Your search keyword '"David Barnes-Seeman"' showing total 16 results

1. Clearance of plasma PCSK9 via the asialoglycoprotein receptor mediated by heterobifunctional ligands

Author

Jeffrey T. Bagdanoff, Thomas M. Smith, Martin Allan, Peter O’Donnell, Zachary Nguyen, Elizabeth A. Moore, Jason Baird, Shuangxi Wang, Vanitha Subramanian, Bruno Tigani, David O. Nettleton, Lauren G. Monovich, Ian Lewis, Alec N. Flyer, Brian Granda, John W. Blankenship, David Barnes-Seeman, and Kevin B. Clairmont

Subjects

Pharmacology, Clinical Biochemistry, Drug Discovery, Molecular Medicine, Molecular Biology, Biochemistry

Published

2023

2. Structure-Based Design and Preclinical Characterization of Selective and Orally Bioavailable Factor XIa Inhibitors: Demonstrating the Power of an Integrated S1 Protease Family Approach

Author

Allan D'Arcy, Nikolaus Schiering, Cary Fridrich, Yu-Hsin Chiu, Donglei Liu, Micah Hollis-Symynkywicz, Edwige Lorthiois, Hyungchul Kim, Darija Dedic, Richard Sedrani, Rose Mo, Solene Dussauge, Calhoun Amy, Stefanie Harlfinger, Treeve Currie, Simon Ruedisser, Lionel Muller, Rohit Duvadie, Ulrich Hassiepen, Adelaide Druet, Louise Kirman, Jason Elliott, Kenji Namoto, Gabriela Monnet, Francesca Perruccio, Paul Ramage, Eva Altmann, David Louis Feldman, Fabien Tritsch, Xueming Huang, Joerg Berghausen, Tanzina Fazal, Richard Zessis, James Roache, Eric T Williams, Christopher M. Adams, Wilhelm A. Weihofen, Viktor Hornak, Peter Delgado, Peter Hoffmann, David Barnes-Seeman, Douglas Bevan, ShuangXi Wang, Hong Liu, Martin Renatus, Celine Dentel, Corinne Durand, Juergen Klaus Maibaum, Guiqing Liang, Kamal Fettis, Gordon Turner, Rajeshri Ganesh Karki, Loren Lindsley, Julie Lachal, and Andreas Hein

Subjects

Drug, Male, Proteases, Peptidomimetic, medicine.medical_treatment, media_common.quotation_subject, Drug Evaluation, Preclinical, Administration, Oral, Biological Availability, Pharmacology, 01 natural sciences, Factor XIa, Rats, Sprague-Dawley, 03 medical and health sciences, Mice, Structure-Activity Relationship, Dogs, Complement Factor D, Drug Discovery, medicine, Animals, Humans, Amino Acid Sequence, 030304 developmental biology, ADME, media_common, Serine protease, 0303 health sciences, Protease, biology, Chemistry, 0104 chemical sciences, Rats, Mice, Inbred C57BL, 010404 medicinal & biomolecular chemistry, Coagulation, biology.protein, Molecular Medicine, Factor Xa Inhibitors

Abstract

The serine protease Factor XI (FXI) is a prominent drug target as it holds promise to deliver efficacious anti-coagulation without an enhanced risk of major bleeds. Several efforts have been described targeting the active form of the enzyme, FXIa. Herein we disclose our efforts to identify potent, selective, and orally bioavailable inhibitors of FXIa. Compound 1, identified from a diverse library of internal serine protease inhibitors, was originally designed as a complement Factor D inhibitor and exhibited sub-micromolar FXIa activity and an encouraging ADME profile while being devoid of peptidomimetic architecture. Optimization of interactions in the S1, S1β, and S1` pockets of FXIa through a combination of structure-based drug design and traditional medicinal chemistry led to the discovery of compound 23 with sub-nanomolar potency on FXIa, enhanced selectivity over other coagulation proteases, and a pre-clinical PK profile consistent with bid dosing in patients.

Published

2020

3. Correlation Between Nasal Epithelial Injury and In Vitro Cytotoxicity Using a Series of Small Molecule Protein Tyrosine Phosphatase 1B Inhibitors Investigated for Reversal of Leptin Resistance in Obesity

Author

Alan P. Brown, Ma Fupeng, Kayo Yasoshima, Ken Yamada, Patrick J. Devine, Chandrassegar Saravanan, David Barnes-Seeman, Maria Magnifico, Valerie Beaulieu, and Jiaping Gao

