Your search keyword '"Rose Ann, Ferre"' showing total 31 results

1. Supplemental Tables S1-S9 from Spectrum and Degree of CDK Drug Interactions Predicts Clinical Performance

Author

Brion W. Murray, Todd VanArsdale, Asako Nagata, Xiu Yu, You-Ai He, Wade Diehl, James Solowiej, Simon Bergqvist, Hieu Lam, Rose Ann Ferre, Meirong Xu, Wenyue Hu, Nathan V. Lee, and Ping Chen

Abstract

Table S1. Statistics for the crystallographic analysis; Table S2. Biochemical and cellular potencies of the second generation CDK-directed drug AG-024322; Table S3. In vitro analysis of binding potency of abemaciclib, dinaciclib, and palbociclib to non-kinase proteins; Table S4. Broad kinase selectivity of selective CDK4/6 drugs; Table S5. Biochemical dose-response follow-up was conducted for a subset of kinases inhibited by the three CDK4/6 drugs using a Km concentration of ATP (Carna Biosciences) (CDK proteins excluded); Table S6. Kinase selectivity toward endogenous human kinases using irreversible ATP analog target engagement assay; Table S7. Biochemical potencies of selective CDK4/6 drugs palbociclib (PD-0332991); Table S8. Human pharmacokinetic properties of CDK-targeted drugs; Table S9. Isothermal titration calorimetry results for CDK-directed drugs binding to CDK6 in the absence of cyclin D.

Published

2023

2. Supplemental Methods from Spectrum and Degree of CDK Drug Interactions Predicts Clinical Performance

Author

Brion W. Murray, Todd VanArsdale, Asako Nagata, Xiu Yu, You-Ai He, Wade Diehl, James Solowiej, Simon Bergqvist, Hieu Lam, Rose Ann Ferre, Meirong Xu, Wenyue Hu, Nathan V. Lee, and Ping Chen

Abstract

Detailed description of the methods used in the manuscript

Published

2023

3. Novel isoquinolone PDK1 inhibitors discovered through fragment-based lead discovery.

Author

M. Catherine Johnson, Qiyue Hu, Laura Lingardo, Rose Ann Ferre, Samantha Greasley, Jiangli Yan, John Kath, Ping Chen, Jacques Ermolieff, and Gordon Alton

Published

2011

4. Discovery of PF-06873600, a CDK2/4/6 Inhibitor for the Treatment of Cancer

Author

Kephart Susan Elizabeth, Tran Khanh Tuan, Kevin Daniel Freeman-Cook, Sherry Niessen, James Solowiej, Buwen Huang, Qin Zhang, Douglas Carl Behenna, Inish O'Doherty, Sacha Ninkovic, Rose Ann Ferre, Andrea Hui, Nichol Miller, Jordan Carelli, Lisa Nguyen, Brion W. Murray, Robert Louis Hoffman, John Lapek, Rhys M. Jones, Meirong Xu, Stephen Dann, Sutton Scott Channing, Asako Nagata, Nanni Huser, Ravi Visswanathan, Zehnder Luke Raymond, Elaine E. Tseng, Britton Boras, You-Ai He, Michele McTigue, Wade Diehl, Cathy Zhang, and Martha A. Ornelas

Subjects

Drug, media_common.quotation_subject, Phases of clinical research, Administration, Oral, Antineoplastic Agents, 01 natural sciences, 03 medical and health sciences, Mice, Structure-Activity Relationship, Breast cancer, Dogs, Cyclin-dependent kinase, Drug Discovery, medicine, Tumor Cells, Cultured, Animals, Humans, Protein Kinase Inhibitors, 030304 developmental biology, media_common, ADME, Cell Proliferation, 0303 health sciences, biology, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Drug discovery, Cyclin-Dependent Kinase 2, Cancer, Cyclin-Dependent Kinase 4, Cyclin-Dependent Kinase 6, Neoplasms, Experimental, Cell cycle, medicine.disease, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Injections, Intravenous, biology.protein, Cancer research, Molecular Medicine, Female, Drug Screening Assays, Antitumor

Abstract

Control of the cell cycle through selective pharmacological inhibition of CDK4/6 has proven beneficial in the treatment of breast cancer. Extending this level of control to additional cell cycle CDK isoforms represents an opportunity to expand to additional tumor types and potentially provide benefits to patients that develop tumors resistant to selective CDK4/6 inhibitors. However, broad-spectrum CDK inhibitors have a long history of failure due to safety concerns. In this approach, we describe the use of structure-based drug design and Free-Wilson analysis to optimize a series of CDK2/4/6 inhibitors. Further, we detail the use of molecular dynamics simulations to provide insights into the basis for selectivity against CDK9. Based on overall potency, selectivity, and ADME profile, PF-06873600 (22) was identified as a candidate for the treatment of cancer and advanced to phase 1 clinical trials.

