Your search keyword '"Dean Hickman"' showing total 28 results

1. Discovery of AM-6494: A Potent and Orally Efficacious β-Site Amyloid Precursor Protein Cleaving Enzyme 1 (BACE1) Inhibitor with in Vivo Selectivity over BACE2

Author

Paul H. Wen, Stephen J. Wood, Qingyian Liu, Aaron C. Siegmund, Liping H. Pettus, Adrian Nanez, Matthew P. Bourbeau, Jennifer R. Allen, Michael D. Bartberger, Douglas A. Whittington, Jodi Bradley, James R. Manning, Kui Chen, Dean Hickman, and Michael E. Johnson

Subjects

Cyclopropanes, Male, Models, Molecular, Thiazines, Pharmacology, 01 natural sciences, Rats, Sprague-Dawley, 03 medical and health sciences, Mice, In vivo, Alzheimer Disease, mental disorders, Drug Discovery, Amyloid precursor protein, medicine, Animals, Aspartic Acid Endopeptidases, Humans, Enzyme Inhibitors, IC50, 030304 developmental biology, Hypopigmentation, Melanosome, chemistry.chemical_classification, 0303 health sciences, Amyloid beta-Peptides, biology, Chemistry, Brain, Peptide Fragments, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Enzyme, Pharmacodynamics, biology.protein, Molecular Medicine, medicine.symptom, Amyloid Precursor Protein Secretases, Selectivity

Abstract

β-Site amyloid precursor protein cleaving enzyme 1 (BACE1) is an aspartyl protease that plays a key role in the production of amyloid β (Aβ) in the brain and has been extensively pursued as a target for the treatment of Alzheimer's disease (AD). BACE2, an aspartyl protease that is structurally related to BACE1, has been recently reported to be involved in melanosome maturation and pigmentation. Herein, we describe the development of a series of cyclopropylthiazines as potent and orally efficacious BACE1 inhibitors. Lead optimization led to the identification of 20, a molecule with biochemical IC50 BACE2/BACE1 ratio of 47. Administration of 20 resulted in no skin/fur color change in a 13-day mouse hypopigmentation study and demonstrated robust and sustained reduction of CSF and brain Aβ40 levels in rat and monkey pharmacodynamic models. On the basis of a compelling data package, 20 (AM-6494) was advanced to preclinical development.

Published

2019

2. Development of 2-aminooxazoline 3-azaxanthene β-amyloid cleaving enzyme (BACE) inhibitors with improved selectivity against Cathepsin D

Author

Michael D. Bartberger, Vijay Keshav Gore, Mark R. Fielden, Ryan White, Qingyian Liu, E. Allen Sickmier, Stephen J. Wood, Jonathan D. Low, Jonathan Werner, Yuan Cheng, Dean Hickman, Hugo M. Vargas, Douglas A. Whittington, Ana Elena Minatti, and Kui Chen

Subjects

0301 basic medicine, Pharmaceutical Science, Cathepsin D, Pharmacology, Biology, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, β amyloid, mental disorders, Drug Discovery, Hydrolase, chemistry.chemical_classification, Cardiovascular safety, Organic Chemistry, Retinal, stomatognathic diseases, Chemistry, 030104 developmental biology, Retinal toxicity, Enzyme, chemistry, Molecular Medicine, Selectivity

Abstract

As part of an ongoing effort at Amgen to develop a disease-modifying therapy for Alzheimer's disease, we have previously used the aminooxazoline xanthene (AOX) scaffold to generate potent and orally efficacious BACE1 inhibitors. While AOX-BACE1 inhibitors demonstrated acceptable cardiovascular safety margins, a retinal pathological finding in rat toxicological studies demanded further investigation. It has been widely postulated that such retinal toxicity might be related to off-target inhibition of Cathepsin D (CatD), a closely related aspartyl protease. We report the development of AOX-BACE1 inhibitors with improved selectivity against CatD by following a structure- and property-based approach. Our efforts culminated in the discovery of a picolinamide-substituted 3-aza-AOX-BACE1 inhibitor absent of retinal effects in an early screening rat toxicology study.

Published

2017

3. Discovery and Optimization of Quinazolinone-pyrrolopyrrolones as Potent and Orally Bioavailable Pan-Pim Kinase Inhibitors

Author

Heather Eastwood, Andrew Tasker, Yuping Chen, David Powers, Nadia Guerrero, Christopher Mohr, Anthony B. Reed, Jimmy Laszlo, Paul Wang, Yihong Zhou, Ryan Wurz, Mark H. Norman, Karen Rex, Jeffrey T. Winston, Liping H. Pettus, Dean Hickman, Yang Xu, Brian A. Lanman, Tian Wu, Yen Nguyen, Kristin L. Andrews, J. Russell Lipford, Frank Chavez, Hui-Ling Wang, Christine Sastri, Matthew R. Lee, Bethany Mattson, Nuria A. Tamayo, Victor J. Cee, Jie Chen, Bradley J. Herberich, Bin Wu, and Shon Booker

Subjects

Models, Molecular, 0301 basic medicine, Cell, Administration, Oral, Antineoplastic Agents, Pharmacology, Mice, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, Proto-Oncogene Proteins c-pim-1, hemic and lymphatic diseases, Drug Discovery, Murine leukemia virus, medicine, Animals, Humans, Pyrroles, Kinase activity, Protein Kinase Inhibitors, Cell Proliferation, Quinazolinones, Dose-Response Relationship, Drug, Molecular Structure, biology, Cell growth, Chemistry, Drug discovery, Kinase, Neoplasms, Experimental, biology.organism_classification, Xenograft Model Antitumor Assays, 030104 developmental biology, medicine.anatomical_structure, Apoptosis, 030220 oncology & carcinogenesis, Molecular Medicine

Abstract

The high expression of proviral insertion site of Moloney murine leukemia virus kinases (Pim-1, -2, and -3) in cancers, particularly the hematopoietic malignancies, is believed to play a role in promoting cell survival and proliferation while suppressing apoptosis. The three isoforms of Pim protein appear largely redundant in their oncogenic functions. Thus, a pan-Pim kinase inhibitor is highly desirable. However, cell active pan-Pim inhibitors have proven difficult to develop because Pim-2 has a low Km for ATP and therefore requires a very potent inhibitor to effectively block the kinase activity at cellular ATP concentrations. Herein, we report a series of quinazolinone-pyrrolopyrrolones as potent and selective pan-Pim inhibitors. In particular, compound 17 is orally efficacious in a mouse xenograft model (KMS-12 BM) of multiple myeloma, with 93% tumor growth inhibition at 50 mg/kg QD upon oral dosing.

Published

2016

4. Inhibitors of β-Site Amyloid Precursor Protein Cleaving Enzyme (BACE1): Identification of (S)-7-(2-Fluoropyridin-3-yl)-3-((3-methyloxetan-3-yl)ethynyl)-5′H-spiro[chromeno[2,3-b]pyridine-5,4′-oxazol]-2′-amine (AMG-8718)

Author

Paul H. Wen, Robert C. Wahl, Ryan White, Oleg Epstein, Stephen J. Wood, Katayoun Derakhchan, Douglas A. Whittington, Chuck E. Kreiman, Isaac E. Marx, Thomas Dineen, Dean Hickman, Kui Chen, Matthew Weiss, Joel Esmay, Vinod F. Patel, Alan C. Cheng, and Robert T. Fremeau

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Pyridines, Stereochemistry, hERG, Rats, Sprague-Dawley, Inhibitory Concentration 50, Structure-Activity Relationship, chemistry.chemical_compound, mental disorders, Drug Discovery, Pyridine, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Humans, Structure–activity relationship, Potency, Benzopyrans, Protease Inhibitors, Spiro Compounds, cardiovascular diseases, chemistry.chemical_classification, Xanthene, Amyloid beta-Peptides, biology, Ether-A-Go-Go Potassium Channels, HEK293 Cells, Enzyme, chemistry, Microsomes, Liver, biology.protein, Molecular Medicine, Amine gas treating, Amyloid Precursor Protein Secretases

Abstract

We have previously shown that the aminooxazoline xanthene scaffold can generate potent and orally efficacious BACE1 inhibitors although certain of these compounds exhibited potential hERG liabilities. In this article, we describe 4-aza substitution on the xanthene core as a means to increase BACE1 potency while reducing hERG binding affinity. Further optimization of the P3 and P2' side chains resulted in the identification of 42 (AMG-8718), a compound with a balanced profile of BACE1 potency, hERG binding affinity, and Pgp recognition. This compound produced robust and sustained reductions of CSF and brain Aβ levels in a rat pharmacodynamic model and exhibited significantly reduced potential for QTc elongation in a cardiovascular safety model.