Subjects

0301 basic medicine, Male, Pharmacology, Biology, Toxicology, 03 medical and health sciences, chemistry.chemical_compound, Eating, Mice, Structure-Activity Relationship, Paraquat, In vivo, medicine, Animals, Obesity, Enzyme Inhibitors, Mode of action, Cytotoxicity, Administration, Intranasal, Cells, Cultured, Protein Tyrosine Phosphatase, Non-Receptor Type 1, Dose-Response Relationship, Drug, Fibroblasts, In vitro, Rats, Ketorolac, Mice, Inbred C57BL, Nasal Mucosa, 030104 developmental biology, chemistry, Toxicity, Immunology, Nasal administration, hormones, hormone substitutes, and hormone antagonists, medicine.drug

Abstract

This research provides a cautionary example when evaluating changes in behavioral end points with respect to postulated pharmacologic activity. Various small molecule substrate mimetic protein tyrosine phosphatase 1B (PTP1B) inhibitors were investigated as pharmacologic agents for decreasing food consumption using intranasal (IN) dosing as a means for direct nose-to-brain delivery along the olfactory/trigeminal nerve pathways. Although food consumption was decreased in diet-induced obese (DIO) mice, nasal discharge was observed. Studies were conducted to investigate local effects on the nasal airway and to develop structure–activity relationships. Intranasal administration of PTP1B inhibitors at ≥0.03 mg/d to DIO mice produced dose-dependent injury to various cell types of the nasal epithelia. Protein tyrosine phosphatase 1B inhibitors with calculated log octanol >3.0 were the most toxic. Whereas a pharmacologically inactive analog of a PTP1B inhibitor produced nasal injury, along with decreased food consumption, the marketed IN drug ketorolac produced no lesions at the same dose of 0.3 mg/d and only minor changes at 3 mg/d. Rat skin fibroblast cells were exposed in vitro to PTP1B inhibitors, ketorolac, paraquat, and the detergent sodium dodecylbenzene sulfonate (NDS) followed by measures of cytotoxicity. The most potent PTP1B inhibitors were similar to NDS, whereas ketorolac was the least toxic compound. Cytotoxic potency in vitro was similar to in vivo. In conclusion, PTP1B inhibitors injured nasal epithelium through a mechanism independent of PTP1B inhibition and likely due to nonspecific cytotoxicity such as disruption of the cell membrane. Decreased food consumption in DIO mice was due to toxicity rather than a pharmacologic mode of action.

Published

2017

4. Design and synthesis of lactam–thiophene carboxylic acids as potent hepatitis C virus polymerase inhibitors

Author

Carri Boiselle, Christina Capacci-Daniel, Mei Xu, Leah Whiteman, Sue Ma, Kai Lin, Christopher T. Jones, Rajiv Chopra, Guoyu Pan, Mitsunori Kato, Zheng Rui, Lei Shu, Keith Hoffmaster, David Barnes-Seeman, Jiping Fu, and Jianling Wang

Subjects

Lactams, Stereochemistry, viruses, Carboxylic acid, Hepatitis C virus, Clinical Biochemistry, Carboxylic Acids, Pharmaceutical Science, Hepacivirus, Thiophenes, Viral Nonstructural Proteins, medicine.disease_cause, Antiviral Agents, Biochemistry, Structure-Activity Relationship, chemistry.chemical_compound, Dogs, Amide, Drug Discovery, medicine, Thiophene, Animals, Enzyme Inhibitors, Molecular Biology, NS5B, Polymerase, chemistry.chemical_classification, Dose-Response Relationship, Drug, Molecular Structure, biology, Organic Chemistry, biochemical phenomena, metabolism, and nutrition, RNA-Dependent RNA Polymerase, Rats, chemistry, Drug Design, Lactam, biology.protein, Molecular Medicine, Lead compound

Abstract

Herein we report the successful incorporation of a lactam as an amide replacement in the design of hepatitis C virus NS5B Site II thiophene carboxylic acid inhibitors. Optimizing potency in a replicon assay and minimizing potential risk for CYP3A4 induction led to the discovery of inhibitor 22a. This lead compound has a favorable pharmacokinetic profile in rats and dogs.

Published

2014

5. Fluorinated Compounds in Medicinal Chemistry: Recent Applications, Synthetic Advances and Matched-Pair Analyses

Author

David Barnes-Seeman, Jeremy M. Beck, and Clayton Springer

Subjects

Trifluoromethyl, Halogenation, Drug discovery, Chemistry, Chemistry, Pharmaceutical, Matched-Pair Analysis, Fluorine Compounds, General Medicine, Medicinal chemistry, Combinatorial chemistry, Matched pair, chemistry.chemical_compound, Drug Discovery, Humans, Organic chemistry, ADME

Abstract

In recent years, several new fluorinated functional groups have been employed in medicinal chemistry. This review will highlight some recent developments in this area. We draw attention to useful synthetic advances for the installation of fluorine-containing groups. In addition, we examine the application of some fluorinated functional groups that have recently been gaining popularity in drug discovery. We use matched-pair analysis to assemble aggregate data on the impact on potency of one of these groups, pentafluorosulfanyl, as compared to trifluoromethyl. We further used matchedpair analysis to identify some interesting effects on in vitro ADME properties of replacing H by F on certain moieties.