Published

2021

5. Expanding control of the tumor cell cycle with a CDK2/4/6 inhibitor

Author

Xinmeng Jasmine Mu, Meirong Xu, Shahram Salek-Ardakani, Cinthia Costa-Jones, Lisa Nguyen, James Solowiej, David Looper, Scott L. Weinrich, Robert Louis Hoffman, Sutton Scott Channing, Sacha Ninkovic, Kephart Susan Elizabeth, Sherry Niessen, John Chionis, Jadwiga Bienkowska, Kevin Daniel Freeman-Cook, Rose Ann Ferre, John Lapek, Cecilia Oderup, Jordan Carelli, Cathy Zhang, Nanni Huser, Elizabeth A. McMillan, Asako Nagata, Martha A. Ornelas, Brion W. Murray, Douglas Carl Behenna, Koleen Eisele, Todd VanArsdale, Zhou Zhu, Zhengyan Kan, Chaoting Liu, Nichol Miller, Zehnder Luke Raymond, Michael A. White, Ying Ding, Nathan V. Lee, Jonathan Almaden, Qin Zhang, Tran Khanh Tuan, Ping Wei, Stephen Dann, Britton Boras, Tim S. Wang, Ravi Visswanathan, You-Ai He, Michele McTigue, and Elizabeth Wilson

Subjects

Male, Cancer Research, Cyclin E, Palbociclib, Neoplasms, medicine, Humans, Oncogene, biology, business.industry, Cell Cycle, Cyclin-Dependent Kinase 2, Cyclin-dependent kinase 2, Cyclin-Dependent Kinase 4, Cancer, Cyclin-Dependent Kinase 6, Cell cycle, medicine.disease, Immune checkpoint, Oncology, Cancer research, biology.protein, Female, Cyclin-dependent kinase 6, biological phenomena, cell phenomena, and immunity, business

Abstract

Summary The CDK4/6 inhibitor, palbociclib (PAL), significantly improves progression-free survival in HR+/HER2− breast cancer when combined with anti-hormonals. We sought to discover PAL resistance mechanisms in preclinical models and through analysis of clinical transcriptome specimens, which coalesced on induction of MYC oncogene and Cyclin E/CDK2 activity. We propose that targeting the G1 kinases CDK2, CDK4, and CDK6 with a small-molecule overcomes resistance to CDK4/6 inhibition. We describe the pharmacodynamics and efficacy of PF-06873600 (PF3600), a pyridopyrimidine with potent inhibition of CDK2/4/6 activity and efficacy in multiple in vivo tumor models. Together with the clinical analysis, MYC activity predicts (PF3600) efficacy across multiple cell lineages. Finally, we find that CDK2/4/6 inhibition does not compromise tumor-specific immune checkpoint blockade responses in syngeneic models. We anticipate that (PF3600), currently in phase 1 clinical trials, offers a therapeutic option to cancer patients in whom CDK4/6 inhibition is insufficient to alter disease progression.

Published

2021

6. Discovery of N-((3R,4R)-4-Fluoro-1-(6-((3-methoxy-1-methyl-1H-pyrazol-4-yl)amino)-9-methyl-9H-purin-2-yl)pyrrolidine-3-yl)acrylamide (PF-06747775) through Structure-Based Drug Design: A High Affinity Irreversible Inhibitor Targeting Oncogenic EGFR Mutants with Selectivity over Wild-Type EGFR

Author

Chengyi Zhang, Sujin Cho-Schultz, Tran Khanh Tuan, Manli Shi, Rose Ann Ferre, Sherry Niessen, Sajiv Krishnan Nair, Douglas Carl Behenna, Dac M. Dinh, Elaine E. Tseng, Theodore O. Johnson, Cheng Hengmiao, Ru Zhou, Michael Zientek, T. Eric Ballard, Brion W. Murray, Suvi T. M. Orr, James Solowiej, Jennifer Lafontaine, Jean Joo Matthews, Scott L. Weinrich, Paolo Vicini, Deal Judith G, Longqing Liu, John Charles Kath, Pairish Mason Alan, Simon Paul Planken, Louise Bernier, Deepak Dalvie, Yiqin Luo, Martin Paul Edwards, Asako Nagata, Hong Shen, Neal W. Sach, Yuli Wang, Ketan S. Gajiwala, Shuibo Xin, Simon Bailey, Chau Almaden, Robert Steven Kania, and Michelle Hemkens

