clinical trials and have demonstrated promising efficacy; however, hypoglycemia represents a key risk for this mechanism. In an effort to mitigate this hypoglycemia risk while maintaining the efficacy of the GK mechanism, we have investigated a series of amino heteroaryl phosphonate benzamides as ''partial" GK activators. The structure-activity relationship studies starting from a "full GK activator"

Published

2022

6. Rationally Designed, Conformationally Constrained Inverse Agonists of RORγt—Identification of a Potent, Selective Series with Biologic-Like in Vivo Efficacy

Author

Carolyn A. Weigelt, Sha Li, David Marcoux, Georgia Cornelius, Qihong Zhao, Mary Ellen Cvijic, John E. Macor, Jingwu Duan, Melissa Yarde, Muthalagu Vetrichelvan, David J. Shuster, Qingjie Liu, Richard Rampulla, Kim W. McIntyre, Mary T. Obermeier, Shiuhang Yip, Purnima Khandelwal, Sureshbabu Vishwakrishnan, Anuradha Gupta, Virna Borowski, Peng Li, Kevin Stefanski, Sridharan Ramlingam, Myra Beaudoin-Bertrand, Nageswara Maddala, Sridhar Vanteru, Percy H. Carter, Arvind Mathur, Aberra Fura, Max Ruzanov, John Hynes, Dauh-Rurng Wu, Jinhong Wang, Luisa Salter-Cid, John S. Sack, Cornelius Lyndon A M, Anurag S. Srivastava, Robert J. Cherney, Kumaravel Selvakumar, Mushkin Basha, Arun Kumar Gupta, Douglas G. Batt, Rex Denton, Sukhen Karmakar, Qing Shi, Ananta Karmakar, Naveen Manjunath, Javed Khan, Jenny Xie, Joseph A. Tino, and T. G. Murali Dhar

Subjects

Models, Molecular, Pyrrolidines, Drug Inverse Agonism, Protein Conformation, Pharmacology, 01 natural sciences, Jurkat Cells, Mice, Structure-Activity Relationship, 03 medical and health sciences, Psoriatic arthritis, RAR-related orphan receptor gamma, In vivo, Drug Discovery, medicine, Animals, Humans, Inverse agonist, Structure–activity relationship, Tissue Distribution, 030304 developmental biology, 0303 health sciences, Chemistry, Nuclear Receptor Subfamily 1, Group F, Member 3, medicine.disease, In vitro, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Nuclear receptor, Drug Design, Molecular Medicine

Abstract

RORγt is an important nuclear receptor that regulates the production of several pro-inflammatory cytokines such as IL-17 and IL-22. As a result, RORγt has been identified as a potential target for the treatment of various immunological disorders such as psoriasis, psoriatic arthritis, and inflammatory bowel diseases. Structure and computer-assisted drug design led to the identification of a novel series of tricyclic RORγt inverse agonists with significantly improved in vitro activity in the reporter (Gal4) and human whole blood assays compared to our previous chemotype. Through careful structure activity relationship, several potent and selective RORγt inverse agonists have been identified. Pharmacokinetic studies allowed the identification of the lead molecule 32 with a low peak-to-trough ratio. This molecule showed excellent activity in an IL-2/IL-23-induced mouse pharmacodynamic study and demonstrated biologic-like efficacy in an IL-23-induced preclinical model of psoriasis.

Published

2019

7. Driving Potency with Rotationally Stable Atropisomers: Discovery of Pyridopyrimidinedione-Carbazole Inhibitors of BTK

Author

Soo S. Ko, James Kempson, Yingru Zhang, Tracy L. Taylor, Kim W. McIntyre, James R. Burke, Luisa Salter-Cid, Shiuhang Yip, Celia D’Arienzo, Aberra Fura, Stacey Skala, Joseph A. Tino, Jun Dai, Chunlei Wang, Joel C. Barrish, Michael Galella, Kathleen M. Gillooly, Bei Wang, Dauh-Rurng Wu, Lorell Discenza, Xiaoping Hou, Arvind Mathur, Richard Rampulla, Dawn Sun, Scott H. Watterson, Mary T. Obermeier, Percy H. Carter, Mark A. Pattoli, Anurag S. Srivastava, Lihong Cheng, Rulin Zhao, Peng Li, Claudine Pulicicchio, Joseph Pawluczyk, and Rodney Vickery

Subjects

Autoimmune disease, Atropisomer, biology, Stereochemistry, Carbazole, Organic Chemistry, medicine.disease, Biochemistry, Small molecule, chemistry.chemical_compound, chemistry, Drug Discovery, medicine, biology.protein, Bruton's tyrosine kinase, Kinase activity, Chirality (chemistry), Tyrosine kinase

Abstract

[Image: see text] Bruton’s tyrosine kinase (BTK) has been shown to play a key role in the pathogenesis of autoimmunity. Therefore, the inhibition of the kinase activity of BTK with a small molecule inhibitor could offer a breakthrough in the clinical treatment of many autoimmune diseases. This Letter describes the discovery of BMS-986143 through systematic structure–activity relationship (SAR) development. This compound benefits from defined chirality derived from two rotationally stable atropisomeric axes, providing a potent and selective single atropisomer with desirable efficacy and tolerability profiles.

Published

2020

8. Discovery of BMS-986251: A Clinically Viable, Potent, and Selective RORγt Inverse Agonist

Author

Qingjie Liu, Mary T. Obermeier, John S. Sack, Carolyn A. Weigelt, Georgia Cornelius, Percy H. Carter, David J. Shuster, Luisa Salter-Cid, Aberra Fura, Virna Borowski, Jingwu Duan, Purnima Khandelwal, Qing Shi, Robert J. Cherney, Cornelius Lyndon A M, Jinhong Wang, Jenny Xie, Max Ruzanov, Kevin Stefanski, Rex Denton, T. G. Murali Dhar, David Marcoux, Shiuhang Yip, Melissa Yarde, Douglas G. Batt, Javed Khan, Joseph A. Tino, Qihong Zhao, Anurag S. Srivastava, Arvind Mathur, Mary Ellen Cvijic, John E. Macor, Sha Li, and Dauh-Rurng Wu

Subjects

chemistry.chemical_classification, 010405 organic chemistry, Chemistry, Organic Chemistry, Inflammation, Acanthosis, Pharmacology, medicine.disease, 01 natural sciences, Biochemistry, 0104 chemical sciences, Bioavailability, 010404 medicinal & biomolecular chemistry, Pharmacokinetics, Pharmacodynamics, Drug Discovery, medicine, Inverse agonist, medicine.symptom, Whole blood, Tricyclic

Abstract

[Image: see text] Novel tricyclic analogues were designed, synthesized, and evaluated as RORγt inverse agonists. Several of these compounds were potent in an IL-17 human whole blood assay and exhibited excellent oral bioavailability in mouse pharmacokinetic studies. This led to the identification of compound 5, which displayed dose-dependent inhibition of IL-17F production in a mouse IL-2/IL-23 stimulated pharmacodynamic model. In addition, compound 5 was studied in mouse acanthosis and imiquimod-induced models of skin inflammation, where it demonstrated robust efficacy comparable to a positive control. As a result of this excellent overall profile, compound 5 (BMS-986251) was selected as a clinically viable developmental candidate.

Published

2020

9. Discovery of Branebrutinib (BMS-986195): A Strategy for Identifying a Highly Potent and Selective Covalent Inhibitor Providing Rapid in Vivo Inactivation of Bruton's Tyrosine Kinase (BTK)

Author

Richard Rampulla, Stacey Skala, Charu Chaudhry, Percy H. Carter, Alban Allentoff, Tracy L. Taylor, Ling Li, Andrew J. Tebben, Luisa Salter-Cid, Aberra Fura, Rulin Zhao, Ian M. Catlett, Richard A. Westhouse, Myra Beaudoin Bertrand, John E. Macor, Robin Moore, Celia D’Arienzo, Matt Pokross, Douglas G. Batt, Scott H. Watterson, Mary T. Obermeier, Qingjie Liu, Daniel Smith, Lorell Discenza, Michael Galella, Jun Dai, Arvind Mathur, Kathleen M. Gillooly, Elizabeth M. Heimrich, Jianqing Li, Zheng Yang, Michael Wallace, Kim W. McIntyre, James R. Burke, Mark A. Pattoli, Joseph A. Tino, Lihong Cheng, Naiyu Zheng, Rodney Vickery, Claudine Pulicicchio, Yifan Zhang, Qian Ruan, and Paul A. Elzinga

Subjects

Indoles, B-cell receptor, 01 natural sciences, Arthritis, Rheumatoid, 03 medical and health sciences, Inhibitory Concentration 50, Mice, Piperidines, immune system diseases, In vivo, hemic and lymphatic diseases, Drug Discovery, Agammaglobulinaemia Tyrosine Kinase, Bruton's tyrosine kinase, Animals, Humans, Lupus Erythematosus, Systemic, Receptor, Protein Kinase Inhibitors, 030304 developmental biology, 0303 health sciences, biology, Dose-Response Relationship, Drug, Kinase, Drug discovery, Chemistry, breakpoint cluster region, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Macaca fascicularis, Cancer research, biology.protein, Molecular Medicine, Tyrosine kinase

Abstract

Bruton’s tyrosine kinase (BTK), a non-receptor tyrosine kinase, is a member of the Tec family of kinases and is essential for B cell receptor (BCR) mediated signaling. BTK also plays a critical role in the downstream signaling pathways for the Fcγ receptor in monocytes, the Fce receptor in granulocytes, and the RANK receptor in osteoclasts. As a result, pharmacological inhibition of BTK is anticipated to provide an effective strategy for the clinical treatment of autoimmune diseases such as rheumatoid arthritis and lupus. This article will outline the evolution of our strategy to identify a covalent, irreversible inhibitor of BTK that has the intrinsic potency, selectivity, and pharmacokinetic properties necessary to provide a rapid rate of inactivation systemically following a very low dose. With excellent in vivo efficacy and a very desirable tolerability profile, 5a (branebrutinib, BMS-986195) has advanced into clinical studies.

Published

2019

10. Tricyclic sulfones as potent, selective and efficacious RORγt inverse agonists – Exploring C6 and C8 SAR using late-stage functionalization

Author

Georgia Cornelius, Carolyn A. Weigelt, Sha Li, Dauh-Rurng Wu, David Marcoux, Luisa Salter-Cid, Aberra Fura, Melissa Yarde, Shiuhang Yip, Peng Li, John Hynes, Tara Sherry, Max Ruzanov, Rex Denton, Robert J. Cherney, Yue-Zhong Shu, Jinhong Wang, Mary Ellen Cvijic, Zili Xiao, David J. Shuster, Jenny Xie, Purnima Khandelwal, Kevin Stefanski, T. G. Murali Dhar, Qing Shi, Yang Michael G, Mary T. Obermeier, Silvi A. Chacko, Javed Khan, John S. Sack, Joseph A. Tino, and Qihong Zhao

Subjects

Male, Drug Inverse Agonism, Clinical Biochemistry, Pharmaceutical Science, Crystallography, X-Ray, 01 natural sciences, Biochemistry, Melanosis, Sulfone, Structure-Activity Relationship, chemistry.chemical_compound, RAR-related orphan receptor gamma, Drug Discovery, Animals, Inverse agonist, Sulfones, Molecular Biology, chemistry.chemical_classification, Mice, Inbred BALB C, Molecular Structure, 010405 organic chemistry, Chemistry, Organic Chemistry, Interleukin-18, Late stage, Regioselectivity, Nuclear Receptor Subfamily 1, Group F, Member 3, Combinatorial chemistry, 0104 chemical sciences, Mice, Inbred C57BL, 010404 medicinal & biomolecular chemistry, Molecular Medicine, Female, Heterocyclic Compounds, 3-Ring, Protein Binding, Tricyclic

Abstract

In order to rapidly develop C6 and C8 SAR of our reported tricyclic sulfone series of RORγt inverse agonists, a late-stage bromination was employed. Although not regioselective, the bromination protocol allowed us to explore new substitution patterns/vectors that otherwise would have to be incorporated at the very beginning of the synthesis. Based on the SAR obtained from this exercise, compound 15 bearing a C8 fluorine was developed as a very potent and selective RORγt inverse agonist. This analog's in vitro profile, pharmacokinetic (PK) data and efficacy in an IL-23 induced mouse acanthosis model will be discussed.