Published

2014

6. A Robust Small-Molecule Microarray Platform for Screening Cell Lysates

Author

Jasmeet Dhaliwal, Ralph Mazitschek, Seung Bum Park, Paul Nghiem, James E. Bradner, Kristen E. Stevenson, Angela N. Koehler, Donna Neuberg, Olivia M. McPherson, Stuart L. Schreiber, John Paul Shen, Jay L. Duffner, and David Barnes-Seeman

Subjects

Cell lysates, Clinical Biochemistry, Tacrolimus Binding Protein 1A, Biology, 010402 general chemistry, 01 natural sciences, Biochemistry, Fluorescence, Cell Line, chemistry.chemical_compound, Drug Discovery, Humans, Microarray platform, Molecular Biology, Oligonucleotide Array Sequence Analysis, Pharmacology, 010405 organic chemistry, General Medicine, Combinatorial chemistry, Small molecule, 3. Good health, 0104 chemical sciences, CHEMBIO, chemistry, Covalent bond, Functional group, Molecular Medicine, DNA microarray

Abstract

SummaryHerein we report the expanded functional group compatibility of small-molecule microarrays to include immobilization of primary alcohols, secondary alcohols, phenols, carboxylic acids, hydroxamic acids, thiols, and amines on a single slide surface. Small-molecule “diversity microarrays” containing nearly 10,000 known bioactive small molecules, natural products, and small molecules originating from several diversity-oriented syntheses were produced by using an isocyanate-mediated covalent capture strategy. Selected printed bioactive compounds were detected with antibodies against compounds of interest. The new surface of the diversity microarrays is highly compatible with approaches involving cellular lysates. This feature has enabled a robust, optimized screening methodology using cellular lysates, allowing the detection of specific interactions with a broad range of binding affinity by using epitope-tagged or chimeric fluorescent proteins without prior purification. We believe that this expanded research capability has considerable promise in biology and medicine.

Published

2006

7. Metabolically Stable tert-Butyl Replacement

Author

Jakal Amin, Scott Louis Cohen, Brad Snodgrass, Xiao-Hui Chen, Monish Jain, Panos Hatsis, Suzie Ferreira, David Barnes-Seeman, and Leslie Bell

Subjects

Tert butyl, Biochemistry, In vivo, business.industry, Organic Chemistry, Drug Discovery, Medicine, Metabolism, Metabolic stability, Bioinformatics, business, In vitro

Abstract

Susceptibility to metabolism is a common issue with the tert-butyl group on compounds of medicinal interest. We demonstrate an approach of removing all the fully sp(3) C-Hs from a tert-butyl group: replacing some C-Hs with C-Fs and increasing the s-character of the remaining C-Hs. This approach gave a trifluoromethylcyclopropyl group, which increased metabolic stability. Trifluoromethylcyclopropyl-containing analogues had consistently higher metabolic stability in vitro and in vivo compared to their tert-butyl-containing counterparts.

Published

2013

8. A transition-state model for the mikami enantioselective ene reaction

Author

Steven N. Goodman, David Barnes-Seeman, E. J. Corey, and Thomas W. Lee

Subjects

State model, Chemistry, Stereochemistry, Organic Chemistry, Drug Discovery, Enantioselective synthesis, Biochemistry, Ene reaction

Abstract

A logically derived mechanistic model is presented for the Mikami enantioselective ene reaction which correctly describes the absolute and relative stereochemistry resulting from transition-state structures such as 3 and 5.

Published

1997

9. The formyl CH--O hydrogen bond as a critical factor in enantioselective reactions of aldehydes, part 4. Aldol, ethylation, hydrocyanation and Diels-Alder reactions catalyzed by chiral B, Ti and Al lewis acids

Author

E. J. Corey, Thomas W. Lee, and David Barnes-Seeman

Subjects

Addition reaction, Hydrogen bond catalysis, Aldol reaction, Chemistry, Hydrogen bond, Organic Chemistry, Drug Discovery, Hydrocyanation, Enantioselective synthesis, Organic chemistry, Lewis acids and bases, Biochemistry, Catalysis

Abstract

Formyl CH--O hydrogen bonding provides a rational explanation of several diverse catalytic enantioselective addition reactions of aldehydes, as outlined in Figures 1–5.