Subjects

0301 basic medicine, Mutation, biology, Chemistry, Mutant, Wild type, medicine.disease_cause, Molecular biology, respiratory tract diseases, 03 medical and health sciences, T790M, 030104 developmental biology, Drug Discovery, biology.protein, medicine, Molecular Medicine, Kinome, Epidermal growth factor receptor, Erlotinib, ADME, medicine.drug

Abstract

Mutant epidermal growth factor receptor (EGFR) is a major driver of non-small-cell lung cancer (NSCLC). Marketed first generation inhibitors, such as erlotinib, effect a transient beneficial response in EGFR mutant NSCLC patients before resistance mechanisms render these inhibitors ineffective. Secondary oncogenic EGFR mutations account for approximately 50% of relapses, the most common being the gatekeeper T790M substitution that renders existing therapies ineffective. The discovery of PF-06459988 (1), an irreversible pyrrolopyrimidine inhibitor of EGFR T790M mutants, was recently disclosed.1 Herein, we describe our continued efforts to achieve potency across EGFR oncogenic mutations and improved kinome selectivity, resulting in the discovery of clinical candidate PF-06747775 (21), which provides potent EGFR activity against the four common mutants (exon 19 deletion (Del), L858R, and double mutants T790M/L858R and T790M/Del), selectivity over wild-type EGFR, and desirable ADME properties. Compound 21 is ...

Published

2017

7. Discovery of 1-{(3R,4R)-3-[({5-Chloro-2-[(1-methyl-1H-pyrazol-4-yl)amino]-7H-pyrrolo[2,3-d]pyrimidin-4-yl}oxy)methyl]-4-methoxypyrrolidin-1-yl}prop-2-en-1-one (PF-06459988), a Potent, WT Sparing, Irreversible Inhibitor of T790M-Containing EGFR Mutants

Author

Marlena Walls, Tod Smeal, Suvi T. M. Orr, Zhengyu Liu, Cheng Hengmiao, Shuiwang Wang, Kephart Susan Elizabeth, Jean Joo Matthews, Rose Ann Ferre, Neal W. Sach, Scott L. Weinrich, Doug Behenna, Sherry Niessen, Sangita M. Baxi, Deepak Dalvie, Sujin Cho-Schultz, Dac M. Dinh, Kevin Ryan, Jim Solowiej, Elaine E. Tseng, Simon Paul Planken, Sajiv Krishnan Nair, Brion W. Murray, Jun Li Feng, Jennifer Lafontaine, Pairish Mason Alan, Shijian Ren, Michelle Hemkens, Shuibo Xin, Mehran Jalaie, Tran Khanh Tuan, Robert Steven Kania, Sutton Scott Channing, William F. Vernier, Kevin K.-C. Liu, Amy Jackson-Fisher, Beth Lunney, Min-Jean Yin, Ketan S. Gajiwala, Asako Nagata, Haiwei Xu, Michael Zientek, Ru Zhou, Daniel Tyler Richter, Simon Bailey, Martin Paul Edwards, Martha A. Ornelas, Chau Almaden, John Charles Kath, Hong Shen, and Theodore O. Johnson

Subjects

0301 basic medicine, Mutation, 010405 organic chemistry, Stereochemistry, Chemistry, Mutant, medicine.disease_cause, 01 natural sciences, respiratory tract diseases, 0104 chemical sciences, 03 medical and health sciences, T790M, 030104 developmental biology, Gefitinib, Protein kinase domain, Drug Discovery, Cancer research, medicine, Molecular Medicine, Potency, Reactivity (chemistry), Erlotinib, medicine.drug