Published

2020

11. Discovery of 6-Fluoro-5-(R)-(3-(S)-(8-fluoro-1-methyl-2,4-dioxo-1,2-dihydroquinazolin-3(4H)-yl)-2-methylphenyl)-2-(S)-(2-hydroxypropan-2-yl)-2,3,4,9-tetrahydro-1H-carbazole-8-carboxamide (BMS-986142): A Reversible Inhibitor of Bruton’s Tyrosine Kinase (BTK) Conformationally Constrained by Two Locked Atropisomers

Author

Jun Dai, Arvind Mathur, Lihong Cheng, Kim W. McIntyre, Dawn Sun, Joseph A. Tino, Shiuhang Yip, Douglas G. Batt, Jodi K. Muckelbauer, James R. Burke, Joel C. Barrish, Rodney Vickery, Celia D’Arienzo, Luisa Salter-Cid, Qingjie Liu, Tracy L. Taylor, Hua Gong, Mark A. Pattoli, Elizabeth M. Heimrich, Yingru Zhang, Andy J. Tebben, Myra Beaudoin Bertrand, Kathleen M. Gillooly, Chiehying Chang, Percy H. Carter, Scott H. Watterson, Mary T. Obermeier, Claudine Pulicicchio, Aberra Fura, Chunlei Wang, Michael Galella, Charles M. Langevine, Sarah C. Traeger, Lorell Discenza, Peng Li, Yifan Zhang, Qing Shi, Stacey Skala, Dauh-Rurng Wu, Richard Rampulla, and George V. De Lucca

Subjects

0301 basic medicine, Atropisomer, biology, 010405 organic chemistry, medicine.drug_class, Kinase, Chemistry, Stereochemistry, B-cell receptor, Carboxamide, 01 natural sciences, 0104 chemical sciences, 03 medical and health sciences, 030104 developmental biology, immune system diseases, hemic and lymphatic diseases, Drug Discovery, medicine, biology.protein, Molecular Medicine, Structure–activity relationship, Bruton's tyrosine kinase, Transferase, Tyrosine kinase

Abstract

Bruton's tyrosine kinase (BTK), a nonreceptor tyrosine kinase, is a member of the Tec family of kinases. BTK plays an essential role in B cell receptor (BCR)-mediated signaling as well as Fcγ receptor signaling in monocytes and Fce receptor signaling in mast cells and basophils, all of which have been implicated in the pathophysiology of autoimmune disease. As a result, inhibition of BTK is anticipated to provide an effective strategy for the clinical treatment of autoimmune diseases such as lupus and rheumatoid arthritis. This article details the structure–activity relationships (SAR) leading to a novel series of highly potent and selective carbazole and tetrahydrocarbazole based, reversible inhibitors of BTK. Of particular interest is that two atropisomeric centers were rotationally locked to provide a single, stable atropisomer, resulting in enhanced potency and selectivity as well as a reduction in safety liabilities. With significantly enhanced potency and selectivity, excellent in vivo properties an...

Published

2016

12. Discovery of the Selective CYP17A1 Lyase Inhibitor BMS-351 for the Treatment of Prostate Cancer

Author

Gregory D. Vite, Paul A. Elzinga, David L. Gold, Cheryl A. Rizzo, Thomas E. Spires, Sophie Beyer, Vanessa M. Spires, Marco M. Gottardis, George L. Trainor, Aberra Fura, Audris Huang, Gordon Todderud, John A. Newitt, Lata Jayaraman, Aaron Balog, Andrew J. Tebben, Yongxin Zhu, Mary T. Obermeier, Goodenough Angela, Bethanne M. Warrack, Arthur M. Doweyko, and Yi Fan

Subjects

0301 basic medicine, Benzimidazole, education, Organic Chemistry, Pharmacology, medicine.disease, Lyase, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Prostate cancer, 030104 developmental biology, chemistry, In vivo, CYP17A1, Lyase inhibitor, Drug Discovery, medicine, Steroid 11-beta-hydroxylase, Glucocorticoid, medicine.drug

Abstract

Efforts to identify a potent, reversible, nonsteroidal CYP17A1 lyase inhibitor with good selectivity over CYP17A1 hydroxylase and CYPs 11B1 and 21A2 for the treatment of castration-resistant prostate cancer (CRPC) culminated in the discovery of BMS-351 (compound 18), a pyridyl biaryl benzimidazole with an excellent in vivo profile. Biological evaluation of BMS-351 at a dose of 1.5 mg in castrated cynomolgus monkeys revealed a remarkable reduction in testosterone levels with minimal glucocorticoid and mineralcorticoid perturbation. Based on a favorable profile, BMS-351 was selected as a candidate for further preclinical evaluation.

Published

2015

13. Daclatasvir: A Review of Preclinical and Clinical Pharmacokinetics

Author

Tushar Garimella, Yash Gandhi, Aberra Fura, Wenying Li, Timothy Eley, and Richard Bertz

Subjects

Daclatasvir, Pyrrolidines, Abcg2, Hepatitis C virus, Drug Evaluation, Preclinical, Biological Availability, Pharmacology, Viral Nonstructural Proteins, medicine.disease_cause, 030226 pharmacology & pharmacy, Antiviral Agents, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, medicine, Animals, Cytochrome P-450 CYP3A, Humans, Pharmacology (medical), Drug Interactions, Tissue Distribution, Clinical Trials as Topic, Organic cation transport proteins, biology, CYP3A4, Chemistry, Imidazoles, Cytochrome P450, Valine, Hepatitis C, Hepatitis C, Chronic, medicine.disease, Absorption, Physiological, biology.protein, 030211 gastroenterology & hepatology, Carbamates, medicine.drug, Half-Life

Abstract

Daclatasvir is a first-in-class, highly selective, hepatitis C virus, non-structural protein 5a polymerase replication complex inhibitor with picomolar potency and broad genotypic coverage in vitro. Daclatasvir undergoes rapid absorption, with a time to reach maximum plasma concentration of 1–2 h and an elimination half-life of ~ 10 to 14 h observed in single-ascending dose studies. Steady state was achieved by day 4 in multiple-ascending dose studies. Daclatasvir can be administered without regard to food or pH modifiers. Daclatasvir exposure is similar between healthy subjects and subjects infected with hepatitis C virus. Intrinsic factors such as age, race, or sex do not impact daclatasvir exposure. No dose adjustment is necessary for patients with any degree of hepatic or renal impairment. Daclatasvir has low-to-moderate clearance with the predominant route of elimination via cytochrome P450 3A4-mediated metabolism and P-glycoprotein excretion and intestinal secretion. Renal clearance is a minor route of elimination for daclatasvir. As a result, the dose of daclatasvir should be reduced from 60 to 30 mg once daily when co-administered with strong inhibitors of cytochrome P450 3A4. No dose adjustment is required when daclatasvir is co-administered with moderate inhibitors of cytochrome P450 3A4. The dose of daclatasvir should be increased from 60 to 90 mg once daily when co-administered with moderate inducers of cytochrome P450 3A4. Co-administration of daclatasvir with strong inducers of cytochrome P450 3A4 is contraindicated. Concurrent medications with inhibitory effects on P-glycoprotein without concurrent inhibition of cytochrome P450 3A4 are unlikely to cause marked changes in daclatasvir exposure, as the clearance of daclatasvir is through both cytochrome P450 3A4 and P-glycoprotein. The potential for daclatasvir to affect the pharmacokinetics of concomitantly administered drugs that are substrates of the cytochrome P450 enzyme system is low. In vitro, daclatasvir is a weak-to-moderate inhibitor of transporters including organic cation transporter 1, P-glycoprotein, organic transporting polypeptide 1B1, organic transporting polypeptide 1B3, and breast cancer resistance protein, although in clinical studies, daclatasvir has not altered the pharmacokinetics of concomitantly administered drugs that are substrates of these transporters to an appreciable degree, except for rosuvastatin. In summary, daclatasvir is a hepatitis C virus, non-structural protein 5a-selective inhibitor with a well-characterized pharmacokinetic profile that forms part of potent and well-tolerated all-oral treatment regimens for chronic hepatitis C virus infection.

Published

2018

14. Discovery of pyrrolo[1,2-b]pyridazine-3-carboxamides as Janus kinase (JAK) inhibitors

Author

Joel C. Barrish, Aberra Fura, Guoxiang Shen, Jingwu Duan, David S. Nirschl, Jonathan Lippy, Stephen T. Wrobleski, Rosemary Zhang, Lidia M. Doweyko, Bingwei V. Yang, Lauren Haque, Murray McKinnon, Shuqun Lin, Luisa Salter-Cid, Sidney Pitt, William J. Pitts, Percy H. Carter, John S. Sack, Gary L. Schieven, Bin Jiang, John Hynes, Gregory D. Brown, John S. Tokarski, Zhonghui Lu, Javed Khan, and Steven G. Nadler

Subjects

Models, Molecular, Protein Conformation, Stereochemistry, Clinical Biochemistry, Substituent, Administration, Oral, Pharmaceutical Science, Enzyme-Linked Immunosorbent Assay, Biochemistry, Pyrrolopyridazine, Pyridazine, Interferon-gamma, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, Functional selectivity, Animals, Humans, Pyrroles, Tissue Distribution, Protein Kinase Inhibitors, Molecular Biology, Whole blood, Mice, Inbred BALB C, Molecular Structure, Organic Chemistry, Janus Kinase 3, Janus Kinase 1, Janus Kinase 2, Pyridazines, chemistry, Tyrosine kinase 2, Molecular Medicine, Amine gas treating, Janus kinase

Abstract

A new class of Janus kinase (JAK) inhibitors was discovered using a rationally designed pyrrolo[1,2-b]pyridazine-3-carboxamide scaffold. Preliminary studies identified (R)-(2,2-dimethylcyclopentyl)amine as a preferred C4 substituent on the pyrrolopyridazine core (3b). Incorporation of amino group to 3-position of the cyclopentane ring resulted in a series of JAK3 inhibitors (4g-4j) that potently inhibited IFNγ production in an IL2-induced whole blood assay and displayed high functional selectivity for JAK3-JAK1 pathway relative to JAK2. Further modifications led to the discovery of an orally bioavailable (2-fluoro-2-methylcyclopentyl)amino analogue 5g which is a nanomolar inhibitor of both JAK3 and TYK2, functionally selective for the JAK3-JAK1 pathway versus JAK2, and active in a human whole blood assay.