Published

2014

5. A Potent and Orally Efficacious, Hydroxyethylamine-Based Inhibitor of β-Secretase

Author

Kui Chen, Daniel La, Michael D. Bartberger, Russell Graceffa, Thomas T. Nguyen, Tisha San Miguel, E. Allen Sickmier, Ryan Brown, Vivian S. W. Li, Stephen J. Wood, Lewis D. Pennington, James Brown, Jianhua Zhang, Craig E. Masse, Holger Monenschein, Patricia Lopez, Dean Hickman, Brian K. Albrecht, May Xue, Michael Croghan, Scott Harried, Safura Babu-Khan, Yuan Cheng, Yi Luo, Martin Citron, Matthew R. Kaller, Patricia Amarante, Wenge Zhong, Paul H. Wen, Bryant Yang, Robert C. Wahl, Matthew Weiss, Chuck Kriemen, Stephen Hitchcock, Vinod F. Patel, Ted Judd, and Toni Williamson

Subjects

chemistry.chemical_classification, Enzyme, biology, Chemistry, Cerebral Spinal Fluid, Organic Chemistry, Drug Discovery, β secretase, Amyloid precursor protein, biology.protein, Potency, Pharmacology, Biochemistry

Abstract

β-Secretase inhibitors are potentially disease-modifying treatments for Alzheimer's disease. Previous efforts in our laboratory have resulted in hydroxyethylamine-derived inhibitors such as 1 with low nanomolar potency against β-site amyloid precursor protein cleaving enzyme (BACE). When dosed intravenously, compound 1 was also shown to significantly reduce Aβ40 levels in plasma, brain, and cerebral spinal fluid. Herein, we report further optimizations that led to the discovery of inhibitor 16 as a novel, potent, and orally efficacious BACE inhibitor.

Published

2012

6. Design and Synthesis of Potent, Orally Efficacious Hydroxyethylamine Derived β-Site Amyloid Precursor Protein Cleaving Enzyme (BACE1) Inhibitors

Author

Paul H. Wen, Robert C. Wahl, Michael Croghan, Ronke Imbeah-Ampiah, Paul Acton, Stephen J. Wood, Charles Kreiman, Vivian S. W. Li, Qiufen Xue, Lewis D. Pennington, Safura Babu-Khan, Daniel B. Horne, Thomas Dineen, Wenge Zhong, Scott Harried, Douglas A. Whittington, Dean Hickman, James Brown, Martin Citron, Matthew Weiss, Daniel S. La, Holger Monenschein, Bryant Yang, E. Allen Sickmier, Tisha San Miguel, Robert T. Dunn, Russell Graceffa, Patricia Lopez, Toni Williamson, Hongbing Huang, Yuan Cheng, Kui Chen, Matthew R. Kaller, Michael D. Bartberger, Steven W. Louie, Hugo M. Vargas, Stephen Hitchcock, Thomas T. Nguyen, Vinod F. Patel, Ted Judd, and Joel Esmay

Subjects

Male, Models, Molecular, Protein Conformation, Swine, Administration, Oral, Peptide, In Vitro Techniques, Pharmacology, Crystallography, X-Ray, Inhibitory postsynaptic potential, Cell Line, Rats, Sprague-Dawley, Structure-Activity Relationship, Dogs, Pharmacokinetics, mental disorders, Drug Discovery, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme Inhibitors, Humans, Spiro Compounds, Dosing, chemistry.chemical_classification, Amyloid beta-Peptides, Cardiovascular safety, biology, Brain, Stereoisomerism, Blood Proteins, Peptide Fragments, Rats, Bioavailability, Thiazoles, Enzyme, Biochemistry, chemistry, Drug Design, Microsomes, Liver, biology.protein, Molecular Medicine, Amyloid Precursor Protein Secretases, Protein Binding

Abstract

We have previously shown that hydroxyethylamines can be potent inhibitors of the BACE1 enzyme and that the generation of BACE1 inhibitors with CYP 3A4 inhibitory activities in this scaffold affords compounds (e.g., 1) with sufficient bioavailability and pharmacokinetic profiles to reduce central amyloid-β peptide (Aβ) levels in wild-type rats following oral dosing. In this article, we describe further modifications of the P1-phenyl ring of the hydroxyethylamine series to afford potent, dual BACE1/CYP 3A4 inhibitors which demonstrate improved penetration into the CNS. Several of these compounds caused robust reduction of Aβ levels in rat CSF and brain following oral dosing, and compound 37 exhibited an improved cardiovascular safety profile relative to 1.

Published

2012

7. From Fragment Screening to In Vivo Efficacy: Optimization of a Series of 2-Aminoquinolines as Potent Inhibitors of Beta-Site Amyloid Precursor Protein Cleaving Enzyme 1 (BACE1)

Author

Timothy Powers, Stephen J. Wood, Ted Judd, Vivian S. W. Li, James Brown, E. Allen Sickmier, Klaus Michelsen, David J. St. Jean, Yi Luo, Dean Hickman, Yuan Cheng, Kui Chen, Stephen Hitchcock, Steven W. Louie, Patricia Lopez, Brad Jordan, Thomas Nixey, Robert T. Fremeau, Michael D. Bartberger, Paul H. Wen, Robert C. Wahl, and Claire Rattan

Subjects

Male, Models, Molecular, Molecular model, Drug Evaluation, Preclinical, Crystallography, X-Ray, Cell Line, Rats, Sprague-Dawley, Structure-Activity Relationship, In vivo, Catalytic Domain, mental disorders, Drug Discovery, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Humans, Potency, Enzyme Inhibitors, Aminoquinolines, IC50, chemistry.chemical_classification, Amyloid beta-Peptides, Dose-Response Relationship, Drug, Molecular Structure, biology, Ligand, Brain, Combinatorial chemistry, Protein Structure, Tertiary, Rats, HEK293 Cells, Enzyme, Models, Chemical, Biochemistry, chemistry, Biocatalysis, biology.protein, Molecular Medicine, Amyloid Precursor Protein Secretases

Abstract

Using fragment-based screening of a focused fragment library, 2-aminoquinoline 1 was identified as an initial hit for BACE1. Further SAR development was supported by X-ray structures of BACE1 cocrystallized with various ligands and molecular modeling studies to expedite the discovery of potent compounds. These strategies enabled us to integrate the C-3 side chain on 2-aminoquinoline 1 extending deep into the P2' binding pocket of BACE1 and enhancing the ligand's potency. We were able to improve the BACE1 potency to subnanomolar range, over 10(6)-fold more potent than the initial hit (900 μM). Further elaboration of the physical properties of the lead compounds to those more consistent with good blood-brain barrier permeability led to inhibitors with greatly improved cellular activity and permeability. Compound 59 showed an IC(50) value of 11 nM on BACE1 and cellular activity of 80 nM. This compound was advanced into rat pharmacokinetic and pharmacodynamic studies and demonstrated significant reduction of Aβ levels in cerebrospinal fluid (CSF).