Published

1997

10. The formyl CH--O hydrogen bond as a key to transition-state organization in enantioselective allylation, aldol and Diels-Alder reactions catalyzed by chiral lewis acids

Author

E. J. Corey, David Barnes-Seeman, and Thomas W. Lee

Subjects

Hydrogen bond catalysis, Chemistry, Hydrogen bond, Organic Chemistry, Enantioselective synthesis, Chiral Lewis acid, Biochemistry, Catalysis, chemistry.chemical_compound, Aldol reaction, Drug Discovery, Diels alder, Organic chemistry, Lewis acids and bases

Abstract

The occurrence of formyl CH--O hydrogen bonding in enantioselective allylation, aldol and Diels-Alder reactions of aldehydes with chiral Lewis acid catalysts is a key to the understanding of absolute stereochemistry.

Published

1997

11. ChemInform Abstract: A Transition-State Model for the Mikami Enantioselective Ene Reaction

Author

Thomas W. Lee, Steven N. Goodman, David Barnes-Seeman, and E. J. Corey

Subjects

State model, Chemistry, Computational chemistry, Enantioselective synthesis, General Medicine, Ene reaction

Abstract

A logically derived mechanistic model is presented for the Mikami enantioselective ene reaction which correctly describes the absolute and relative stereochemistry resulting from transition-state structures such as 3 and 5.

Published

2010

12. The mechanistic basis for diastereoselectivity in the Matteson rearrangement

Author

David Barnes-Seeman, Thomas W. Lee, and E. J. Corey

Subjects

Inorganic Chemistry, Denticity, Chemistry, Stereochemistry, Organic Chemistry, Lewis acids and bases, Physical and Theoretical Chemistry, Sigmatropic reaction, Catalysis, Transition state, Carroll rearrangement, Cope rearrangement

Abstract

The diastereoselective rearrangement of α,α-dichloromethylboronate derivatives of chiral 1,2-diols (Matteson rearrangement) can be understood readily in terms of a bidentate interaction between the catalytic Lewis acid (ZnCl 2 ) and the substrate, leading to favored transition states such as 4 and 5 .

Published

1997

13. A Two-Step Total Synthesis of the Natural Pentacycle Trichodimerol, a Novel Inhibitor of TNF-α Production

Author

E. J. Corey and David Barnes-Seeman

Subjects

Bridged-Ring Compounds, Trichodimerol, Molecular Structure, Tumor Necrosis Factor-alpha, Stereochemistry, TNF-alpha production, Spectrum Analysis, Organic Chemistry, Two step, Total synthesis, Tumor Necrosis Factor alpha biosynthesis, Biochemistry, chemistry.chemical_compound, chemistry, Molecule, Physical and Theoretical Chemistry, Spectrum analysis, Dimerization

Abstract

[formula: see text] Trichodimerol (1) can be synthesized by a remarkable dimerization of the chiral hydroxy dienone 5.

Published

1999

14. Titelbild: Expanding the Functional Group Compatibility of Small-Molecule Microarrays: Discovery of Novel Calmodulin Ligands (Angew. Chem. 21/2003)

Author

David Barnes-Seeman, Angela N. Koehler, Seung Bum Park, and Stuart L. Schreiber

Subjects

chemistry.chemical_compound, Calmodulin, biology, Chemistry, Functional group, Polymer chemistry, biology.protein, Compatibility (geochemistry), General Medicine, DNA microarray, Small molecule, Combinatorial chemistry

Published

2003

15. Expanding the Functional Group Compatibility of Small-Molecule Microarrays: Discovery of Novel Calmodulin Ligands () We are especially grateful to John Tallarico and Max Narovlyansky of the Harvard Institute of Chemistry and Cell Biology (ICCB) for donation of 2 b and synthesis resin, and to Jason Gatlin and Jennifer Raggio of the ICCB for their assistance with decoding. A.N.K. was supported by an Eli Lilly Predoctoral Fellowship. S.B.P. and D.B.-S. are Research Associates and S.L.S. is an Investigator at the Howard Hughes Medical Institute in the Department of Chemistry and Chemical Biology. We thank the National Institute for General Medical Sciences for support of this research, the National Cancer Institute (NCI), Merck KGaA, Merck & Co., and the Keck Foundation for support of the ICCB, and the NCI for support of the Initiative for Chemical Genetics (formerly known as the Molecular Target Laboratory).

Author

David Barnes-Seeman, Seung Bum Park, Angela N. Koehler, and Stuart L. Schreiber

Published

2003

16. Cover Picture: Expanding the Functional Group Compatibility of Small-Molecule Microarrays: Discovery of Novel Calmodulin Ligands (Angew. Chem. Int. Ed. 21/2003).

Author

David Barnes-Seeman, Seung Bum Park, Angela N. Koehler, and Stuart L. Schreiber

Published

2003