Published

2014

15. Identification of a Potent, Selective, and Efficacious Phosphatidylinositol 3-Kinase δ (PI3Kδ) Inhibitor for the Treatment of Immunological Disorders

Author

Dezhi Xing, Carolyn A. Weigelt, Luisa Salter-Cid, Pirama Nayagam Arunachalam, Rodney B.W. Smith, Ling Li, Melissa Yarde, Jodi K. Muckelbauer, Jonathan Lippy, Mary Ellen Cvijic, Sidney Pitt, John S. Sack, Thatipamula Rp, Michael A. Poss, Paul Levesque, Robert J. Cherney, Ipsit Kundu, David Marcoux, Gary L. Schieven, Arvind Mathur, Qingjie Liu, Zheming Ruan, Rosemary Zhang, R M Fancher, Shweta Padmanabhan, Scott H. Watterson, Qing Shi, Mary T. Obermeier, Anurag S. Srivastava, Anuradha Gupta, Douglas G. Batt, James Neels, Joseph A. Tino, Kevin Stefanski, Percy H. Carter, Macor John E, John Hynes, Myra Beaudoin-Bertrand, Hao Lu, Kim W. McIntyre, Stacey Skala, Aberra Fura, Lan-Ying Qin, Cornelius Lyndon A M, James Hennan, Richard Rampulla, Bogdan Sleczka, Jenny Xie, Kallem Rajareddy, Jie Pan, Christine B. Goldstine, Hua Gong, Qian Ruan, Kathleen M. Gillooly, Donna L. Pedicord, Jingsong Fan, Rajeev S. Bhide, and Stefan Ruepp

Subjects

0301 basic medicine, Antigens, Differentiation, T-Lymphocyte, Male, ERG1 Potassium Channel, hERG, Drug Evaluation, Preclinical, Phosphatidylinositol 3-Kinases, Pharmacology, Pyrazole, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, Dogs, Antigens, CD, Drug Discovery, Structure–activity relationship, Potency, Animals, Humans, Lectins, C-Type, Phosphatidylinositol, Enzyme Inhibitors, Phosphoinositide-3 Kinase Inhibitors, Mice, Inbred BALB C, biology, Kinase, Arthritis, Experimental, Isoenzymes, 030104 developmental biology, chemistry, Immune System Diseases, biology.protein, Molecular Medicine, Pyrazoles, Female, Efflux, Rabbits, Caco-2 Cells

Abstract

PI3Kδ plays an important role controlling immune cell function and has therefore been identified as a potential target for the treatment of immunological disorders. This article highlights our work toward the identification of a potent, selective, and efficacious PI3Kδ inhibitor. Through careful SAR, the successful replacement of a polar pyrazole group by a simple chloro or trifluoromethyl group led to improved Caco-2 permeability, reduced Caco-2 efflux, reduced hERG PC activity, and increased selectivity profile while maintaining potency in the CD69 hWB assay. The optimization of the aryl substitution then identified a 4′-CN group that improved the human/rodent correlation in microsomal metabolic stability. Our lead molecule is very potent in PK/PD assays and highly efficacious in a mouse collagen-induced arthritis model.

Published

2017

16. Discovery of highly potent, selective, covalent inhibitors of JAK3

Author

Jingwu Duan, Stephen T. Wrobleski, Joel C. Barrish, Jagabandhu Das, Gary L. Schieven, Steven H. Spergel, Charu Chaudhry, Percy H. Carter, John S. Tokarski, Damaso Ovalle, John S. Sack, Aberra Fura, Zhonghui Lu, James Kempson, Luisa Salter-Cid, William J. Pitts, Junqing Guo, Yuval Blatt, John Hynes, Shuqun Lin, Hong Wu, Bin Jiang, Bingwei V. Yang, and Javed Khan

Subjects

0301 basic medicine, Stereochemistry, Cell Survival, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Crystal structure, Biochemistry, Active site cysteine, Cell Line, 03 medical and health sciences, Residue (chemistry), Inhibitory Concentration 50, Structure-Activity Relationship, Catalytic Domain, Drug Discovery, Molecule, Humans, Molecular Biology, Protein Kinase Inhibitors, Binding Sites, Chemistry, Organic Chemistry, Janus Kinase 3, Janus Kinase 1, Janus Kinase 2, Combinatorial chemistry, Molecular Docking Simulation, 030104 developmental biology, Covalent bond, Electrophile, Molecular Medicine

Abstract

A useful and novel set of tool molecules have been identified which bind irreversibly to the JAK3 active site cysteine residue. The design was based on crystal structure information and a comparative study of several electrophilic warheads.

Published

2017

17. Discovery of potent and efficacious pyrrolopyridazines as dual JAK1/3 inhibitors

Author

Sidney Pitt, Sylwia Stachura, Rosemary Zhang, Steven G. Nadler, Kim W. McIntyre, Hong Wu, James Kempson, Jonathan Lippy, John Hynes, Joel C. Barrish, Zhonghui Lu, Percy H. Carter, Gary L. Schieven, Bin Jiang, Kate Gillooly, William J. Pitts, Javed Khan, Stephen T. Wrobleski, Jingwu Duan, Aberra Fura, Guoxiang Shen, John S. Tokarski, John S. Sack, and Luisa Salter-Cid

Subjects

0301 basic medicine, Clinical Biochemistry, Drug Evaluation, Preclinical, Molecular Conformation, Pharmaceutical Science, Pharmacology, Crystallography, X-Ray, 01 natural sciences, Biochemistry, Rats, Sprague-Dawley, chemistry.chemical_compound, Mice, Catalytic Domain, Drug Discovery, Mice, Inbred BALB C, biology, Chemistry, Translation (biology), Pyridazines, Tyrosine kinase 2, Molecular Medicine, Half-Life, hERG, Molecular Dynamics Simulation, Pyrrolopyridazine, Cell Line, 03 medical and health sciences, Inhibitory Concentration 50, Structure-Activity Relationship, In vivo, Potency, Animals, Humans, Pyrroles, Molecular Biology, Protein Kinase Inhibitors, Inflammation, TYK2 Kinase, Binding Sites, 010405 organic chemistry, Aryl, Organic Chemistry, Janus Kinase 3, Janus Kinase 1, Janus Kinase 2, 0104 chemical sciences, Rats, Disease Models, Animal, 030104 developmental biology, Murine model, biology.protein

Abstract

A series of potent dual JAK1/3 inhibitors have been developed from a moderately selective JAK3 inhibitor. Substitution at the C6 position of the pyrrolopyridazine core with aryl groups provided exceptional biochemical potency against JAK1 and JAK3 while maintaining good selectivity against JAK2 and Tyk2. Translation to in vivo efficacy was observed in a murine model of chronic inflammation. X-ray co-crystal structure determination confirmed the presumed inhibitor binding orientation in JAK3. Efforts to reduce hERG channel inhibition will be described.

Published

2017

18. Hepatitis C Virus NS5A Replication Complex Inhibitors: The Discovery of Daclatasvir

Author

Donald R. O'Boyle, Anjaneya Chimalakonda, Benjamin M. Johnson, Lavoie Rico, Alain Martel, James Clint A, Denis R. St. Laurent, Julie A. Lemm, Van N. Nguyen, David R. Langley, Henry S. Wong, Fukang Yang, Robert A. Fridell, Deon Daniel H, Juliang Zhu, Glenn H. Cantor, Lawrence B. Snyder, Jeffrey L. Romine, Makonen Belema, Lopez Omar D, Kenneth S. Santone, Carol Bachand, Goodrich Jason, Ruediger Edward H, Richard J. Colonno, Stephen P. Adams, Nicholas A. Meanwell, Min Gao, Aberra Fura, Lawrence G. Hamann, Dawn D. Parker, and Jay O. Knipe

Subjects

Spectrometry, Mass, Electrospray Ionization, Magnetic Resonance Spectroscopy, Pyrrolidines, Daclatasvir, Hepatitis C virus, Hepacivirus, Viral Nonstructural Proteins, Pharmacology, Virus Replication, medicine.disease_cause, Antiviral Agents, Structure-Activity Relationship, Dogs, Pharmacokinetics, Drug Discovery, medicine, Animals, Structure–activity relationship, Replicon, Enzyme Inhibitors, NS5A, EC50, Chemistry, Drug discovery, Imidazoles, Valine, Virology, Rats, Area Under Curve, Molecular Medicine, Carbamates, medicine.drug

Abstract

The biphenyl derivatives 2 and 3 are prototypes of a novel class of NS5A replication complex inhibitors that demonstrate high inhibitory potency toward a panel of clinically relevant HCV strains encompassing genotypes 1-6. However, these compounds exhibit poor systemic exposure in rat pharmacokinetic studies after oral dosing. The structure-activity relationship investigations that improved the exposure properties of the parent bis-phenylimidazole chemotype, culminating in the identification of the highly potent NS5A replication complex inhibitor daclatasvir (33) are described. An element critical to success was the realization that the arylglycine cap of 2 could be replaced with an alkylglycine derivative and still maintain the high inhibitory potency of the series if accompanied with a stereoinversion, a finding that enabled a rapid optimization of exposure properties. Compound 33 had EC50 values of 50 and 9 pM toward genotype-1a and -1b replicons, respectively, and oral bioavailabilities of 38-108% in preclinical species. Compound 33 provided clinical proof-of-concept for the NS5A replication complex inhibitor class, and regulatory approval to market it with the NS3/4A protease inhibitor asunaprevir for the treatment of HCV genotype-1b infection has recently been sought in Japan.

Published

2014

19. Small Molecule Reversible Inhibitors of Bruton's Tyrosine Kinase (BTK): Structure-Activity Relationships Leading to the Identification of 7-(2-Hydroxypropan-2-yl)-4-[2-methyl-3-(4-oxo-3,4-dihydroquinazolin-3-yl)phenyl]-9H-carbazole-1-carboxamide (BMS-935177)

Author

Tracy L. Taylor, Douglas G. Batt, Lorell Discenza, ChiehYing J. Chang, Luisa Salter-Cid, Kim W. McIntyre, Myra Beaudoin Bertrand, Percy H. Carter, Yingru Zhang, Qingjie Liu, James R. Burke, Andrew J. Tebben, Zheng Yang, Joel C. Barrish, Rick Rampulla, Aberra Fura, Daniel W. Kukral, Joseph A. Tino, Punit Marathe, Huiping Zhang, Jun Dai, Qing Shi, Arvind Mathur, Kathleen M. Gillooly, Mark A. Pattoli, Mary T. Obermeier, Stacey Skala, Jodi K. Muckelbauer, George V. De Lucca, Rodney Vickery, and Celia D’Arienzo

Subjects

0301 basic medicine, medicine.drug_class, Stereochemistry, Carbazoles, Administration, Oral, Biological Availability, Carboxamide, Crystallography, X-Ray, Permeability, Cell Line, Arthritis, Rheumatoid, 03 medical and health sciences, chemistry.chemical_compound, Mice, Structure-Activity Relationship, 0302 clinical medicine, Dogs, In vivo, Drug Discovery, medicine, Agammaglobulinaemia Tyrosine Kinase, Bruton's tyrosine kinase, Structure–activity relationship, Animals, Humans, Quinazolinones, biology, Carbazole, Protein-Tyrosine Kinases, Small molecule, Arthritis, Experimental, Macaca fascicularis, 030104 developmental biology, chemistry, Cell culture, 030220 oncology & carcinogenesis, Antirheumatic Agents, biology.protein, Microsomes, Liver, Molecular Medicine, Tyrosine kinase

Abstract

Bruton’s tyrosine kinase (BTK) belongs to the TEC family of nonreceptor tyrosine kinases and plays a critical role in multiple cell types responsible for numerous autoimmune diseases. This article will detail the structure–activity relationships (SARs) leading to a novel second generation series of potent and selective reversible carbazole inhibitors of BTK. With an excellent pharmacokinetic profile as well as demonstrated in vivo activity and an acceptable safety profile, 7-(2-hydroxypropan-2-yl)-4-[2-methyl-3-(4-oxo-3,4-dihydroquinazolin-3-yl)phenyl]-9H-carbazole-1-carboxamide 6 (BMS-935177) was selected to advance into clinical development.