Published

2011

8. 2-Amino-1,3-thiazol-4(5H)-ones as Potent and Selective 11β-Hydroxysteroid Dehydrogenase Type 1 Inhibitors: Enzyme−Ligand Co-Crystal Structure and Demonstration of Pharmacodynamic Effects in C57Bl/6 Mice

Author

Meredith Williams, Sonja Gustafsson, Carlos Orihuela, Murielle M. Véniant, Minghan Wang, Evert Homan, Gunnar Palm, George A. Moniz, Aiwen Li, Victor M. Castro, Michael D. Bartberger, Jiandong Zhang, Christopher H. Fotsch, Dean Hickman, Guy Matsumoto, Michelle Chen, Steven R. Jordan, Clarence Hale, Renee Komorowski, Maurice Emery, Kenneth Mcrae, and Lars Johansson

Subjects

Male, Models, Molecular, Hydrocortisone, Stereochemistry, Adamantane, Dehydrogenase, Crystallography, X-Ray, Ligands, Chemical synthesis, Mice, Structure-Activity Relationship, Oxidoreductase, In vivo, 11-beta-Hydroxysteroid Dehydrogenase Type 1, Drug Discovery, Animals, Humans, Hypoglycemic Agents, Structure–activity relationship, chemistry.chemical_classification, Molecular Structure, biology, Chemistry, Stereoisomerism, Triazoles, Rats, Cortisone, Mice, Inbred C57BL, Thiazoles, Enzyme, Adipose Tissue, Diabetes Mellitus, Type 2, Liver, Biochemistry, Enzyme inhibitor, biology.protein, Molecular Medicine, hormones, hormone substitutes, and hormone antagonists, Ex vivo

Abstract

11beta-hydroxysteroid dehydrogenase type 1 (11beta-HSD1) has attracted considerable attention during the past few years as a potential target for the treatment of diseases associated with metabolic syndrome. In our ongoing work on 11beta-HSD1 inhibitors, a series of new 2-amino-1,3-thiazol-4(5 H)-ones were explored. By inserting various cycloalkylamines at the 2-position and alkyl groups or spirocycloalkyl groups at the 5-position of the thiazolone, several potent 11beta-HSD1 inhibitors were identified. An X-ray cocrystal structure of human 11beta-HSD1 with compound 6d (Ki=28 nM) revealed a large lipophilic pocket accessible by substitution off the 2-position of the thiazolone. To increase potency, analogues were prepared with larger lipophilic groups at this position. One of these compounds, the 3-noradamantyl analogue 8b, was a potent inhibitor of human 11beta-HSD1 (Ki=3 nM) and also inhibited 11beta-HSD1 activity in lean C57Bl/6 mice when evaluated in an ex vivo adipose and liver cortisone to cortisol conversion assay.

Published

2008

9. Structural Characterization and Pharmacodynamic Effects of an Orally Active 11β-Hydroxysteroid Dehydrogenase Type 1 Inhibitor

Author

Haoda Xu, Michelle Chen, David J. St. Jean, Guy Matsumoto, Zhulun Wang, Christopher H. Fotsch, Minghan Wang, Rod Cupples, Jocelyn McCormick, Clarence Hale, Athena Sudom, Xiaoshan Min, Dean Hickman, and Murielle M. Véniant

Subjects

Pharmacology, chemistry.chemical_classification, Chinese hamster ovary cell, Organic Chemistry, Dehydrogenase, Biology, Biochemistry, chemistry.chemical_compound, Enzyme, Protein structure, chemistry, In vivo, Oxidoreductase, Drug Discovery, Molecular Medicine, Nicotinamide adenine dinucleotide phosphate, Ex vivo

Abstract

11Beta-hydroxysteroid dehydrogenase type 1 regulates glucocorticoid action and inhibition of this enzyme is a viable therapeutic strategy for the treatment of type 2 diabetes and the metabolic syndrome. Here, we report a potent and selective 11beta-hydroxysteroid dehydrogenase type 1 inhibitor with a binding mode elucidated from the co-crystal structure with the human 11beta-hydroxysteroid dehydrogenase type 1. The inhibitor is bound to the steroid-binding pocket making contacts with the catalytic center and the solvent channel. The inhibitor binding is facilitated by two direct hydrogen bond interactions involving Tyrosine183 of the catalytic motif Tyr-X-X-X-Lys and Alanine172. In addition, the inhibitor makes many hydrophobic interactions with both the enzyme and the co-factor nicotinamide adenine dinucleotide phosphate (reduced). In lean C57BL/6 mice, the compound inhibited both the in vivo and ex vivo 11beta-hydroxysteroid dehydrogenase type 1 activities in a dose-dependent manner. The inhibitory effects correlate with the plasma compound concentrations, suggesting that there is a clear pharmacokinetic and pharmacodynamic relationship. Moreover, at the same doses used in the pharmacokinetic/pharmacodynamic studies, the inhibitor did not cause the activation of the hypothalamic-pituitary-adrenal axis in an acute mouse model, suggesting that this compound exhibits biological effects with minimal risk of activating the hypothalamic-pituitary-adrenal axis.

Published

2007

10. 1,4-Dihydroindeno[1,2-c]pyrazoles as potent checkpoint kinase 1 inhibitors: Extended exploration on phenyl ring substitutions and preliminary ADME/PK studies

Author

Tim J. Stratton, Yunsong Tong, Jian Wu, Hing L. Sham, Nan-Horng Lin, Elizabeth A. Everitt, Bernard P. Murry, Kent D. Stewart, Zehan Chen, Haiying Zhang, Robert B. Credo, Saul H. Rosenberg, Philip Merta, Zhi-Fu Tao, Peter Kovar, Jennifer J. Bouska, Thomas J. Sowin, Dean Hickman, Akiyo Claiborne, Ran Guan, and Magdalena Pyzytulinska

Subjects

Stereochemistry, Chemistry, Pharmaceutical, Clinical Biochemistry, Pharmaceutical Science, Antineoplastic Agents, Biochemistry, Chemical synthesis, HeLa, Inhibitory Concentration 50, Mice, Drug Discovery, Animals, Humans, Chemosensitizing agent, CHEK1, Protein kinase A, Protein Kinase Inhibitors, Molecular Biology, ADME, chemistry.chemical_classification, biology, Organic Chemistry, Flow Cytometry, biology.organism_classification, Rats, Enzyme, chemistry, Enzyme inhibitor, Drug Design, Checkpoint Kinase 1, Microsomes, Liver, biology.protein, Molecular Medicine, Caco-2 Cells, Drug Screening Assays, Antitumor, Protein Kinases, DNA Damage

Abstract

A study on substitutions at the four open positions on the phenyl ring of the 1,4-dihydroindeno[1,2-c]pyrazoles as potent CHK-1 inhibitors is described. Bis-substitution at both the 6- and 7-positions led to inhibitors with IC(50) values below 0.3nM. The compound with the best overall activities (36) was able to potentiate the anti-proliferative effect of doxorubicin in HeLa cells by at least 47-fold. Physicochemical, metabolic, and pharmacokinetic properties of selected inhibitors are also disclosed.