Abstract

First generation EGFR TKIs (gefitinib, erlotinib) provide significant clinical benefit for NSCLC cancer patients with oncogenic EGFR mutations. Ultimately, these patients’ disease progresses, often driven by a second-site mutation in the EGFR kinase domain (T790M). Another liability of the first generation drugs is severe adverse events driven by inhibition of WT EGFR. As such, our goal was to develop a highly potent irreversible inhibitor with the largest selectivity ratio between the drug-resistant double mutants (L858R/T790M, Del/T790M) and WT EGFR. A unique approach to develop covalent inhibitors, optimization of reversible binding affinity, served as a cornerstone of this effort. PF-06459988 was discovered as a novel, third generation irreversible inhibitor, which demonstrates (i) high potency and specificity to the T790M-containing double mutant EGFRs, (ii) minimal intrinsic chemical reactivity of the electrophilic warhead, (iii) greatly reduced proteome reactivity relative to earlier irreversible E...

Published

2016

8. Discovery of N-((3R,4R)-4-Fluoro-1-(6-((3-methoxy-1-methyl-1H-pyrazol-4-yl)amino)-9-methyl-9H-purin-2-yl)pyrrolidine-3-yl)acrylamide (PF-06747775) through Structure-Based Drug Design: A High Affinity Irreversible Inhibitor Targeting Oncogenic EGFR Mutants with Selectivity over Wild-Type EGFR

Author

Simon, Planken, Douglas C, Behenna, Sajiv K, Nair, Theodore O, Johnson, Asako, Nagata, Chau, Almaden, Simon, Bailey, T Eric, Ballard, Louise, Bernier, Hengmiao, Cheng, Sujin, Cho-Schultz, Deepak, Dalvie, Judith G, Deal, Dac M, Dinh, Martin P, Edwards, Rose Ann, Ferre, Ketan S, Gajiwala, Michelle, Hemkens, Robert S, Kania, John C, Kath, Jean, Matthews, Brion W, Murray, Sherry, Niessen, Suvi T M, Orr, Mason, Pairish, Neal W, Sach, Hong, Shen, Manli, Shi, James, Solowiej, Khanh, Tran, Elaine, Tseng, Paolo, Vicini, Yuli, Wang, Scott L, Weinrich, Ru, Zhou, Michael, Zientek, Longqing, Liu, Yiqin, Luo, Shuibo, Xin, Chengyi, Zhang, and Jennifer, Lafontaine

Subjects

Models, Molecular, Acrylamides, Lung Neoplasms, Pyrrolidines, Halogenation, Rats, ErbB Receptors, Molecular Docking Simulation, Mice, Dogs, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, Drug Design, Mutation, Animals, Humans, Lung, Protein Kinase Inhibitors

Abstract

Mutant epidermal growth factor receptor (EGFR) is a major driver of non-small-cell lung cancer (NSCLC). Marketed first generation inhibitors, such as erlotinib, effect a transient beneficial response in EGFR mutant NSCLC patients before resistance mechanisms render these inhibitors ineffective. Secondary oncogenic EGFR mutations account for approximately 50% of relapses, the most common being the gatekeeper T790M substitution that renders existing therapies ineffective. The discovery of PF-06459988 (1), an irreversible pyrrolopyrimidine inhibitor of EGFR T790M mutants, was recently disclosed.1 Herein, we describe our continued efforts to achieve potency across EGFR oncogenic mutations and improved kinome selectivity, resulting in the discovery of clinical candidate PF-06747775 (21), which provides potent EGFR activity against the four common mutants (exon 19 deletion (Del), L858R, and double mutants T790M/L858R and T790M/Del), selectivity over wild-type EGFR, and desirable ADME properties. Compound 21 is currently being evaluated in phase-I clinical trials of mutant EGFR driven NSCLC.

Published

2017

9. Spectrum and Degree of CDK Drug Interactions Predicts Clinical Performance

Author

Todd VanArsdale, James Solowiej, Simon Bergqvist, You-Ai He, Wade Diehl, Rose Ann Ferre, Wenyue Hu, Hieu Lam, Brion W. Murray, Nathan V. Lee, Meirong Xu, Asako Nagata, Xiu Yu, and Ping Chen

Subjects

0301 basic medicine, Models, Molecular, Cancer Research, Cell Survival, Molecular Conformation, Antineoplastic Agents, Pharmacology, Biology, Palbociclib, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cyclin-dependent kinase, Cell Line, Tumor, Animals, Cluster Analysis, Humans, Kinome, Drug Interactions, Myocytes, Cardiac, Dinaciclib, Phosphorylation, Abemaciclib, Protein Kinase Inhibitors, Epithelial Cells, Cyclin-Dependent Kinases, Rats, 030104 developmental biology, Oncology, chemistry, Drug development, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Leukocytes, Mononuclear, Cyclin-dependent kinase 6, CDK inhibitor, Protein Binding