Published

2016

20. Discovery of 6-(Aminomethyl)-5-(2,4-dichlorophenyl)-7-methylimidazo[1,2-a]pyrimidine-2-carboxamides as Potent, Selective Dipeptidyl Peptidase-4 (DPP4) Inhibitors

Author

Yaqun Zhang, Dianlin Xie, Kevin Kish, Aiying Wang, Stephen P. O'connor, Wei Meng, Herbert E. Klei, Huji Turdi, Lawrence G. Hamann, Robert Zahler, Jovita Marcinkeviciene, Robert Paul Brigance, Thomas Harrity, James K. Tamura, Aberra Fura, Carolyn A. Weigelt, Chao Hannguang J, and Mark S. Kirby

Subjects

Male, Models, Molecular, ERG1 Potassium Channel, Pyrimidine, Stereochemistry, Dipeptidyl Peptidase 4, hERG, Mice, Obese, Crystallography, X-Ray, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Dogs, Catalytic Domain, Amide, Drug Discovery, Hydrolase, Animals, Humans, Hypoglycemic Agents, Imidazole, Dipeptidyl peptidase-4, Dipeptidyl-Peptidase IV Inhibitors, biology, Aryl, Imidazoles, Active site, Stereoisomerism, Ether-A-Go-Go Potassium Channels, Rats, Pyrimidines, Diabetes Mellitus, Type 2, chemistry, biology.protein, Molecular Medicine, Sodium Channel Blockers

Abstract

Continued structure-activity relationship (SAR) exploration within our previously disclosed azolopyrimidine containing dipeptidyl peptidase-4 (DPP4) inhibitors led us to focus on an imidazolopyrimidine series in particular. Further study revealed that by replacing the aryl substitution on the imidazole ring with a more polar carboxylic ester or amide, these compounds displayed not only increased DPP4 binding activity but also significantly reduced human ether-a-go-go related gene (hERG) and sodium channel inhibitory activities. Additional incremental adjustment of polarity led to permeable molecules which exhibited favorable pharmacokinetic (PK) profiles in preclinical animal species. The active site binding mode of these compounds was determined by X-ray crystallography as exemplified by amide 24c. A subsequent lead molecule from this series, (+)-6-(aminomethyl)-5-(2,4-dichlorophenyl)-N-(1-ethyl-1H-pyrazol-5-yl)-7-methylimidazo[1,2-a]pyrimidine-2-carboxamide (24s), emerged as a potent, selective DPP4 inhibitor that displayed excellent PK profiles and in vivo efficacy in ob/ob mice.

Published

2010

21. N-Aryl-oxazolidin-2-imine Muscle Selective Androgen Receptor Modulators Enhance Potency through Pharmacophore Reorientation

Author

Stanley R. Krystek, Donald Egan, John S. Sack, Joyce E. Kuhns, Alexandra A. Nirschl, Gary J. Grover, Rajasree Golla, John A. Lupisella, James A. Bryson, John D. Dimarco, Jack Z. Gougoutas, Ligaya M. Simpkins, Aberra Fura, Jacek Ostrowski, Yan Zou, Yi-Xin Li, Robert Zahler, Yongmi An, James C. Sutton, Kevin Kish, Viral Vyas, Lawrence G. Hamann, Ramakrishna Seethala, Paul G. Sleph, and Blake C. Beehler

Subjects

Male, Models, Molecular, Stereochemistry, Imine, Molecular Conformation, Crystallography, X-Ray, Substrate Specificity, chemistry.chemical_compound, Drug Discovery, Animals, Humans, Potency, Oxazoles, Chemistry, Muscles, Aryl, Prostate, Hydrogen-Ion Concentration, In vitro, Rats, Bioavailability, Androgen receptor, Selective androgen receptor modulator, Androgens, Molecular Medicine, Pharmacophore

Abstract

A novel selective androgen receptor modulator (SARM) scaffold was discovered as a byproduct obtained during synthesis of our earlier series of imidazolidin-2-ones. The resulting oxazolidin-2-imines are among the most potent SARMs known, with many analogues exhibiting sub-nM in vitro potency in binding and functional assays. Despite the potential for hydrolytic instability at gut pH, compounds of the present class showed good oral bioavailability and were highly active in a standard rodent pharmacological model.

Published

2009

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

Author

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

Subjects

Male, Models, Molecular, Bicalutamide, medicine.drug_class, Stereochemistry, Clinical Biochemistry, Administration, Oral, Pharmaceutical Science, Isoindoles, Pharmacology, Antiandrogen, Biochemistry, Tosyl Compounds, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Prostate cancer, In vivo, Nitriles, Drug Discovery, Androgen Receptor Antagonists, Tumor Cells, Cultured, medicine, Animals, Humans, Anilides, Imide, Molecular Biology, Chromatography, High Pressure Liquid, Mice, Inbred BALB C, Molecular Structure, Organic Chemistry, Prostatic Neoplasms, Androgen Antagonists, Bridged Bicyclo Compounds, Heterocyclic, medicine.disease, Androgen receptor, chemistry, Receptors, Androgen, Drug Design, Molecular Medicine, Lead compound, Protein Binding, medicine.drug

Abstract

A novel series of [2.2.1]-oxabicyclo imide-based compounds were identified as potent antagonists of the androgen receptor. Molecular modeling and iterative drug design were applied to optimize this series. The lead compound [3aS-(3aalpha,4beta,5beta,7beta,7aalpha)]-4-(octahydro-5-hydroxy-4,7-dimethyl-1,3-dioxo-4,7-epoxy-2H-isoindol-2-yl)-2-iodobenzonitrile was shown to have potent in vivo efficacy after oral dosing in the CWR22 human prostate tumor xenograph model.

Published

2008

23. Discovery of Potent and Muscle Selective Androgen Receptor Modulators through Scaffold Modifications

Author

Aberra Fura, James J. Li, Chongqing Sun, Jack Z. Gougoutas, Cindy Y. Li, Gary J. Grover, Viral Vyas, Robert Zahler, Lawrence G. Hamann, Michael Galella, Haixia Wang, Stanley R. Krystek, Alexandra A. Nirschl, Zulan Pi, Rebecca Johnson, Jacek Ostrowski, Blake C. Beehler, Ramakrishna Seethala, Rajasree Golla, James C. Sutton, Yan Zou, and Paul G. Sleph

Subjects

Male, Models, Molecular, medicine.medical_specialty, Administration, Oral, Biological Availability, Crystallography, X-Ray, Anabolic Agents, Muscle hypertrophy, Structure-Activity Relationship, chemistry.chemical_compound, Prostate, In vivo, Internal medicine, Drug Discovery, medicine, Animals, Structure–activity relationship, Pyrroles, Muscle, Skeletal, Chemistry, Imidazoles, Stereoisomerism, Rats, Androgen receptor, Endocrinology, medicine.anatomical_structure, Selective androgen receptor modulator, Receptors, Androgen, Molecular Medicine, Orchiectomy, Lead compound, Half-Life

Abstract

A novel series of imidazolin-2-ones were designed and synthesized as highly potent, orally active and muscle selective androgen receptor modulators (SARMs), with most of the compounds exhibiting low nM in vitro potency in androgen receptor (AR) binding and functional assays. Once daily oral treatment with the lead compound 11a (AR Ki = 0.9 nM, EC50 = 1.8 nM) for 14 days induced muscle growth with an ED50 of 0.09 mg/kg, providing approximately 50-fold selectivity over prostate growth in an orchidectomized rat model. Pharmacokinetic studies in rats demonstrated that the lead compound 11a had oral bioavailability of 65% and a plasma half-life of 5.5 h. On the basis of their preclinical profiles, the SARMs in this series are expected to provide beneficial anabolic effects on muscle with minimal androgenic effects on prostate tissue.

Published

2007

24. Pharmacological and X-Ray Structural Characterization of a Novel Selective Androgen Receptor Modulator: Potent Hyperanabolic Stimulation of Skeletal Muscle with Hypostimulation of Prostate in Rats

Author

Kevin Kish, Gary J. Grover, Jacek Ostrowski, Joyce E. Kuhns, Kasim A. Mookhtiar, Rajasree Golla, Chongqing Sun, John A. Lupisella, John S. Sack, Yingzhi Bi, Aberra Fura, Stanley R. Krystek, Lawrence G. Hamann, Mark C. Manfredi, Paul G. Sleph, Yongmi An, Ramakrishna Seethala, and Blake C. Beehler

Subjects

Male, Agonist, Aging, medicine.medical_specialty, Transcription, Genetic, medicine.drug_class, medicine.medical_treatment, Biology, Crystallography, X-Ray, Ligands, Binding, Competitive, Article, Rats, Sprague-Dawley, Aromatase, Endocrinology, Cell Line, Tumor, Internal medicine, medicine, Animals, Humans, Pyrroles, Testosterone, Muscle, Skeletal, Receptor, Imidazoles, Prostate, Skeletal muscle, Dihydrotestosterone, Epithelial Cells, Luteinizing Hormone, Androgen, Protein Structure, Tertiary, Rats, Androgen receptor, Steroid hormone, medicine.anatomical_structure, Selective androgen receptor modulator, Receptors, Androgen, Orchiectomy, Cell Division

Abstract

A novel, highly potent, orally active, nonsteroidal tissue selective androgen receptor (AR) modulator (BMS-564929) has been identified, and this compound has been advanced to clinical trials for the treatment of age-related functional decline. BMS-564929 is a subnanomolar AR agonist in vitro, is highly selective for the AR vs. other steroid hormone receptors, and exhibits no significant interactions with SHBG or aromatase. Dose response studies in castrated male rats show that BMS-564929 is substantially more potent than testosterone (T) in stimulating the growth of the levator ani muscle, and unlike T, highly selective for muscle vs. prostate. Key differences in the binding interactions of BMS-564929 with the AR relative to the native hormones were revealed through x-ray crystallography, including several unique contacts located in specific helices of the ligand binding domain important for coregulatory protein recruitment. Results from additional pharmacological studies effectively exclude alternative mechanistic contributions to the observed tissue selectivity of this unique, orally active androgen. Because concerns regarding the potential hyperstimulatory effects on prostate and an inconvenient route of administration are major drawbacks that limit the clinical use of T, the potent oral activity and tissue selectivity exhibited by BMS-564929 are expected to yield a clinical profile that provides the demonstrated beneficial effects of T in muscle and other tissues with a more favorable safety window.