Published

2007

11. Oxopyrido[2,3-d]pyrimidines as Covalent L858R/T790M Mutant Selective Epidermal Growth Factor Receptor (EGFR) Inhibitors

Author

Andrew Tasker, Pedro J. Beltran, Darren L. Reid, Robert Radinsky, Jian J. Chen, Dina A. Andrews, David J. St. Jean, Keegan Cooke, Ryan Wurz, Tian Wu, Nataraj Kalyanaraman, Essa Hu-Harrington, Faye Hsieh, Simon J. Hedley, Kristin L. Andrews, Brad Herberich, Nancy E. Everds, Seifu Tadesse, Michele Kubryk, Jinghui Zhan, Jason S. Tedrow, Kate Ashton, Petia Mitchell, Andrew T. Parsons, Roberto E. Guzman, Liping H. Pettus, James Brown, Dean Hickman, Tom Nguyen, Matthew S. Potter, Edward K. Lobenhofer, David Bauer, Fang-Tsao Hong, and Oliver R. Thiel

Subjects

biology, Kinase, business.industry, Organic Chemistry, Pharmacology, Biochemistry, respiratory tract diseases, T790M, Gefitinib, Cell culture, Drug Discovery, medicine, Cancer research, biology.protein, Erlotinib, Epidermal growth factor receptor, business, Tyrosine kinase, medicine.drug, EGFR inhibitors

Abstract

In nonsmall cell lung cancer (NSCLC), the threonine(790)-methionine(790) (T790M) point mutation of EGFR kinase is one of the leading causes of acquired resistance to the first generation tyrosine kinase inhibitors (TKIs), such as gefitinib and erlotinib. Herein, we describe the optimization of a series of 7-oxopyrido[2,3-d]pyrimidinyl-derived irreversible inhibitors of EGFR kinase. This led to the discovery of compound 24 which potently inhibits gefitinib-resistant EGFR(L858R,T790M) with 100-fold selectivity over wild-type EGFR. Compound 24 displays strong antiproliferative activity against the H1975 nonsmall cell lung cancer cell line, the first line mutant HCC827 cell line, and promising antitumor activity in an EGFR(L858R,T790M) driven H1975 xenograft model sparing the side effects associated with the inhibition of wild-type EGFR.

Published

2015

12. Estimation of Serum-Free 50-Percent Inhibitory Concentrations for Human Immunodeficiency Virus Protease Inhibitors Lopinavir and Ritonavir

Author

Dale J. Kempf, Dean Hickman, Richard Bertz, Ann Hsu, Lynn Colletti, Sudthida Vasavanonda, Warren M. Kati, and George Nequist

Subjects

medicine.medical_treatment, Pyrimidinones, Pharmacology, Biology, Antiviral Agents, Lopinavir, HIV Protease, medicine, Animals, Humans, HIV Protease Inhibitor, Potency, Pharmacology (medical), Protease inhibitor (pharmacology), IC50, Chromatography, High Pressure Liquid, Ritonavir, Protease, HIV Protease Inhibitors, Virology, Kinetics, Infectious Diseases, Free fraction, Biological Assay, Cattle, Algorithms, Protein Binding, medicine.drug

Abstract

Using measured free fraction and 50% inhibitory concentration (IC 50 ) values for the human immunodeficiency virus protease inhibitors lopinavir (LPV) and ritonavir (RTV) in tissue culture media with various protein concentrations ranging from 5 to 50%, we estimated serum-free IC 50 values for each drug. The range of serum-free IC 50 values (0.64 to 0.77 ng/ml for LPV and 3.0 to 5.0 ng/ml for RTV) did not exhibit a trend with increasing protein concentrations, despite a 10-fold difference in the free fraction value (0.006 to 0.063) for LPV and a 5-fold difference in the free fraction value (0.013 to 0.057) for RTV. The mean serum-free IC 50 by the MTT-MT4 assay (0.69 ng/ml for LPV and 4.0 ng/ml for RTV) may be the most accurate parameter for the estimation of the inhibitory quotient (IQ), a relative measure of in vivo potency defined as the ratio of the minimal free drug concentration in plasma ( C trough,free ) for a specific patient population and the serum-free IC 50 . Using this approach, we calculated the average IQs for protease inhibitor-naïve patients for LPV and RTV to be 67 and 5.6, respectively.

Published

2004

13. An Orally Available BACE1 Inhibitor That Affords Robust CNS Aβ Reduction without Cardiovascular Liabilities

Author

Kui Chen, Ryan White, Robert T. Fremeau, Stephen J. Wood, Oleg Epstein, Scott Harried, Paul H. Wen, Michael D. Bartberger, James Brown, Robert C. Wahl, Douglas A. Whittington, Robert T. Dunn, Xiao Mei Zheng, Matthew Weiss, Yuan Cheng, Patricia Lopez, Dean Hickman, Wenyuan Qian, Jian J. Chen, Vinod F. Patel, Timothy Powers, Ted Judd, Yi Luo, Ana Elena Minatti, Stephen Hitchcock, and Hugo M. Vargas

Subjects

Cardiovascular safety, biology, Chemistry, mental disorders, Organic Chemistry, Drug Discovery, hERG, Aβ peptide, biology.protein, Low activity, Pharmacology, Biochemistry

Abstract

BACE1 inhibition to prevent Aβ peptide formation is considered to be a potential route to a disease-modifying treatment for Alzheimer’s disease. Previous efforts in our laboratory using a combined structure- and property-based approach have resulted in the identification of aminooxazoline xanthenes as potent BACE1 inhibitors. Herein, we report further optimization leading to the discovery of inhibitor 15 as an orally available and highly efficacious BACE1 inhibitor that robustly reduces CSF and brain Aβ levels in both rats and nonhuman primates. In addition, compound 15 exhibited low activity on the hERG ion channel and was well tolerated in an integrated cardiovascular safety model.

Published

2014

14. Lead optimization and modulation of hERG activity in a series of aminooxazoline xanthene β-site amyloid precursor protein cleaving enzyme (BACE1) inhibitors

Author

Paul H. Wen, Robert C. Wahl, Ryan White, Zihao Hua, Robert T. Fremeau, Thomas Dineen, Stephen J. Wood, Jason Brooks Human, Vinod F. Patel, Marian C. Bryan, Oleg Epstein, Douglas A. Whittington, Katayoun Derakhchan, Charles Kreiman, Matthew Weiss, Alan C. Cheng, Dean Hickman, Xiao Mei Zheng, and Isaac E. Marx

Subjects

Male, Stereochemistry, hERG, Crystallography, X-Ray, Polar surface area, Rats, Sprague-Dawley, chemistry.chemical_compound, Inhibitory Concentration 50, Structure-Activity Relationship, Drug Discovery, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Humans, Protease Inhibitors, Ion channel, Xanthene, chemistry.chemical_classification, biology, Oxazolone, Ether-A-Go-Go Potassium Channels, Enzyme, HEK293 Cells, chemistry, Xanthenes, biology.protein, Microsomes, Liver, Molecular Medicine, Efflux, Amyloid Precursor Protein Secretases, Lead compound

Abstract

The optimization of a series of aminooxazoline xanthene inhibitors of β-site amyloid precursor protein cleaving enzyme 1 (BACE1) is described. An early lead compound showed robust Aβ lowering activity in a rat pharmacodynamic model, but advancement was precluded by a low therapeutic window to QTc prolongation in cardiovascular models consistent with in vitro activity on the hERG ion channel. While the introduction of polar groups was effective in reducing hERG binding affinity, this came at the expense of higher than desired Pgp-mediated efflux. A balance of low Pgp efflux and hERG activity was achieved by lowering the polar surface area of the P3 substituent while retaining polarity in the P2' side chain. The introduction of a fluorine in position 4 of the xanthene ring improved BACE1 potency (5-10-fold). The combination of these optimized fragments resulted in identification of compound 40, which showed robust Aβ reduction in a rat pharmacodynamic model (78% Aβ reduction in CSF at 10 mg/kg po) and also showed acceptable cardiovascular safety in vivo.