Abstract

Therapeutically targeting aberrant intracellular kinase signaling is attractive from a biological perspective but drug development is often hindered by toxicities and inadequate efficacy. Predicting drug behaviors using cellular and animal models is confounded by redundant kinase activities, a lack of unique substrates, and cell-specific signaling networks. Cyclin-dependent kinase (CDK) drugs exemplify this phenomenon because they are reported to target common processes yet have distinct clinical activities. Tumor cell studies of ATP-competitive CDK drugs (dinaciclib, AG-024322, abemaciclib, palbociclib, ribociclib) indicate similar pharmacology while analyses in untransformed cells illuminates significant differences. To resolve this apparent disconnect, drug behaviors are described at the molecular level. Nonkinase binding studies and kinome interaction analysis (recombinant and endogenous kinases) reveal that proteins outside of the CDK family appear to have little role in dinaciclib/palbociclib/ribociclib pharmacology, may contribute for abemaciclib, and confounds AG-024322 analysis. CDK2 and CDK6 cocrystal structures with the drugs identify the molecular interactions responsible for potency and kinase selectivity. Efficient drug binding to the unique hinge architecture of CDKs enables selectivity toward most of the human kinome. Selectivity between CDK family members is achieved through interactions with nonconserved elements of the ATP-binding pocket. Integrating clinical drug exposures into the analysis predicts that both palbociclib and ribociclib are CDK4/6 inhibitors, abemaciclib inhibits CDK4/6/9, and dinaciclib is a broad-spectrum CDK inhibitor (CDK2/3/4/6/9). Understanding the molecular components of potency and selectivity also facilitates rational design of future generations of kinase-directed drugs. Mol Cancer Ther; 15(10); 2273–81. ©2016 AACR.

Published

2016

10. Discovery of 1-{(3R,4R)-3-[({5-Chloro-2-[(1-methyl-1H-pyrazol-4-yl)amino]-7H-pyrrolo[2,3-d]pyrimidin-4-yl}oxy)methyl]-4-methoxypyrrolidin-1-yl}prop-2-en-1-one (PF-06459988), a Potent, WT Sparing, Irreversible Inhibitor of T790M-Containing EGFR Mutants

Author

Hengmiao, Cheng, Sajiv K, Nair, Brion W, Murray, Chau, Almaden, Simon, Bailey, Sangita, Baxi, Doug, Behenna, Sujin, Cho-Schultz, Deepak, Dalvie, Dac M, Dinh, Martin P, Edwards, Jun Li, Feng, Rose Ann, Ferre, Ketan S, Gajiwala, Michelle D, Hemkens, Amy, Jackson-Fisher, Mehran, Jalaie, Ted O, Johnson, Robert S, Kania, Susan, Kephart, Jennifer, Lafontaine, Beth, Lunney, Kevin K-C, Liu, Zhengyu, Liu, Jean, Matthews, Asako, Nagata, Sherry, Niessen, Martha A, Ornelas, Suvi T M, Orr, Mason, Pairish, Simon, Planken, Shijian, Ren, Daniel, Richter, Kevin, Ryan, Neal, Sach, Hong, Shen, Tod, Smeal, Jim, Solowiej, Scott, Sutton, Khanh, Tran, Elaine, Tseng, William, Vernier, Marlena, Walls, Shuiwang, Wang, Scott L, Weinrich, Shuibo, Xin, Haiwei, Xu, Min-Jean, Yin, Michael, Zientek, Ru, Zhou, and John C, Kath

Subjects

Models, Molecular, Lung Neoplasms, Dose-Response Relationship, Drug, Molecular Structure, ErbB Receptors, Structure-Activity Relationship, Pyrimidines, Carcinoma, Non-Small-Cell Lung, Drug Discovery, Mutation, Tumor Cells, Cultured, Humans, Mutant Proteins, Pyrroles, Protein Kinase Inhibitors