Published

2007

25. Role of pharmacologically active metabolites in drug discovery and development

Author

Aberra Fura

Subjects

Drug, media_common.quotation_subject, Metabolite, Pharmacology, Structure-Activity Relationship, chemistry.chemical_compound, Pharmacokinetics, Drug Discovery, Medicine, Pharmaceutical sciences, Adverse effect, Biotransformation, Active metabolite, media_common, business.industry, Drug discovery, fungi, food and beverages, Pharmaceutical Preparations, Mechanism of action, chemistry, Drug Design, medicine.symptom, business

Abstract

Pharmacologically active metabolites can contribute significantly to the overall therapeutic and adverse effects of drugs. Therefore, to fully understand the mechanism of action of drugs, it is important to recognize the role of active metabolites. Active metabolites can also be developed as drugs in their own right. Using illustrative examples, this paper discusses a variety of biotransformation reactions that produce active metabolites and their structure-activity relationships. The paper also describes the role and significance of active metabolites in drug discovery and development, various experimental observations that can be used as indicators of their presence, and methods that can be used to assess their biological activities and contribution to the overall therapeutic and adverse effects of drugs.

Published

2006

26. Design, Synthesis, and Evaluation of Orally Active 4-(2,4-Difluoro-5-(methoxycarbamoyl)phenylamino)pyrrolo[2,1-f][1,2,4]triazines as Dual Vascular Endothelial Growth Factor Receptor-2 and Fibroblast Growth Factor Receptor-1 Inhibitors

Author

Joseph Fargnoli, Daniel W. Kukral, Steve Mortillo, Viral Vyas, John S. Tokarski, John T. Hunt, Robert M. Borzilleri, Rajeev S. Bhide, Robert Jeyaseelan, Louis J. Lombardo, Amrita Kamath, Xiaoping Zheng, Ligang Qian, Barri Wautlet, Zhen-Wei Cai, Joel C. Barrish, Aberra Fura, and Christopher D. Ellis

Subjects

Male, Models, Molecular, Stereochemistry, Administration, Oral, Biological Availability, Mice, Nude, Antineoplastic Agents, In Vitro Techniques, Hydroxamic Acids, Fibroblast growth factor, Chemical synthesis, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Growth factor receptor, Drug Discovery, Animals, Humans, Pyrroles, Receptor, Fibroblast Growth Factor, Type 1, Cell Proliferation, Mice, Inbred BALB C, Oxadiazoles, Hydroxamic acid, Triazines, Fibroblast growth factor receptor 1, Receptor Protein-Tyrosine Kinases, Kinase insert domain receptor, Blood Proteins, Receptors, Fibroblast Growth Factor, Vascular Endothelial Growth Factor Receptor-2, Xenograft Model Antitumor Assays, chemistry, Drug Design, Microsomes, Liver, Molecular Medicine, Human umbilical vein endothelial cell, Endothelium, Vascular, Tyrosine kinase, Protein Binding

Abstract

A series of substituted 4-(2,4-difluoro-5-(methoxycarbamoyl)phenylamino)pyrrolo[2,1-f][1,2,4]triazines was identified as potent and selective inhibitors of the tyrosine kinase activity of the growth factor receptors VEGFR-2 (Flk-1, KDR) and FGFR-1. The enzyme kinetics associated with the VEGFR-2 inhibition of compound 50 (K(i) = 52 +/- 3 nM) confirmed that the pyrrolo[2,1-f][1,2,4]triazine analogues are competitive with ATP. Several analogues demonstrated low-nanomolar inhibition of VEGF- and FGF-dependent human umbilical vein endothelial cell (HUVEC) proliferation. Replacement of the C6-ester substituent of the pyrrolo[2,1-f][1,2,4]triazine core with heterocyclic bioisosteres, such as substituted 1,3,5-oxadiazoles, afforded compounds with excellent oral bioavailability in mice (i.e., 50 F(po) = 79%). Significant antitumor efficacy was observed with compounds 44, 49, and 50 against established L2987 human lung carcinoma xenografts implanted in athymic mice. A full account of the synthesis, structure-activity relationships, pharmacology, and pharmacokinetic properties of analogues within the series is presented.

Published

2005

27. Shift in pH of biological fluids during storage and processing: effect on bioanalysis

Author

Timothy W. Harper, Wen Chyi Shyu, Lawrence K. Fung, Aberra Fura, and Hongjian Zhang

Subjects

Time Factors, Metabolite, Clinical Biochemistry, Pharmaceutical Science, Buffers, Urine, High-performance liquid chromatography, Mass Spectrometry, Specimen Handling, Analytical Chemistry, chemistry.chemical_compound, In vivo, Drug Discovery, Blood plasma, Animals, Bile, Centrifugation, Lung, Chromatography, High Pressure Liquid, Spectroscopy, Chromatography, Methanol, Hydrogen-Ion Concentration, Reference Standards, Phosphate, Blood proteins, Body Fluids, Rats, chemistry, Solvents, Indicators and Reagents, Digestive System, Ex vivo

Abstract

The pH of ex vivo plasma, bile and urine was monitored at different times and temperatures of storage, and following different sample processing methods such as ultrafiltration, centrifugation, precipitation and evaporation. The results showed that the pH of ex vivo plasma, bile and urine increased upon storage, and following sample processing and could lead to significant degradation of pH-labile compounds. Several compounds were used to illustrate the impact of pH shifts on drug stability and interpretation of results obtained from in vivo studies. For example, after 1 h of incubation (37 degrees C) in rat plasma (pH 8.3), about 60%, of I was lost. However, in phosphate buffer, losses were about 12% at pH 7.4 and 40% at pH 8.0. Plasma pH also increased during ultrafiltration, centrifugation and extraction. After methanol precipitation of plasma proteins, and evaporation of the supernatant and redissolution of the residue, the resulting solution had a pH of 9.5. Under these conditions, II was degraded by 60% but was stable when phosphate buffer was used to maintain the pH at 7.4. The shift in plasma pH can yield misleading results from in vivo studies if the pH is not controlled. For example, the major circulating metabolite of II was also formed in plasma ex-vivo. This ex vivo degradation was prevented when blood samples were collected into tubes containing 0.1 volume of phosphate buffer (0.3 M, pH 5). The pH of ex vivo plasma can best be stabilized at physiological conditions using 10% CO2 atmosphere in a CO2 incubator. Changes in pH of ex vivo urine and bile samples can have similar adverse effect on pH-labile samples. Thus, processing of plasma samples under a 10% CO2 atmosphere is a method of choice for stability or protein binding studies in plasma, whereas citrate or phosphate buffers are suitable for stabilizing pH in bile and urine and for plasma samples requiring extensive preparations or long term storage.

Published

2003

28. Small carbon clusters (Cn0, Cn+, Cn−) from acyclic and cyclic precursors

Author

František Tureček, Aberra Fura, and Fred W. McLafferty

Subjects

Chemistry, Ab initio, Condensed Matter Physics, Dissociation (chemistry), Standard enthalpy of formation, Crystallography, Computational chemistry, Ionization, Mass spectrum, Molecule, Density functional theory, Physical and Theoretical Chemistry, Ionization energy, Instrumentation, Spectroscopy

Abstract

Dissociative ionization of several linear, cyclic, and branched molecules was used to generate C 3 + and C 4 + carbon clusters. However, mass spectra from collisionally activated dissociation (CAD) and neutralization–reionization (NR) under a wide variety conditions were indistinguishable, indicating only one isomer or same mixture of isomers. Likewise, CAD and NR spectra of C 4 + and C 3 + from 13 CH 2 CHCH 13 CH 2 and CH 3  13 C CH 2 show complete 12 C / 13 C scrambling. CAD cross sections are consistent with C 4 + –C 6 + ions as mainly linear isomers and C 7 + ions from cyclic precursors as mainly cyclic. CCSD(T) ab initio and B3LYP density functional theory calculations with large basis sets yielded structures and energies for a variety of cationic, neutral, and anionic carbon clusters and transition states for some cationic rearrangements. The calculated enthalpies of formation, dissociation energies, ionization energies, and electron affinities mostly agree with currently accepted experimental data. However, CCSD(T) calculations indicate adiabatic ionization energies for C 3 (11.79 eV) and C 4 isomers (10.48, 10.82, and 10.86 eV) that differ >1 eV from recent measurements.

Published

2002

29. Synthesis of CMI-977, a Potent 5-Lipoxygenase Inhibitor

Author

C. Grace Yeh, Raju Penmasta, Zhengzhe Song, Liang Guo, James P. Staszewski, Robert M. Moriarty, Sanmin Yang, Xiong Cai, and Michelle A. Young, Ralph Scannell, Karen A. Jauregui, Shaoxia Yu, and Sudersan M. Tuladhar, Aberra Fura, Heather A. Lounsbury, Munagala S. Rao, Rajesh K. Singhal, Gurmit S. Grewal, and Mukund S. Chorghade

Subjects

Chronic asthma, Chemistry, Stereochemistry, Organic Chemistry, 5-Lipoxygenase Inhibitor, Biological activity, Physical and Theoretical Chemistry, Enantiomer

Abstract

CMI-977 is a potent 5-lipoxygenase inhibitor that intervenes in the production of leukotrienes and is presently being developed for the treatment of chronic asthma. It is a single enantiomer with an all-trans (2S,5S) configuration. Of the four isomers of CMI-977, the S,S isomer was found to have the best biological activity and was selected for further development. The enantiomerically pure product was synthesized on a 2-kg scale from (S)-(+)-hydroxymethyl-γ-butyrolactone.

Published

1998

30. Optimization of activity, selectivity, and liability profiles in 5-oxopyrrolopyridine DPP4 inhibitors leading to clinical candidate (Sa)-2-(3-(aminomethyl)-4-(2,4-dichlorophenyl)-2-methyl-5-oxo-5H-pyrrolo[3,4-b]pyridin-6(7H)-yl)-N,N-dimethylacetamide (BMS-767778)

Author

Carolyn A. Weigelt, John M. Fevig, Wei Wang, Paul Levesque, Frederic Moulin, T. W. Harrity, Lawrence G. Hamann, Herbert E. Klei, Don Egan, Robert Zahler, Lucy Sun, Jianxin Feng, Pratik Devasthale, Michael Cap, Ying Wang, Mark S. Kirby, Nathan Morgan, Yi-Xin Li, Aiying Wang, Kevin Kish, and Aberra Fura

Subjects

Male, Models, Molecular, Stereochemistry, Dipeptidyl Peptidase 4, Dimethylacetamide, Substrate Specificity, chemistry.chemical_compound, Mice, Bridged Bicyclo Compounds, Catalytic Domain, Drug Discovery, Hydrolase, Acetamides, Animals, Humans, Pyrroles, skin and connective tissue diseases, Dipeptidyl-Peptidase IV Inhibitors, Bicyclic molecule, fungi, Glucose Tolerance Test, Bridged Bicyclo Compounds, Heterocyclic, body regions, chemistry, Drug Design, Molecular Medicine, Substrate specificity, Selectivity

Abstract

Optimization of a 5-oxopyrrolopyridine series based upon structure-activity relationships (SARs) developed from our previous efforts on a number of related bicyclic series yielded compound 2s (BMS-767778) with an overall activity, selectivity, efficacy, PK, and developability profile suitable for progression into the clinic. SAR in the series and characterization of 2s are described.