Published

2014

15. Development of 2-aminooxazoline 3-azaxanthenes as orally efficacious β-secretase inhibitors for the potential treatment of Alzheimer's disease

Author

Vinod F. Patel, Timothy Powers, Michael D. Bartberger, Ted Judd, Ryan White, Stephen J. Wood, Ana Elena Minatti, Stephen Hitchcock, Vijay Keshav Gore, Wenge Zhong, Hugo M. Vargas, Jason Brooks Human, Kui Chen, Steven Vonderfecht, Robert T. Fremeau, Robert T. Dunn, James Brown, Patricia Lopez, Qingyian Liu, Vu Van Ma, Nancy E. Everds, Matthew Weiss, Charles Kreiman, Oleg Epstein, May Xue, Chester Chenguang Yuan, Jonathan Werner, Alan C. Cheng, Jian J. Chen, Albert Amegadzie, Paul H. Wen, Yuan Cheng, Douglas A. Whittington, Wenyuan Qian, Isaac E. Marx, Thomas Dineen, and Dean Hickman

Subjects

Drug, Amyloid, media_common.quotation_subject, Clinical Biochemistry, Pharmaceutical Science, Disease, Pharmacology, Biochemistry, Cell Line, Alzheimer Disease, mental disorders, Drug Discovery, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Humans, Protease Inhibitors, Molecular Biology, media_common, chemistry.chemical_classification, biology, Organic Chemistry, P3 peptide, Rats, Enzyme, HEK293 Cells, chemistry, Xanthenes, Pharmacodynamics, β secretase, biology.protein, Molecular Medicine, Amyloid Precursor Protein Secretases

Abstract

The β-site amyloid precursor protein (APP) cleaving enzyme 1 (BACE1) is one of the most hotly pursued targets for the treatment of Alzheimer’s disease. We used a structure- and property-based drug design approach to identify 2-aminooxazoline 3-azaxanthenes as potent BACE1 inhibitors which significantly reduced CSF and brain Aβ levels in a rat pharmacodynamic model. Compared to the initial lead 2, compound 28 exhibited reduced potential for QTc prolongation in a non-human primate cardiovascular safety model.

Published

2014

16. Retinal Toxicity Induced by a Novel β-secretase Inhibitor in the Sprague-Dawley Rat

Author

Cynthia A. Afshari, Robert T. Dunn, Esther S. Trueblood, Jonathan Werner, Aldo Coppi, Ruth Lightfoot-Dunn, Jeffrey A. Jamison, Dean Hickman, Mark R. Fielden, and Lei Zhou

Subjects

Male, medicine.medical_specialty, Knockout rat, Pyridines, Biology, Toxicology, Retina, Pathology and Forensic Medicine, Lesion, Rats, Sprague-Dawley, chemistry.chemical_compound, Retinal Diseases, Internal medicine, medicine, Electroretinography, Animals, Aspartic Acid Endopeptidases, Benzopyrans, Spiro Compounds, Enzyme Inhibitors, Outer nuclear layer, Molecular Biology, Retinal thinning, Retinal pigment epithelium, Retinal, Cell Biology, Anatomy, eye diseases, Rats, medicine.anatomical_structure, Endocrinology, chemistry, Toxicity, sense organs, medicine.symptom, Amyloid Precursor Protein Secretases, Tomography, Optical Coherence

Abstract

β-Secretase 1 (BACE1) represents an attractive target for the treatment of Alzheimer’s disease. In the course of development of a novel small molecule BACE1 inhibitor (AMG-8718), retinal thinning was observed in a 1-month toxicity study in the rat. To further understand the lesion, an investigational study was conducted whereby rats were treated daily with AMG-8718 for 1 month followed by a 2-month treatment-free phase. The earliest detectable change in the retina was an increase in autofluorescent granules in the retinal pigment epithelium (RPE) on day 5; however, there were no treatment-related light microscopic changes observed in the neuroretina and no changes observed by fundus autofluorescence or routine ophthalmoscopic examination after 28 days of dosing. Following 2 months of recovery, there was significant retinal thinning attributed to loss of photoreceptor nuclei from the outer nuclear layer. Electroretinographic changes were observed as early as day 14, before any microscopic evidence of photoreceptor loss. BACE1 knockout rats were generated and found to have normal retinal morphology indicating that the retinal toxicity induced by AMG-8718 was likely off-target. These results suggest that AMG-8718 impairs phagolysosomal function in the rat RPE, which leads to photoreceptor dysfunction and ultimately loss of photoreceptors.

Published

2014

17. Analysis of two matrix metalloproteinase inhibitors and their metabolites for induction of phospholipidosis in rat and human hepatocytes11Abbreviations: MMP, matrix metalloproteinase; MMPI, matrix metalloproteinase inhibitor; DMEM, Dulbecco’s modified Eagle’s medium; FBS, fetal bovine serum; NBD-PE, N-(7-nitrobenz-2-oxa-1,3-diazol-4-yl)1,2-dihexadecanoyl-sn-glycero-3-phosphoethanolamine; and MTT, 3-[4,5-dimethylthiazol-2-yl]-2,5-diphenyltetrazolium bromide; DMSO, dimethylsulfoxide; HPLC, high performance liquid chromatography

Author

Steven K. Davidsen, Jane A. Fagerland, Michael R. Michaelides, Matthew Heindel, Roger G. Ulrich, James M. Schmidt, Gerard D. Gagne, Rebecca J. Gum, and Dean Hickman

Subjects

Pharmacology, Phospholipidosis, biology, Matrix metalloproteinase inhibitor, Metabolite, Phospholipid, Biochemistry, In vitro, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Enzyme inhibitor, In vivo, Hepatocyte, medicine, biology.protein

Abstract

ABT-770 [(S)-N-[1-[[4′-trifluoromethoxy-[1,1′-biphenyl]-4-yl]oxy]methyl-2-(4,4-dimethyl-2,5-dioxo-1-imidazolidinyl)ethyl]-N-hydroxyformamide], a matrix metalloproteinase inhibitor (MMPI), produced generalized phospholipidosis in rats. Phospholipid accumulation was accompanied by retention of drug-related material and was associated with increased mortality. Generation of a successful drug candidate depended upon understanding the cause of the phospholipidosis and redesigning the chemical structure accordingly. ABT-770 and other MMPIs, plus several metabolites of each, were assayed for their ability to induce phospholipidosis in primary cultured rat and human hepatocytes. Phospholipid accumulation was detected by following the incorporation of a fluorescent phospholipid analogue into intracytoplasmic inclusion bodies characteristic of phospholipid storage disorders. At 24 and 48 hr, none of the parent compounds induced phospholipidosis in vitro in rat or human hepatocytes. Phospholipidosis was associated primarily with an amine metabolite of ABT-770. The amine metabolite of another MMPI, ABT-518 ([S-(R∗,R∗)]-N-[1-(2,2-dimethyl-1,3-dioxol-4-yl)-2-[[4-[4-(trifluoromethoxy)-phenoxy]phenyl]sulfonyl]ethyl]-N-hydroxyformamide), produced little phospholipidosis in rat and human hepatocytes even at concentrations up to 100 μM. The presence or absence of phospholipidosis in the in vitro assay correlated well with ultrastructural findings and drug accumulation in rat tissues. ABT-770, which produced phospholipidosis associated with its amine metabolite in vitro and in vivo, also generated a higher tissue to plasma distribution of metabolites particularly in tissues where phospholipidosis was observed. ABT-518 and its amine metabolite, however, produced low tissue to plasma ratios and induced little to no phospholipidosis in vitro or in vivo. These results demonstrate that the phospholipidosis observed for ABT-770 could be attributed to a cationic metabolite, and that altering the properties of such a metabolite, by modification of the parent compound, alleviated the disorder.