Abstract

First generation EGFR TKIs (gefitinib, erlotinib) provide significant clinical benefit for NSCLC cancer patients with oncogenic EGFR mutations. Ultimately, these patients' disease progresses, often driven by a second-site mutation in the EGFR kinase domain (T790M). Another liability of the first generation drugs is severe adverse events driven by inhibition of WT EGFR. As such, our goal was to develop a highly potent irreversible inhibitor with the largest selectivity ratio between the drug-resistant double mutants (L858R/T790M, Del/T790M) and WT EGFR. A unique approach to develop covalent inhibitors, optimization of reversible binding affinity, served as a cornerstone of this effort. PF-06459988 was discovered as a novel, third generation irreversible inhibitor, which demonstrates (i) high potency and specificity to the T790M-containing double mutant EGFRs, (ii) minimal intrinsic chemical reactivity of the electrophilic warhead, (iii) greatly reduced proteome reactivity relative to earlier irreversible EGFR inhibitors, and (iv) minimal activity against WT EGFR.

Published

2016

11. The Crystal Structure of the RNA-Dependent RNA Polymerase from Human Rhinovirus

Author

Wade Diehl, Robert A. Love, Peter S. Dragovich, Shella A. Fuhrman, Hans E. Parge, Xiu Yu, Laura Lingardo, Rose Ann Ferre, and Karen A. Maegley

Subjects

Genetics, viruses, Poliovirus, Hepatitis C virus, Picornaviridae, RNA-dependent RNA polymerase, RNA, Biology, medicine.disease_cause, Virology, Virus, chemistry.chemical_compound, chemistry, Structural Biology, RNA polymerase, medicine, Primer (molecular biology), Molecular Biology

Abstract

Human rhinoviruses (HRV), the predominant members of the Picornaviridae family of positive-strand RNA viruses, are the major causative agents of the common cold. Given the lack of effective treatments for rhinoviral infections, virally encoded proteins have become attractive therapeutic targets. The HRV genome encodes an RNA-dependent RNA polymerase (RdRp) denoted 3Dpol, which is responsible for replicating the viral genome and for synthesizing a protein primer used in the replication. Here the crystal structures for three viral serotypes (1B, 14, and 16) of HRV 3Dpol have been determined. The three structures are very similar to one another, and to the closely related poliovirus (PV) 3Dpol enzyme. Because the reported PV crystal structure shows significant disorder, HRV 3Dpol provides the first complete view of a picornaviral RdRp. The folding topology of HRV 3Dpol also resembles that of RdRps from hepatitis C virus (HCV) and rabbit hemorrhagic disease virus (RHDV) despite very low sequence homology.

Published

2004

12. Structure of pteridine reductase (PTR1) fromLeishmania tarentolae

Author

Ming Zhao, Haiyan Zhao, David A. Matthews, Kottayil I. Varughese, Rose Ann Ferre, Tom Bray, John M. Whiteley, and Marc Ouellette

Subjects

Models, Molecular, Protein Conformation, Stereochemistry, Protozoan Proteins, Crystal structure, Crystallography, X-Ray, Tetramer, Structural Biology, Oxidoreductase, Animals, Molecule, Amino Acid Sequence, Leishmania, chemistry.chemical_classification, biology, Active site, General Medicine, biology.organism_classification, Pteridine reductase, Crystallography, Enzyme, chemistry, biology.protein, Oxidoreductases, Sequence Alignment, NADP

Abstract

The protozoan parasites Leishmania utilize a pteridine-reducing enzyme, pteridine reductase (PTR1), to bypass antifolate inhibition. The crystal structure of PTR1 from L. tarentolae has been solved as a binary complex with NADPH at 2.8 A resolution. The structure was solved by molecular-replacement techniques using the recently reported L. major PTR1 structure as a search model. Comparisons of the present structure with the L. major PTR1 allowed us to identify regions of flexibility in the molecule. PTR1 is a member of the growing family of short-chain dehydrogenases (SDR) which share the characteristic Tyr(Xaa)(3)Lys motif in the vicinity of the active site. The functional enzyme is a tetramer and the crystallographic asymmetric unit contains a tetramer with 222 point-group symmetry.