Published

2013

31. Attribution of the discrepancy between ELISA and LC-MS/MS assay results of a PEGylated scaffold protein in post-dose monkey plasma samples due to the presence of anti-drug antibodies

Author

Aberra Fura, Guodong Chen, Adrienne A. Tymiak, David B. Wang-Iverson, Russell Weiner, Shujie J. Wang, Murli Krishna, Timothy V Olah, Karen Price, Paul E. Morin, Steven T. Wu, Jochem Gokemeijer, and Mohammed Jemal

Subjects

Drug, Bioanalysis, medicine.drug_class, media_common.quotation_subject, Enzyme-Linked Immunosorbent Assay, Antigen-Antibody Complex, Monoclonal antibody, Biochemistry, Antibodies, Analytical Chemistry, Polyethylene Glycols, Pharmacokinetics, Western blot, Tandem Mass Spectrometry, medicine, Animals, media_common, Chromatography, biology, medicine.diagnostic_test, Chemistry, Proteins, Haplorhini, Epitope mapping, Pharmaceutical Preparations, biology.protein, Protein G, Antibody

Abstract

High-performance liquid chromatography–tandem mass spectrometry (LC-MS/MS) and enzyme-linked immunosorbent assay (ELISA) methods were developed for the quantification of a PEGylated scaffold protein drug in monkey plasma samples. The LC-MS/MS method was based on the extraction of the therapeutic protein with a water-miscible organic solvent and the subsequent trypsin digestion of the extract followed by the detection of a surrogate peptide. The assay was linear over a range of 10–3,000 ng/mL. The ELISA method utilized a therapeutic target-binding format in which the recombinant target antigen was used to capture the drug in the sample, followed by detection with an anti-PEG monoclonal antibody. The assay range was 30–2,000 ng/mL. A correlation study between the two methods was performed by measuring the drug concentrations in plasma samples from a single-dose pharmacokinetic (PK) study in cynomolgus monkeys following a 5-mg/kg subcutaneous administration (n = 4). In the early time points of the PK profile, the drug concentrations obtained by the LC-MS/MS method agreed very well with those obtained by the ELISA method. However, at later time points, the drug concentrations measured by the LC-MS/MS method were consistently higher than those measured by the ELISA method. The PK parameters calculated based on the concentration data showed that the two methods gave equivalent peak exposure (C max) at 24–48 h. However, the LC-MS/MS results exhibited about 1.53-fold higher total exposure (AUCtot) than the ELISA results. The discrepancy between the LC-MS/MS and ELISA results was investigated by conducting immunogenicity testing, anti-drug antibody (ADA) epitope mapping, and Western blot analysis of the drug concentrations coupled with Protein G separation. The results demonstrated the presence of ADA specific to the engineered antigen-binding region of the scaffold protein drug that interfered with the ability of the drug to bind to the target antigen used in the ELISA method. In the presence of the ADAs, the ELISA method measured only the active circulating drug (target-binding), while the LC-MS/MS method measured the total circulating drug. The work presented here indicates that the bioanalysis of protein drugs may be complicated owing to the presence of drug-binding endogenous components or ADAs in the post-dose (incurred) samples. The clear understanding of the behavior of different bioanalytical techniques vis-a-vis the potentially interfering components found in incurred samples is critical in selecting bioanalytical strategies for measuring protein drugs.

Published

2011

32. 7-Oxopyrrolopyridine-derived DPP4 inhibitors-mitigation of CYP and hERG liabilities via introduction of polar functionalities in the active site

Author

Aberra Fura, Carolyn A. Weigelt, Robert Zahler, Michael Cap, Herbert E. Klei, Yi-Xin Li, Paul Levesque, Aiying Wang, Mark S. Kirby, Nathan Morgan, Lawrence G. Hamann, Pratik Devasthale, T. W. Harrity, Don Egan, Kevin Kish, Lucy Sun, and Wei Wang

Subjects

Models, Molecular, Stereochemistry, Pyridines, Dipeptidyl Peptidase 4, Clinical Biochemistry, hERG, Pharmaceutical Science, Stereoisomerism, Biochemistry, Mice, Diabetes mellitus, Catalytic Domain, Drug Discovery, Insulin response, medicine, Diabetes Mellitus, Animals, Cytochrome P-450 CYP3A, Humans, Insulin, Pyrroles, Molecular Biology, Atropisomer, Dipeptidyl-Peptidase IV Inhibitors, Insulin blood, biology, Chemistry, Organic Chemistry, Active site, medicine.disease, Ether-A-Go-Go Potassium Channels, Rats, Mice, Inbred C57BL, biology.protein, Molecular Medicine, Insulin metabolism

Abstract

Design, synthesis, and SAR of 7-oxopyrrolopyridine-derived DPP4 inhibitors are described. The preferred stereochemistry of these atropisomeric biaryl analogs has been identified as Sa. Compound (+)-3t, with a K(i) against DPP4, DPP8, and DPP9 of 0.37 nM, 2.2, and 5.7 μM, respectively, showed a significant improvement in insulin response after single doses of 3 and 10 μmol/kg in ob/ob mice.

Published

2011

33. ChemInform Abstract: The Isomerization of Oxirane. Stable ×CH2OCH× 2, × CH2CH2O×, and :CHOCH3 and Their Counterpart Ions

Author

Chrysostomos Wesdemiotis, Aberra Fura, Fred W. McLafferty, and B. Leyh

Subjects

Chemistry, Organic chemistry, General Medicine, Photochemistry, Isomerization, Ion

Published

2010

34. ChemInform Abstract: Synthesis of CMI-977, a Potent 5-Lipoxygenase Inhibitor

Author

Young Michelle, Heather A. Lounsbury, Aberra Fura, Shaoxia Yu, Gurmit S. Grewal, Karen A. Jauregui, Ralph Scannell, Mukund S. Chorghade, C. Grace Yeh, and Xiong Cai

Subjects

Chemistry, 5-Lipoxygenase Inhibitor, General Medicine, Pharmacology

Published

2010

35. Synthesis and SAR of azolopyrimidines as potent and selective dipeptidyl peptidase-4 (DPP4) inhibitors for type 2 diabetes

Author

Aiying Wang, Robert Zahler, Aberra Fura, Mark S. Kirby, Robert Paul Brigance, Thomas Harrity, Wei Meng, and Lawrence G. Hamann

Subjects

Stereochemistry, Dipeptidyl Peptidase 4, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Chemical synthesis, Structure-Activity Relationship, Drug Discovery, Potency, Humans, Hypoglycemic Agents, Protease Inhibitors, Molecular Biology, Dipeptidyl peptidase-4, chemistry.chemical_classification, Bicyclic molecule, biology, Organic Chemistry, In vitro, Enzyme, Pyrimidines, chemistry, Diabetes Mellitus, Type 2, Enzyme inhibitor, biology.protein, Molecular Medicine, Selectivity

Abstract

Several pyrazolo-, triazolo-, and imidazolopyrimidines were synthesized and evaluated as inhibitors of DPP4. Of these three classes of compounds, the imidazolopyrimidines displayed the greatest potency and demonstrated excellent selectivity over the other dipeptidyl peptidases. SAR evaluation for these scaffolds was described as they may represent potential treatments for type 2 diabetes.

Published

2010

36. Pharmacokinetics of the dipeptidyl peptidase 4 inhibitor saxagliptin in rats, dogs, and monkeys and clinical projections

Author

Mark S. Kirby, David W. Boulton, Shu-Ying Chang, W. Griffith Humphreys, Viral Vyas, Lisa J. Christopher, Barry Koplowitz, Ashish Khanna, Aberra Fura, Lawrence G. Hamann, Kristina D. Chadwick, and Christian Caporuscio

Subjects

medicine.medical_specialty, Metabolic Clearance Rate, Metabolite, Drug Evaluation, Preclinical, Pharmaceutical Science, Biological Availability, Adamantane, Dipeptidyl peptidase-4 inhibitor, Biology, Saxagliptin, Rats, Sprague-Dawley, chemistry.chemical_compound, Dogs, Pharmacokinetics, Species Specificity, Internal medicine, medicine, Animals, Humans, Dipeptidyl peptidase-4, Pharmacology, Volume of distribution, Dipeptidyl-Peptidase IV Inhibitors, Dipeptides, Haplorhini, Bioavailability, Rats, Rats, Zucker, Endocrinology, chemistry, Pharmacodynamics, Microsomes, Liver, medicine.drug, Half-Life, Protein Binding

Abstract

Saxagliptin is a potent, selective, reversible dipeptidyl peptidase 4 (DPP4) inhibitor specifically designed for extended inhibition of the DPP4 enzyme and is currently under development for the treatment of type-2 diabetes. The pharmacokinetics of saxagliptin were evaluated in rats, dogs, and monkeys and used to predict its human pharmacokinetics. Saxagliptin was rapidly absorbed and had good bioavailability (50-75%) in the species tested. The plasma clearance of saxagliptin was higher in rats (115 ml/min/kg) than in dogs (9.3 ml/min/kg) and monkeys (14.5 ml/min/kg) and was predicted to be low to moderate in humans. The plasma elimination half-life was between 2.1 and 4.4 h in rats, dogs, and monkeys, and both metabolism and renal excretion contributed to the overall elimination. The primary metabolic clearance pathway involved the formation of a significant circulating, pharmacologically active hydroxylated metabolite, M2. The volume of distribution values observed in rats, dogs, and monkeys (1.3-5.2 l/kg) and predicted for humans (2.7 l/kg) were greater than those for total body water, indicating extravascular distribution. The in vitro serum protein binding was low (< or =30%) in rats, dogs, monkeys, and humans. After intra-arterial administration of saxagliptin to Sprague-Dawley and Zucker diabetic fatty rats, higher levels of saxagliptin and M2 were observed in the intestine (a proposed major site of drug action) relative to that in plasma. Saxagliptin has prolonged pharmacodynamic properties relative to its plasma pharmacokinetic profile, presumably due to additional contributions from M2, distribution of saxagliptin and M2 to the intestinal tissue, and prolonged dissociation of both saxagliptin and M2 from DPP4.

Published

2009

37. Angle-resolved neutralization-reionization mass spectrometry

Author

František Tureček, Aberra Fura, and Fred W. McLafferty

Subjects

Chemical ionization, Scattering, Analytical chemistry, Mass spectrometry, Ion, chemistry.chemical_compound, chemistry, Structural Biology, Hexene, Physics::Atomic and Molecular Clusters, Mass spectrum, Physics::Chemical Physics, Nuclear Experiment, Aliphatic compound, Reionization, Spectroscopy

Abstract

Neutralization -reionization mass spectra of 2-propenal, isomeric butenes, and isomeric n-hexenes have been found to depend significantly on the z-axis scattering angle of the neutralization event. As shown by Cooks for ion dissociations, increasing scattering angles generally favor products of higher activation-energy reactions. For isomeric butenes and n-hexenes, these reactions provide more definitive information for isomeric characterization.

Published

1991

38. Protonated ethanol and its neutral counterparts

Author

Chrysostomos Wesdemiotis, Aberra Fura, and Fred W. McLafferty

Subjects

Chemical ionization, Chemistry, Stereochemistry, 010401 analytical chemistry, Hypervalent molecule, Protonation, Primary alcohol, 010402 general chemistry, 01 natural sciences, Dissociation (chemistry), 0104 chemical sciences, 3. Good health, Ion, Crystallography, Structural Biology, Kinetic isotope effect, Mass spectrum, Spectroscopy

Abstract

Collisionally activated dissociation and neutralization-reionization experiments reveal that protonation of ethanol leads to two distinct isomers, the classical ion CH3CH2OH+2 and the proton-bound complex C2H4…H+…OH2. The neutral counterpart of the latter is unstable, whereas that of the former can be produced in a bound state if the CH3CH2OH+2 precursor ion is formed under low ion source pressure conditions and, thus, with higher internal energies. This suggests that there are substantial differences in the geometries of CH3CH2OH+2 and the hypervalent CH3CH2OH2 ·. This provides only a partial explanation for unusual isotope effects; C2H5OD2 ·, CH3CD2OD2 ·, and CD3CH2OD2 · are substantially more stable than C2D5OD2 · and C2H5OH2 ·.