Published

2001

18. Expression of arylamine N-acetyltransferase in human intestine

Author

Edith Sim, M Payton, S D Patil, Dean Hickman, G Fakis, V Smelt, J Pope, Jashvant D. Unadkat, and L A Stanley

Subjects

Nutrition and Metabolism, Polymorphism, Genetic, Genotype, Arylamine N-acetyltransferase, Arylamine N-Acetyltransferase, Gastroenterology, Biology, Immunohistochemistry, Isozyme, Small intestine, Staining, Intestines, Isoenzymes, Blot, Cytosol, medicine.anatomical_structure, Biochemistry, medicine, Humans, Drug metabolism, Carcinogen

Abstract

Background—ArylamineN-acetyltransferases in humans (NAT1 and NAT2) catalyse the acetylation of arylamines including food derived heterocyclic arylamine carcinogens. Other substrates include the sulphonamide 5-aminosalicylic acid (5-ASA), which is an NAT1 specific substrate; N-acetylation of 5-ASA is a major route of metabolism. NAT1 and NAT2 are both polymorphic.Aims—To investigate NAT expression in apparently healthy human intestines in order to understand the possible role of NAT in colorectal cancer and in the therapeutic response to 5-ASA.Methods—The intestines of four organ donors were divided into eight sections. DNA was prepared for genotypingNAT1 and NAT2 and enzymic activities of NAT1 and NAT2 were determined in cytosols prepared from each section. Tissue was fixed for immunohistochemistry with specific NAT antibodies. Western blotting was carried out on all samples of cytosol and on homogenates of separated muscle and villi after microdissection.Results—NAT1 activity of all cytosols was greater than NAT2 activity. NAT1 and NAT2 activities correlated with the genotypes of NAT1 and NAT2 and with the levels of NAT1 staining determined by western blotting. The ratio of NAT1:NAT2 activities showed interindividual variations from 2 to 70. NAT1 antigenic activity was greater in villi than in muscle. NAT1 was detected along the length of the villi in the small intestine. In colon samples there was less NAT1 at the base of the crypts with intense staining at the tips.Conclusions—The interindividual variation in NAT1 and NAT2 in the colon could affect how individuals respond to exposure to specific NAT substrates including carcinogens and 5-ASA.

Published

1998

19. Establishing the relationship between in vitro potency, pharmacokinetic, and pharmacodynamic parameters in a series of orally available, hydroxyethylamine-derived β-secretase inhibitors

Author

Yi Luo, Stephen J. Wood, Toni Williamson, Jianhua Zhang, Thomas Dineen, Dean Hickman, Matthew R. Kaller, Kui Chen, Safura Babu-Khan, Li Zhu, Stephen Hitchcock, Joel Esmay, Roger Pham, Martin Citron, Wenge Zhong, Matthew Weiss, and Paul H. Wen

Subjects

Male, Cell Membrane Permeability, Drug design, Administration, Oral, Pharmacology, In Vitro Techniques, Polar surface area, Rats, Sprague-Dawley, Structure-Activity Relationship, In vivo, mental disorders, Amyloid precursor protein, Ethylamines, Fluorescence Resonance Energy Transfer, Structure–activity relationship, Potency, Animals, Aspartic Acid Endopeptidases, Humans, ATP Binding Cassette Transporter, Subfamily B, Member 1, Enzyme Inhibitors, Amyloid beta-Peptides, biology, Chemistry, Blood Proteins, Recombinant Proteins, Rats, HEK293 Cells, Drug development, biology.protein, Microsomes, Liver, Molecular Medicine, Amyloid Precursor Protein Secretases, Amyloid precursor protein secretase, Protein Binding

Abstract

Sequential proteolytic cleavage of the amyloid precursor protein (APP) by β-site APP-cleaving enzyme 1 (BACE1) and the γ-secretase complex produces the amyloid-β peptide (Aβ), which is believed to play a critical role in the pathology of Alzheimer's disease (AD). The aspartyl protease BACE1 catalyzes the rate-limiting step in the production of Aβ, and as such it is considered to be an important target for drug development in AD. The development of a BACE1 inhibitor therapeutic has proven to be difficult. The active site of BACE1 is relatively large. Consequently, to achieve sufficient potency, many BACE1 inhibitors have required unfavorable physicochemical properties such as high molecular weight and polar surface area that are detrimental to efficient passage across the blood-brain barrier. Using a rational drug design approach we have designed and developed a new series of hydroxyethylamine-based inhibitors of BACE1 capable of lowering Aβ levels in the brains of rats after oral administration. Herein we describe the in vitro and in vivo characterization of two of these molecules and the overall relationship of compound properties [e.g., in vitro permeability, P-glycoprotein (P-gp) efflux, metabolic stability, and pharmacological potency] to the in vivo pharmacodynamic effect with more than 100 compounds across the chemical series. We demonstrate that high in vitro potency for BACE1 was not sufficient to provide central efficacy. A combination of potency, high permeability, low P-gp-mediated efflux, and low clearance was required for compounds to produce robust central Aβ reduction after oral dosing.

Published

2012

20. P1‐243: Pharmacokinetic and pharmacodynamic evaluation of orally available hydroxyethylamine‐derived beta‐secretase inhibitors in Sprague Dawley rats

Author

Yi Luo, Matthew Weiss, Stephen J. Wood, Tom Dineen, Kui Chen, Jodi Bradley, Hongbing Huang, Ted Judd, Patricia Lopez, Li Zhu, Yuan Cheng, Patricia Amarante, Dean Hickman, Bryant Yang, Paul Acton, Safura Babu-Khan, Steven W. Louie, Mathew Kaller, Joel Esmay, Jan Zhang, Russell Graceffa, Wenge Zhong, Daniel B. Horne, Toni Williamson, Paul H. Wen, and Robert C. Wahl

Subjects

biology, Epidemiology, Chemistry, Health Policy, Pharmacology, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Pharmacokinetics, Pharmacodynamics, Sprague dawley rats, biology.protein, Neurology (clinical), Geriatrics and Gerontology, Beta (finance), Amyloid precursor protein secretase

Published

2012

21. Chromosomal localization of human genes for arylamine N-acetyltransferase

Author

Nigel K. Spurr, Edith Sim, Angela Risch, A McCarthy, S J Jeremiah, Dean Hickman, and V Buckle

Subjects

Yeast artificial chromosome, Arylamine N-Acetyltransferase, Molecular Sequence Data, In situ hybridization, Biology, Polymerase Chain Reaction, Biochemistry, chemistry.chemical_compound, Gene mapping, Humans, heterocyclic compounds, Chromosomes, Artificial, Yeast, Molecular Biology, In Situ Hybridization, Fluorescence, DNA Primers, Genetics, Base Sequence, Arylamine N-acetyltransferase, Chromosome Mapping, Chromosome, Cell Biology, biochemical phenomena, metabolism, and nutrition, bacterial infections and mycoses, Molecular biology, Phenotype, Benzidine, carbohydrates (lipids), Blotting, Southern, chemistry, bacteria, Human genome, Research Article, Chromosomes, Human, Pair 8

Abstract

Arylamine N-acetyltransferase is encoded at two loci, AAC-1 and AAC-2, on human chromosome 8. The products of the two loci are able to catalyse N-acetylation of arylamine carcinogens, such as benzidine and other xenobiotics. AAC-2 is polymorphic and individuals carrying the slow-acetylator phenotype are more susceptible to benzidine-induced bladder cancer. We have identified yeast artificial chromosome clones encoding AAC-1 and AAC-2 and have used the cloned DNAs as fluorescent probes for in situ hybridization. The hybridization patterns allow assignment of AAC-1 and AAC-2 to chromosome 8p21.3-23.1, a region in which deletions have been associated with bladder cancer [Knowles, Shaw and Proctor (1993) Oncogene 8, 1357-1364].