Published

2003

13. Structure-Based Design, Synthesis, and Biological Evaluation of Irreversible Human Rhinovirus 3C Protease Inhibitors. 6. Structure−Activity Studies of Orally Bioavailable, 2-Pyridone-Containing Peptidomimetics

Author

and Rose Ann Ferre, Minerva R. Batugo, Thomas J. Prins, Peter S. Dragovich, Maha B. Kosa, Tove Tuntland, Stephen T. Worland, Fausto Maldonado, Thomas F. Hendrickson, Leora S. Zalman, Lijian Chen, David A. Matthews, Jean-Paul R. Gleeson, Edward L. Brown, Amy K. Patick, Shella A. Fuhrman, James W. Meador, Ru Zhou, Bo Liu, Mark Christopher Guzman, Caroline A. Lee, and Sylvie K. Sakata

Subjects

Models, Molecular, Rhinovirus, Picornain 3C, Pyridones, Stereochemistry, Peptidomimetic, Administration, Oral, Biological Availability, In Vitro Techniques, Crystallography, X-Ray, Ligands, Antiviral Agents, Chemical synthesis, Structure-Activity Relationship, Viral Proteins, Dogs, Drug Stability, Drug Discovery, medicine, Animals, Humans, Moiety, Structure–activity relationship, Protease Inhibitors, chemistry.chemical_classification, biology, Chemistry, Molecular Mimicry, 3C Viral Proteases, Protease inhibitor (biology), Cysteine Endopeptidases, Enzyme, Enzyme inhibitor, Microsomes, Liver, biology.protein, Molecular Medicine, Peptides, Protein Binding, medicine.drug

Abstract

The structure-based design, chemical synthesis, and biological evaluation of various 2-pyridone-containing human rhinovirus (HRV) 3C protease (3CP) inhibitors are described. These compounds are comprised of a peptidomimetic binding determinant and a Michael acceptor moiety, which forms an irreversible covalent adduct with the active site cysteine residue of the 3C enzyme. The 2-pyridone-containing inhibitors typically display improved 3CP inhibition properties relative to related peptide-derived molecules along with more favorable antiviral properties. The cocrystal structure of one pyridone-derived 3CP inhibitor complexed with HRV-2 3CP is also described along with certain ab initio conformation analyses. Optimization of the 2-pyridone-containing compounds is shown to provide several highly active 3CP inhibitors (k(obs)/[I]500,00 M(-1) s(-1)) that function as potent antirhinoviral agents (EC(50) =0.05 microM) against multiple virus serotypes in cell culture. One 2-pyridone-containing 3CP inhibitor is shown to be bioavailable in the dog after oral dosing (F = 48%).

Published

2002

14. Structure-Based Design, Synthesis, and Biological Evaluation of Irreversible Human Rhinovirus 3C Protease Inhibitors. Part 7: Structure–Activity Studies of Bicyclic 2-Pyridone-Containing Peptidomimetics

Author

Ru Zhou, Theodore O. Johnson, Shella A. Fuhrman, David A. Matthews, Stephen T. Worland, Fausto Maldonado, Amy K. Patick, Leora S. Zalman, Thomas J. Prins, Peter S. Dragovich, Rose Ann Ferre, James W. Meador, Edward L. Brown, and Xinjun Hou

Subjects

Rhinovirus, Picornain 3C, Pyridones, medicine.drug_class, Stereochemistry, Peptidomimetic, Clinical Biochemistry, Pharmaceutical Science, Carboxamide, Cysteine Proteinase Inhibitors, Antiviral Agents, Biochemistry, Chemical synthesis, Cell Line, Structure-Activity Relationship, Viral Proteins, stomatognathic system, Drug Discovery, medicine, Humans, Structure–activity relationship, Serotyping, Molecular Biology, chemistry.chemical_classification, biology, Bicyclic molecule, Chemistry, Molecular Mimicry, Organic Chemistry, 3C Viral Proteases, virus diseases, Bridged Bicyclo Compounds, Heterocyclic, Cysteine Endopeptidases, Enzyme, Enzyme inhibitor, Drug Design, biology.protein, Molecular Medicine

Abstract

The structure-based design, chemical synthesis, and biological evaluation of bicyclic 2-pyridone-containing human rhinovirus (HRV) 3C protease (3CP) inhibitors are described. An optimized compound is shown to exhibit antiviral activity when tested against a variety of HRV serotypes (EC(50)'s ranging from 0.037 to 0.162 microM).