Published

1991

39. Improved metal vapor neutralization and resolution in neutralization-reionization mass spectrometry

Author

Aberra Fura, Fred W. McLafferty, Mei-Yi Zhang, and Donald E. Drinkwater

Subjects

Chemistry, Analytical chemistry, Mass spectrometry, Biochemistry, Dissociation (chemistry), Neutralization, Ion, Ionization, Vaporization, Physics::Atomic and Molecular Clusters, Mass spectrum, Molecular Medicine, Ionization energy, Instrumentation, Spectroscopy

Abstract

Increased differential pumping improves the simultaneous sequential operation of ion-beam neutralization, neutral dissociation, neutral product ionization, and ion product dissociation for neutralization-reionization (NR) mass spectrometry. Following Porter's developments for neutralized ion-beam spectroscopy, instrument modifications allow a wider variety of metals (vaporization up to 800 °C) to be used for neutralization and eliminate multiplier instabilities seen previously using neutralization metals such as sodium. Irreproducibility of recovered precursor ion signals using metal vapors of low ionization potential has been traced to mercury background. Double focusing of the ionized neutral beam yields NR mass spectra of the highest resolution yet reported.

Published

1991

40. Prediction of human oral pharmacokinetics using nonclinical data: examples involving four proprietary compounds

Author

Aberra Fura, William G. Humphreys, Viral Vyas, Anjaneya Chimalokonda, and David Rodrigues

Subjects

Male, Metabolic Clearance Rate, Pharmaceutical Science, Administration, Oral, Biological Availability, Pharmacology, Absorption rate, Dogs, Pharmacokinetics, Metabolic clearance rate, Area under curve, Animals, Humans, Pharmacology (medical), Volume of distribution, Chromatography, Chemistry, General Medicine, Blood Proteins, Bioavailability, Rats, Macaca fascicularis, Area Under Curve, Steady state (chemistry), Biological availability, Protein Binding

Abstract

The oral pharmacokinetics (concentration-time profile) of four proprietary compounds in humans were predicted using the C(vss)-MRT method. The first step was to demonstrate superposition of intravenous (i.v.) pharmacokinetic profiles of preclinical species following mathematical transformation of their respective concentration-time curves using the corresponding C(vss) (where C(vss)=dose/Vss; Vss is the volume of distribution at steady state) and mean residence time (MRT) values. The resultant profiles were then back-transformed to estimate human i.v. plasma concentration-time profiles using human C(vss) and MRT values. Human C(vss) and MRT values were estimated from projected human Vss and CL values. Projection of CL was based on scaled (in vitro) metabolic clearance, simple allometry with and without various correction factors and the unbound fraction corrected intercept method. Vss values were estimated by allometric scaling with and without correction for interspecies differences in plasma protein binding. The predicted human i.v. profiles, in combination with the estimated mean absorption rate constants and bioavailability, were then used to simulate the oral pharmacokinetics in human using one- or multi-compartment kinetic models. Overall, with this approach, key oral pharmacokinetic parameters such as AUC, C(max), C(min) and oral plasma T((1/2)) were projected to be within two-fold of the actual values in humans.

Published

2008

41. The isomerization of oxirane. Stable .cntdot.CH2OCH2.cntdot., .cntdot.CH2CH2O.cntdot., and :CHOCH3, and their counterpart ions

Author

Bernard Leyh, Chrysostomos Wesdemiotis, Aberra Fura, and Fred W. McLafferty

Subjects

Chemical ionization, Stereochemistry, Cationic polymerization, Ether, General Chemistry, Biochemistry, Medicinal chemistry, Catalysis, Dissociation (chemistry), chemistry.chemical_compound, Colloid and Surface Chemistry, chemistry, Mass spectrum, Aliphatic compound, Isomerization, Carbene

Abstract

Unimolecular C-C bond rupture in oxirane leading to • CH 2 OCH 2 • is favored over C-O rupture to • CH 2 CH 2 O • , but the latter is the first-step in the lowest energy dissociation pathway through excited CH 3 CH=O to CH 3 • + • CHO. With collisional activation, • CH 2 OCH 2 • isomerizes mainly to oxirane, not methoxycarbene, :C(H)OCH 3 , while • CH 2 CH 2 O • isomerizes mainly to CH 3 CHO. All of these neutral isomers were prepared in the gas-phase via neutralization on the corresponding radical cations. Their structures, and those of their precursor cations, were established by collisionally activated dissociation (CAD), neutralization-anionization, and CAD of the mass-selected recovered molecular ions (MS/MS/MS) from neutralization-cationization. All of the neutrals and cationic isomers are found to represent stable bound structures, clarifying in particular previous contrary evidence concerning • CH 2 CH 2 O • , + CH 2 CH 2 O • , and the oxirane cation. Anionization showed the isomers • CH 2 CH 2 O − , −• C(H)OCH 3 , and −• C(OH)CH 3 to be stable

Published

1990

42. Abstract 5417: The identification of BMS-595, an orally active imidazo[1,2-b]pyridazine CK2 inhibitor with in vivo anti-tumor activity

Author

Joseph Fargnoli, Jonathan Lippy, Ashok V. Purandare, John T. Hunt, Libing Chen, Brian E. Fink, John S. Tokarski, Andrew Nation, Soong-Hoon Kim, Yufen Zhao, William R. Foster, Ashvinikumar V. Gavai, Tai W. Wong, Gregory D. Vite, Urvashi V. Roongta, Aberra Fura, Brent A. Rupnow, Jonathan G. Pabalan, Benjamin J. Henley, Christine M. Tarby, Mary T. Obermeier, Chiang Yu, Liqi He, and Paul A. Elzinga

Subjects

chemistry.chemical_classification, Cancer Research, biology, Chemistry, Kinase, CREB, Serine, Enzyme, Oncology, In vivo, RNA interference, biology.protein, Cancer research, Signal transduction, Transcription factor

Abstract

CK2 is a highly conserved, and constitutively active family of serine/threonine kinases abnormally elevated in a wide variety of cancers and linked to poor prognosis and disease progression. The enzymes form as hetero-tetrameric complexes comprised of two highly related catalytic subunits (α or α´) with two regulatory β subunits in various combinations and distributions, depending on cell type. While CK2 plays a role in normal growth and development, deregulation of the enzymes has been shown to promote and maintain a malignant phenotype through mechanisms in both the anti-apoptotic and the pro-proliferative signaling pathways. CK2 has been reported to modulate the activity of several oncogenic transcription factors including CREB, Myc, Jun and Fos. Studies with RNAi and small molecule compounds have demonstrated tumor cell dependence on CK2. We sought to identify potent CK2 inhibitors to probe the function of CK2 in cancer-linked pathways and for evaluation in CK2 dependent tumor xenograft models. Herein we report SAR studies in the imidazo[1,2-b]pyridazine chemotype leading to the discovery of BMS-595, a highly potent and selective ATP-competitive CK2 inhibitor with a commensurate level of cellular potency. BMS-595 demonstrates strong PK/PD correlations and robust, oral anti-tumor efficacy in CK2-driven xenograft models at tolerated doses. Citation Format: Christine M. Tarby, Liqi He, Brian E. Fink, Andrew Nation, Yufen Zhao, Soong-Hoon Kim, Libing Chen, John S. Tokarski, Chiang Yu, Jonathan G. Pabalan, Urvashi V. Roongta, Jonathan Lippy, Mary Obermeier, Paul A. Elzinga, Aberra Fura, Benjamin Henley, Joseph J. Fargnoli, William R. Foster, Ashvinikumar V. Gavai, Tai W. Wong, John T. Hunt, Gregory D. Vite, Ashok V. Purandare, Brent A. Rupnow. The identification of BMS-595, an orally active imidazo[1,2-b]pyridazine CK2 inhibitor with in vivo anti-tumor activity. [abstract]. In: Proceedings of the 106th Annual Meeting of the American Association for Cancer Research; 2015 Apr 18-22; Philadelphia, PA. Philadelphia (PA): AACR; Cancer Res 2015;75(15 Suppl):Abstract nr 5417. doi:10.1158/1538-7445.AM2015-5417

Published

2015

43. Abstract 5395: Anti-tumor activity of BMS-595, a novel CK2 kinase inhibitor

Author

Gregory D. Vite, Aberra Fura, William R. Foster, Brian E. Fink, Jonathan Lippy, Tai W. Wong, Urvashi V. Roongta, Ashok Dongre, Chiang Yu, Ashvinikumar V. Gavai, John T. Hunt, John S. Tokarski, Ashok V. Purandare, Joseph Fargnoli, Paul A. Elzinga, Brent A. Rupnow, Jonathan G. Pabalan, Benjamin J. Henley, Christine M. Tarby, Mary T. Obermeier, and Francis Y. Lee

Subjects

Cancer Research, MAP kinase kinase kinase, Kinase, Cyclin-dependent kinase 2, Mitogen-activated protein kinase kinase, Biology, medicine.disease, Oncology, TANK-binding kinase 1, Cancer research, biology.protein, medicine, Cyclin-dependent kinase 9, Kinase activity, Lung cancer

Abstract

The CK2 protein kinases are a small family of two highly related serine/threonine kinases composed of two catalytic subunits, α and α’, and a single β subunit. Numerous substrates have been reported for CK2 and these proteins are known to participate in diverse cellular processes, including cell signaling, transcription, DNA repair, apoptosis regulation and tumor suppression. Elevated CK2 expression and kinase activity has been observed in many cancer types. Further, mRNA knockdown and enzyme inhibition studies have demonstrated that many cancer cell lines are dependent on CK2 for growth and survival. To further evaluate CK2 kinases as targets for therapeutic intervention in cancer, we identified BMS-595, a potent and selective, ATP-competitive CK2 inhibitor. BMS-595 inhibits the in vitro proliferation of human colorectal and lung cancer cell lines with IC50s ranging from less than 10 nM to greater than 1 μM. In sensitive cell lines, anti-proliferative effects of BMS-595 and structurally related analogs strongly correlated with cellular CK2 kinase inhibition. Oral administration of BMS-595 to mice bearing colorectal cancer and lung cancer xenografts demonstrated pharmacodynamic effects and robust efficacy at tolerated doses. These studies confirm the dependence of a subset of human colon and lung cancer cell lines on CK2 activity for growth and demonstrate that pharmacologic inhibition of CK2 can produce anti-tumor efficacy at tolerated doses. Citation Format: Brent A. Rupnow, Chiang Yu, Jonathan G. Pabalan, Urvashi V. Roongta, Jonathan S. Lippy, Ashok R. Dongre, Mary T. Obermeier, Aberra Fura, Paul A. Elzinga, Benjamin J. Henley, Joseph Fargnoli, Francis Y. Lee, William R. Foster, Christine M. Tarby, Brian E. Fink, John S. Tokarski, Ashvinikumar V. Gavai, Tai W. Wong, John T. Hunt, Gregory D. Vite, Ashok V. Purandare. Anti-tumor activity of BMS-595, a novel CK2 kinase inhibitor. [abstract]. In: Proceedings of the 106th Annual Meeting of the American Association for Cancer Research; 2015 Apr 18-22; Philadelphia, PA. Philadelphia (PA): AACR; Cancer Res 2015;75(15 Suppl):Abstract nr 5395. doi:10.1158/1538-7445.AM2015-5395

Published

2015

44. Discovery of potent, orally-active, and muscle-selective androgen receptor modulators based on an N-aryl-hydroxybicyclohydantoin scaffold

Author

Blake C. Beehler, Paul G. Sleph, Aberra Fura, Rajasree Golla, Mark E. Salvati, Joyce E. Kuhns, Lawrence G. Hamann, Ramakrishna Seethala, Yongmi An, Jacek Ostrowski, Mary F. Malley, Tammy C. Wang, Chongqing Sun, Jeffrey A. Robl, Yanting Huang, John S. Sack, Stanley R. Krystek, Gary J. Grover, and John A. Lupisella

Subjects

Agonist, Bridged-Ring Compounds, Male, Transcriptional Activation, medicine.medical_specialty, medicine.drug_class, Administration, Oral, Breast Neoplasms, Myoblasts, Mice, In vivo, Prostate, Internal medicine, Drug Discovery, medicine, Animals, Humans, Androgen Receptor Antagonists, Receptor, Luciferases, Muscle, Skeletal, Cells, Cultured, Chemistry, Hydantoins, Biological activity, Dihydrotestosterone, Rats, Androgen receptor, Muscular Atrophy, medicine.anatomical_structure, Endocrinology, Selective androgen receptor modulator, Receptors, Androgen, Molecular Medicine

Abstract

A novel, N-aryl-bicyclohydantoin selective androgen receptor modulator scaffold was discovered through structure-guided modifications of androgen receptor antagonists. A prototype compound (7R,7aS)-10b from this series is a potent and highly tissue-selective agonist of the androgen receptor. After oral dosing in a rat atrophied levator ani muscle model, (7R,7aS)-10b demonstrated efficacy at restoring levator ani muscle mass to that of intact controls and exhibited >50-fold selectivity for muscle over prostate.