Published

1994

22. Genotyping human polymorphic arylamine N-acetyltransferase: identification of new slow allotypic variants

Author

Angela Risch, Jeremy P. Camilleri, Dean Hickman, and Edith Sim

Subjects

Adult, Genotype, Arylamine N-Acetyltransferase, Molecular Sequence Data, Population, Biology, Polymerase Chain Reaction, Genetics, Humans, Cloning, Molecular, General Pharmacology, Toxicology and Pharmaceutics, Allele, education, Gene, Genotyping, Alleles, Aged, education.field_of_study, Polymorphism, Genetic, Base Sequence, Point mutation, Penicillamine, Gene Amplification, Wild type, DNA, Middle Aged, Proteinuria, Restriction enzyme

Abstract

Arylamine N-acetyltransferase catalyses the N-acetylation of primary arylamine and hydrazine drugs and chemicals. N-acetylation is subject to a polymorphism and humans can be categorized as either fast or slow acetylators according to their ability to N-acetylate polymorphic substrates in vivo. Previously, slow acetylation has been linked to four distinct polymorphic N-acetyltransferase (pnat) alleles each of which contains one or more point mutations within the coding region of the pnat gene. One new rare slow variant of pnat has been identified by cloning and sequencing the pnat DNA from an individual whose NAT phenotype was determined by in vivo acetylation of the polymorphic substrate sulphamethazine. This allele, designated S1c, differs from the wild type fast allele at nucleotide positions 341 and 803. A second new rare slow allotypic variant, designated S3, has been identified by resistance of the pnat specific DNA to digestion with the restriction enzymes Fok I and Bam HI. A method of genotyping individuals for the arylamine N-acetyltransferase (NAT) polymorphism is presented which correctly predicts the phenotype of greater than 95% (21 of 22) of individuals as measured by the extent of acetylation of sulphamethazine in urine. This refined genotyping method was applied to a clinical population of 48 Caucasians with classical or definite rheumatoid arthritis each receiving daily between 150 and 500 mg of the anti-rheumatic drug, D-penicillamine. There is no difference in the N-acetyltransferase phenotype of the individuals who developed proteinuria and the control group with no adverse effects.

Published

1992

23. Arylamine N-acetyltransferase in human red blood cells

Author

Jonathan Gordon, Edith Sim, Dean Hickman, and Alison Ward

Subjects

Erythrocytes, Genotype, Arylamine N-Acetyltransferase, Molecular Sequence Data, Biology, Biochemistry, chemistry.chemical_compound, Folic Acid, medicine, 4-Aminobenzoic acid, Humans, Allele, Gene, Pharmacology, chemistry.chemical_classification, Base Sequence, Arylamine N-acetyltransferase, Gene Amplification, DNA Restriction Enzymes, Molecular biology, Kinetics, Red blood cell, Restriction enzyme, Methotrexate, Enzyme, medicine.anatomical_structure, chemistry, 4-Aminobenzoic Acid

Abstract

N-Acetyltransferase activities associated with erythrocytes from 20 individuals have been determined with p-aminobenzoic acid as substrate. A three-fold variation in Vmax is found. The N-acetyltransferase genotype of the individuals has been determined and there is no correlation between the extent of acetylation measured in the individuals' erythrocytes and the inheritance of alleles at the polymorphic NAT locus. Folate is confirmed to be an inhibitor of arylamine N-acetyltransferase activity measured in erythrocytes. The content of folate in erythrocytes of individuals also varies. The individual with the maximum folate content has the minimum N-acetyltransferase activity. The monomorphic N-acetyltransferase gene from individuals spanning the range of N-acetyltransferase activity have been amplified, using the polymerase chain reaction. The pattern of restriction enzyme digestion of the monomorphic N-acetyltransferase gene with a series of eight restriction enzymes is the same for individuals spanning the activity range of arylamine N-acetyltransferase in their erythrocytes.

Published

1992

24. In vitro metabolism of the novel, highly selective oral angiogenesis inhibitor motesanib diphosphate in preclinical species and in humans

Author

Dean Hickman, Sekhar Surapaneni, Chun Li, Mita Kuchimanchi, Raju Subramanian, Gondi N. Kumar, Mike Hayashi, Leszek Poppe, and Yihong Zhou

Subjects

Indoles, Magnetic Resonance Spectroscopy, Metabolite, Pharmaceutical Science, Administration, Oral, Pharmacology, Isozyme, Receptor tyrosine kinase, Motesanib Diphosphate, chemistry.chemical_compound, Glucuronides, Growth factor receptor, Cytochrome P-450 Enzyme System, Motesanib, Humans, Glucuronosyltransferase, Biotransformation, biology, Cytochrome P450, chemistry, Biochemistry, biology.protein, Microsome, Hepatocytes, Metabolome, Microsomes, Liver, Hydroxymethylglutaryl-CoA Reductase Inhibitors, Metabolic Networks and Pathways

Abstract

Motesanib diphosphate is a novel, investigational, highly selective oral inhibitor of the receptor tyrosine kinases vascular endothelial growth factor receptors 1, 2, and 3, the platelet-derived growth factor receptor, and the stem cell factor receptor (Kit). The in vitro metabolic profiles of [(14)C]motesanib were examined by using microsomes and hepatocytes from preclinical species and humans. Several oxidative metabolites were observed and characterized by tandem mass spectrometry, nuclear magnetic resonance spectroscopy, and coinjection with authentic standards. Cytochrome P450 (P450) 3A4 is the major isozyme involved in the oxidative biotransformation of motesanib, but the CYP2D6 and CYP1A isozymes also make minor contributions. In hepatocyte incubations, oxidative and conjugative pathways were observed for all species examined, and indoline N-glucuronidation was the dominant pathway. Three less common and novel phase II conjugates of the indoline nitrogen were detected in hepatocytes and in microsomes supplemented with specific cofactors, including N-carbamoyl glucuronide, N-glucose, and N-linked beta-N-acetylglucosamine. An N-glucuronide metabolite was the most frequently observed phase II conjugate in liver microsomes of all species, whereas the N-acetylglucosamine conjugate was observed only in monkey liver microsomes. Incubations with recombinant human UDP-glucuronosyltransferases (UGTs) and inhibition by the UGT1A4 and UGT1A1 substrates/inhibitors imipramine and bilirubin suggested that UGT1A4 is the major UGT isozyme catalyzing the N-glucuronidation of motesanib, with a minor contribution from UGT1A1. The in vitro metabolic profiles were similar between the human and preclinical species examined. All metabolites found in humans were also detected in other species.

Published

2009

25. N-acetyltransferase polymorphism

Author

Edith Sim and Dean Hickman

Subjects

Pharmacology, Genetics, endocrine system, education.field_of_study, fungi, Population, Locus (genetics), Biology, Biochemistry, Molecular biology, Nat, Genetic marker, Genotype, Allele, education, Genotyping, Arylamine N-acetyltransferase activity

Abstract

N -Acetyltransferase (NAT) isoenzymes are encoded at two loci. One locus encodes an NAT which is expressed widely in tissues, does not vary amongst human individuals and is termed monomorphic NAT (mNAT). The second locus encodes an NAT which is termed polymorphic NAT (pNAT), has a distinct tissue distribution and is responsible for the difference in ability between individuals in acetylating certain arylamine (e.g. sulphamethazine) and hydrazine (e.g. isoniazid) drugs which are polymorphic substrates. We describe a simple DNA based method for genotyping individuals for pNAT. The ‘fast’ NAT allele (F1) and the three ‘slow’ alleles (S1, S2 and S3) can be distinguished by using PCR with oligonucleotide primers specific for pNAT followed by restriction enzyme digestion of the amplified product. Heterozygotes are easily identified. The genotype of individual Caucasians compares well with the extent of acetylation of sulphamethazine. The allele distribution of the Caucasian population described here differs from that reported after Southern blot analysis of a Japanese population (Deguchi et al , J Biol Chem 265 : 12757–12760, 1990). The most frequent allele at the polymorphic nat locus in Caucasians, S1, is absent in the Japanese population. This difference between the two populations is likely to be the basis of the known interethnic variation in acetylator phenotype frequencies.

Published

1991

26. Further studies with the 2-amino-1,3-thiazol-4(5H)-one class of 11beta-hydroxysteroid dehydrogenase type 1 inhibitors: reducing pregnane X receptor activity and exploring activity in a monkey pharmacodynamic model

Author

Maury G Emery, Anil S. Guram, Qingyian Liu, Renee Komorowski, Michael Hayashi, Randall W. Hungate, David J. St. Jean, Eric A. Bercot, Nianhe Han, Jiandong Zhang, Qiuping Ye, Rod Cupples, Christopher H. Fotsch, Xiping Zhang, Chester Chenguang Yuan, Guy Matsumoto, Guifen Xu, Jenne Fretland, Michael D. Bartberger, Stefania Ursu, Clarence Hale, Minghan Wang, Hua Tu, Murielle M. Véniant, Dean Hickman, and Michelle Chen

Subjects

Male, Models, Molecular, Receptors, Steroid, Stereochemistry, Chemistry, Pharmaceutical, Molecular Conformation, Dehydrogenase, Crystallography, X-Ray, 11β-hydroxysteroid dehydrogenase type 1, Oxidoreductase, Drug Discovery, 11-beta-Hydroxysteroid Dehydrogenase Type 1, Animals, Cytochrome P-450 CYP3A, Humans, Tissue Distribution, Enzyme Inhibitors, chemistry.chemical_classification, Pregnane X receptor, biology, Pregnane X Receptor, Cytochrome P450, In vitro, Kinetics, Macaca fascicularis, Enzyme, Nuclear receptor, chemistry, Biochemistry, Drug Design, biology.protein, Molecular Medicine

Abstract

A series of compounds containing the 2-amino-1,3-thiazol-4(5H)-one core were found to be potent inhibitors of the enzyme 11beta-hydroxysteroid dehydrogenase type 1 (11beta-HSD1). One of our lead compounds from this series activated the human nuclear xenobiotic receptor, pregnane X receptor (PXR). To try and mitigate the PXR activity, we prepared analogues of our lead series that contained polar groups on the right-hand side of the thiazolone. Several analogues containing amides or alcohols appended to the C-5 position of the thiazolone showed a significant reduction in PXR activity. Through these structure-activity efforts, a compound containing a tert-alcohol group off the C-5 position, analogue (S)-33a, was found to have an 11beta-HSD1 Ki = 35 nM and negligible PXR activity. Compound (S)-33a was advanced into a pharmacodynamic model in cynomolgus monkeys, where it inhibited adipose 11beta-HSD1 activity after being orally administered.

Published

2008

27. Discovery of N-(4-(3-amino-1H-indazol-4-yl)phenyl)-N'-(2-fluoro-5-methylphenyl)urea (ABT-869), a 3-aminoindazole-based orally active multitargeted receptor tyrosine kinase inhibitor

Author

Patrick A. Marcotte, Steven K. Davidsen, Joy Bauch, Junling Li, Yujia Dai, Niru B. Soni, David R. Reuter, Lori J. Pease, Paul Tapang, Dean Hickman, Christopher M. Harris, Donald J. Osterling, Amanda M. Olson, Vincent S. Stoll, Ruth L. Martin, Kent D. Stewart, Asma A Ahmed, George A. Cunha, Kresna Hartandi, Daniel H. Albert, Zhiqin Ji, Maria D Moskey, Jennifer J. Bouska, Peter F. Bousquet, Jun Guo, Michael R. Michaelides, Kennan C. Marsh, and Keith B. Glaser

Subjects

Male, Models, Molecular, Platelet-derived growth factor, Indazoles, Receptor Protein-Tyrosine Kinases, Administration, Oral, Angiogenesis Inhibitors, Receptor tyrosine kinase, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Adenosine Triphosphate, Growth factor receptor, Drug Discovery, Animals, Edema, Humans, Phosphorylation, Binding Sites, biology, Estradiol, Phenylurea Compounds, Uterus, Xenograft Model Antitumor Assays, Linifanib, chemistry, Biochemistry, Enzyme inhibitor, biology.protein, NIH 3T3 Cells, Molecular Medicine, Female, Signal transduction, Tyrosine kinase, Hydrophobic and Hydrophilic Interactions

Abstract

In our continued efforts to search for potent and novel receptor tyrosine kinase (RTK) inhibitors as potential anticancer agents, we discovered, through a structure-based design, that 3-aminoindazole could serve as an efficient hinge-binding template for kinase inhibitors. By incorporating an N,N'-diaryl urea moiety at the C4-position of 3-aminodazole, a series of RTK inhibitors were generated, which potently inhibited the tyrosine kinase activity of the vascular endothelial growth factor receptor and the platelet-derived growth factor receptor families. A number of compounds with potent oral activity were identified by utilizing an estradiol-induced mouse uterine edema model and an HT1080 human fibrosarcoma xenograft tumor model. In particular, compound 17p (ABT-869) was found to possess favorable pharmacokinetic profiles across different species and display significant tumor growth inhibition in multiple preclinical animal models.

Published

2007

28. Enzyme kinetic properties of human recombinant arylamine N-acetyltransferase 2 allotypic variants expressed in Escherichia coli

Author

Jairam R. Palamanda, Dean Hickman, Edith Sim, and Jashvant D. Unadkat

Subjects

Arylamine N-Acetyltransferase, Genetic Vectors, Molecular Sequence Data, medicine.disease_cause, Biochemistry, law.invention, chemistry.chemical_compound, law, medicine, Escherichia coli, Humans, Cloning, Molecular, Pharmacology, chemistry.chemical_classification, biology, Arylamine N-acetyltransferase, Base Sequence, Acetyl-CoA, Active site, DNA, Recombinant Proteins, Isoenzymes, Kinetics, Enzyme, chemistry, Acetylation, Acetyltransferase, Recombinant DNA, biology.protein

Abstract

Arylamine N -acetyltransferase (NAT2) catalyses the N -acetylation of primary arylamine and hydrazine drugs and chemicals. N -Acetylation is subject to polymorphism, and humans can be categorized as either fast or slow acetylators according to their ability to N -acetylate certain arylamine substrates in vivo . Genetic variants at the polymorphic NAT2 locus have been described. We expressed five of the most common NAT2 variants (NAT2 4, NAT2 5A, NAT2 5B, NAT2 6A and NAT2 7B) in Escherichia coli as a convenient source of the human variants. The apparent K m values (at 100 μM acetyl CoA as co-substrate) of the different NAT2 variants for sulphamethazine, dapsone, p -anisidine, 2-aminofluorene, procainamide and isoniazid were determined. Data show that the apparent K m of the slow variant NAT2 7B for the arylamine sulphamethazine was 10-fold lower than all the other allotypes. The apparent K m for the structurally related sulphone antibiotic dapsone was 5-fold lower for the slow variant NAT2 7B when compared with the wild-type NAT2 4. These results indicate that the NAT2 7B specific amino acid substitution, Gly286-Glu, is important in promoting the binding of sulphamethazine and dapsone to the active site.

Published

1995