Published

2006

45. Tandem optimization of target activity and elimination of mutagenic potential in a potent series of N-aryl bicyclic hydantoin-based selective androgen receptor modulators

Author

James M. Johnson, David A. Betebenner, Chongqing Sun, Yan Zou, Mark C. Manfredi, Yanting Huang, Tammy C. Wang, Scott A. Biller, Laura Custer, Robert Zahler, Jacek Ostrowski, Jennifer Price, Celia D’Arienzo, Lawrence G. Hamann, Stanley R. Krystek, John A. Lupisella, Rajasree Golla, Ramakrishna Seethala, Joyce E. Kuhns, David J. Augeri, Yingzhi Bi, and Aberra Fura

Subjects

endocrine system, Stereochemistry, Chemistry, Pharmaceutical, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, Hydantoin, Mutagen, medicine.disease_cause, Biochemistry, Ames test, chemistry.chemical_compound, Structure-Activity Relationship, Genes, Reporter, Drug Discovery, medicine, Escherichia coli, Animals, Molecular Biology, chemistry.chemical_classification, Bicyclic molecule, Hydantoins, fungi, Organic Chemistry, food and beverages, Aromatic amine, Biological activity, Androgen Antagonists, Androgen receptor, Kinetics, Macaca fascicularis, Selective androgen receptor modulator, chemistry, Models, Chemical, Mutagenesis, Receptors, Androgen, Drug Design, Molecular Medicine, Mutagens

Abstract

Pharmacokinetic studies in cynomolgus monkeys with a novel prototype selective androgen receptor modulator revealed trace amounts of an aniline fragment released through hydrolytic metabolism. This aniline fragment was determined to be mutagenic in an Ames assay. Subsequent concurrent optimization for target activity and avoidance of mutagenicity led to the identification of a pharmacologically superior clinical candidate without mutagenic potential.

Published

2006

46. Discovery and preclinical studies of (R)-1-(4-(4-fluoro-2-methyl-1H-indol-5-yloxy)-5- methylpyrrolo[2,1-f][1,2,4]triazin-6-yloxy)propan- 2-ol (BMS-540215), an in vivo active potent VEGFR-2 inhibitor

Author

Steven Mortillo, Donna D. Wei, Daniel W. Kukral, Viral Vyas, Arvind Mathur, Stephanie Barbosa, Laurence I. Wu, John T. Hunt, Zhen-Wei Cai, Soong-Hoon Kim, Robert Jeyaseelan, Kenneth J. Leavitt, Sam T. Chao, Joseph Fargnoli, Joel C. Barrish, Ligang Qian, Amrita Kamath, Punit Marathe, Xiaoping Zheng, Barri Wautlet, Yong-Zheng Zhang, Leslie Leith, Louis J. Lombardo, Celia D’Arienzo, George M. Derbin, Rajeev S. Bhide, Robert M. Borzilleri, and Aberra Fura

Subjects

Stereochemistry, Transplantation, Heterologous, Mice, Nude, Angiogenesis Inhibitors, chemistry.chemical_compound, Mice, Structure-Activity Relationship, In vivo, Cell Line, Tumor, Drug Discovery, Structure–activity relationship, Animals, Humans, Prodrugs, Pyrroles, Triazine, Mice, Inbred BALB C, Alanine, Triazines, Stereoisomerism, Prodrug, Vascular Endothelial Growth Factor Receptor-2, In vitro, Brivanib alaninate, chemistry, Alkoxy group, Molecular Medicine, Drug Screening Assays, Antitumor, Neoplasm Transplantation, Methyl group

Abstract

A series of substituted 4-(4-fluoro-1H-indol-5-yloxy)pyrrolo[2,1-f][1,2,4]triazine-based inhibitors of vascular endothelial growth factor receptor-2 kinase is reported. Structure-activity relationship studies revealed that a methyl group at the 5-position and a substituted alkoxy group at the 6-position of the pyrrolo[2,1-f][1,2,4]triazine core gave potent compounds. Biochemical potency, kinase selectivity, and pharmacokinetics of the series were optimized and in vitro safety liabilities were minimized to afford BMS-540215 (12), which demonstrated robust preclinical in vivo activity in human tumor xenograft models. The l-alanine prodrug of 12, BMS-582664 (21), is currently under evaluation in clinical trials for the treatment of solid tumors.

Published

2006

47. Synthesis and SAR of 4-(3-hydroxyphenylamino)pyrrolo[2,1-f][1,2,4]triazine based VEGFR-2 kinase inhibitors

Author

Xioping Zheng, Christopher D. Ellis, Robert M. Borzilleri, Bindu Goyal, Tracy Gerhardt, Rajeev S. Bhide, Aberra Fura, Steven Mortillo, Joseph Fargnoli, Viral Vyas, John T. Hunt, John S. Tokarski, Ligang Qian, Zhen-Wei Cai, and Barri Wautlet

Subjects

Models, Molecular, medicine.drug_class, Stereochemistry, Cell Survival, Clinical Biochemistry, Glucuronidation, Pharmaceutical Science, Carboxamide, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Drug Discovery, medicine, Side chain, Animals, Humans, Phenols, Enzyme Inhibitors, Molecular Biology, Triazine, Bicyclic molecule, biology, Molecular Structure, Triazines, Organic Chemistry, Vascular Endothelial Growth Factor Receptor-2, chemistry, Enzyme inhibitor, biology.protein, Microsomes, Liver, Molecular Medicine, Endothelium, Vascular, Protein Binding

Abstract

A versatile synthesis of the suitably functionalized pyrrolo[2,1-f][1,2,4]triazine nucleus is described. SAR at the C-5 and C-6 positions of the 4-(3-hydroxy-4-methylphenylamino)pyrrolo[2,1-f][1,2,4]triazine template led to compounds with good in vitro potency against VEGFR-2 kinase. Glucuronidation of the phenol group is mitigated by incorporation of a basic amino group on the C-6 side chain of the pyrrolotriazine nucleus.

Published

2004

48. Discovering Drugs Through Biological Transformation: Role of Pharmacologically Active Metabolites in Drug Discovery

Author

Vikram Roongta, W. Griffith Humphreys, Mingshe Zhu, Yue-Zhong Shu, Aberra Fura, and Ronald L. Hanson

Subjects

Chemistry, Drug discovery, Drug Evaluation, Preclinical, General Medicine, Pharmacology, Management, Drug metabolizing enzymes, Investigation methods, Cytochrome P-450 Enzyme System, Pharmaceutical Preparations, Drug Design, Drug Discovery, Molecular Medicine, Pharmaceutical sciences, Bristol-Myers, Analysis method, Biotransformation

Abstract

Bristol Myers Squibb, Pharmaceutical Research Institute, P.O. Box 5400, Princeton, New Jersey 08534, Bristol-Myers Squibb, Pharmaceutical Research Institute, 5 Research Parkway, Wallingford, Connecticut 06492, Bristol Myers Squibb, Pharmaceutical Research Institute, P.O. Box 4000, Princeton, New Jersey 08543, and Bristol-Myers Squibb, Pharmaceutical Research Institute, One Squibb Drive, New Brunswick, New Jersey 08903

Published

2004

49. Differentiation of Ca(2+)- and Mg(2+)-coordinated branched trisaccharide isomers: an electrospray ionization and tandem mass spectrometry study

Author

Julie A. Leary and Aberra. Fura

Subjects

chemistry.chemical_classification, Chromatography, Chemistry, Magnesium, Stereochemistry, Electrospray ionization, Molecular Sequence Data, chemistry.chemical_element, Oligosaccharides, Glycosidic bond, Calcium, Tandem mass spectrometry, Fucose, Mass Spectrometry, Analytical Chemistry, Metal, chemistry.chemical_compound, Carbohydrate Sequence, Isomerism, visual_art, visual_art.visual_art_medium, Electrochemistry, Trisaccharide

Abstract

Three isomeric branched trisaccharides coordinated to calcium and magnesium were analyzed by electrospray ionization followed by tandem mass spectrometry. Studies were undertaken to optimize the singly charged metal coordinated precursor prior to MS/MS and MS/MS/MS experiments. The positioning of the glycosidic linkages between reducing and nonreducing rings could be determined in all three isomers, and the linkage of the fucose ring was obvious in two of the three isomers when calcium was used as the coordinating metal. The ionic radius and charge of the metal appear to be very important in obtaining structural information in these isomers.

Published

1993

50. Spectrophotometric Investigation of Iron(III)-N-Phenylcin-namohydroxamic Acid System

Author

Aberra Fura and Bhagwan Singh Chandravanshi

Subjects

Isosbestic point, Reaction conditions, Chemistry, Biochemistry (medical), Clinical Biochemistry, Spectral properties, Analytical chemistry, Biochemistry, Analytical Chemistry, Metal, Visible spectrometry, Stability constants of complexes, visual_art, Electrochemistry, visual_art.visual_art_medium, Absorption (chemistry), Spectroscopy

Abstract

N-Phenylcinnamohydroxamic acid, PCHA, was found to react with iron (III) to form complex species of different colour depending upon the reaction environment. The reaction conditions for the formation of the complex species were studied in aqueous-ethanolic medium. The general spectral properties of the species were investigated. The absorption curves were found to have two isobestic points. The number and composition of the complexes were determined and found to have composition 1:1, 1:2, 1:3 (Fe: PCHA). The wavelengths of the maximum absorbances were figured out to be 535, 495, and 445 nm for the I, II, and III complex species, respectively. It was verified that the Beer's law holds for these complexes at all wavelengths, and for the mixtures at the wavelengths of the isobestic points in a wide range of pH. The stepwise stability constants have been determined by the method of isobestic point and found to be log K1 = 11.55, log K2 = 10.11, and log Kg3 = 7.44 for the I, II, and III complex specie...

Published

1987