Published

2002

15. Design and synthesis of irreversible depsipeptidyl human rhinovirus 3C protease inhibitors

Author

Stephen E. Webber, Joseph T. Marakovits, Peter S. Dragovich, Thomas J. Prins, Ru Zhou, Shella A. Fuhrman, Amy K. Patick, David A. Matthews, Caroline A. Lee, Babu Srinivasan, Terry Moran, Clifford E. Ford, Mary A. Brothers, James E.V. Harr, James W. Meador, Rose Ann Ferre, and Stephen T. Worland

Subjects

Models, Molecular, Rhinovirus, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Microbial Sensitivity Tests, medicine.disease_cause, Antiviral Agents, Biochemistry, Chemical synthesis, Structure-Activity Relationship, Viral Proteins, Drug Discovery, medicine, Peptide bond, Structure–activity relationship, Protease Inhibitors, Protease inhibitor (pharmacology), Molecular Biology, chemistry.chemical_classification, Depsipeptide, Organic Chemistry, 3C Viral Proteases, Biological activity, Cysteine Endopeptidases, Enzyme, chemistry, Molecular Medicine, Peptides

Abstract

Novel tripeptidyl C-terminal Michael acceptors with an ester replacement of the P(2)-P(3) amide bond were investigated as irreversible inhibitors of the human rhinovirus (HRV) 3C protease (3CP). When screened against HRV serotype-14 the best compound was shown to have very good 3CP inhibition (k(obs)/[I]=270,000M(-1)s(-1)) and potent in vitro antiviral activity (EC(50)=7.0nM).

Published

2001

16. Substituted Benzamide Inhibitors of Human Rhinovirus 3C Protease: Structure-Based Design, Synthesis, and Biological Evaluation

Author

Meador J rd, Clifford E. Ford, Edward L. Brown, Chan F, Johnson T, Reich Siegfried Heinz, Kephart Se, Rose Ann Ferre, D. M. Delisle, David A. Matthews, Susan L. Binford, Shella A. Fuhrman, Amy K. Patick, Thomas F. Hendrickson, Stephen T. Worland, and Wallace Michael B

Subjects

Rhinovirus, Protein Conformation, Stereochemistry, 3C Viral Proteases, Cysteine Proteinase Inhibitors, Crystallography, X-Ray, Antiviral Agents, Cocrystal, Cysteine Endopeptidases, Structure-Activity Relationship, Viral Proteins, chemistry.chemical_compound, Protein structure, chemistry, Nucleophile, Covalent bond, Drug Design, Benzamides, Drug Discovery, Michael reaction, Humans, Molecular Medicine, Structure–activity relationship, Benzamide, Cysteine

Abstract

A series of nonpeptide benzamide-containing inhibitors of human rhinovirus (HRV) 3C protease was identified using structure-based design. The design, synthesis, and biological evaluation of these inhibitors are reported. A Michael acceptor was combined with a benzamide core mimicking the P1 recognition element of the natural 3CP substrate. alpha,beta-Unsaturated cinnamate esters irreversibly inhibited the 3CP and displayed antiviral activity (EC(50) 0.60 microM, HRV-16 infected H1-HeLa cells). On the basis of cocrystal structure information, a library of substituted benzamide derivatives was prepared using parallel synthesis on solid support. A 1.9 A cocrystal structure of a benzamide inhibitor in complex with the 3CP revealed a binding mode similar to that initially modeled wherein covalent attachment of the nucleophilic cysteine residue is observed. Unsaturated ketones displayed potent reversible inhibition but were inactive in the cellular antiviral assay and were found to react with nucleophilic thiols such as DTT.

Published

2000

17. Structure-based design of ketone-containing, tripeptidyl human rhinovirus 3C protease inhibitors

Author

Peter S. Dragovich, Ru Zhou, Stephen E. Webber, Thomas J. Prins, Annette K. Kwok, Koji Okano, Shella A. Fuhrman, Leora S. Zalman, Fausto C. Maldonado, Edward L. Brown, James W. Meador, Amy K. Patick, Clifford E. Ford, Mary A. Brothers, Susan L. Binford, David A. Matthews, Rose Ann Ferre, and Stephen T. Worland

Subjects

Ketone, Rhinovirus, Picornain 3C, Stereochemistry, medicine.drug_class, Clinical Biochemistry, Pharmaceutical Science, Carboxamide, Peptide, Cysteine Proteinase Inhibitors, medicine.disease_cause, Antiviral Agents, Biochemistry, Inhibitory Concentration 50, Structure-Activity Relationship, Viral Proteins, Drug Discovery, medicine, Humans, Molecular Biology, Cells, Cultured, chemistry.chemical_classification, biology, Organic Chemistry, 3C Viral Proteases, Ketones, In vitro, Cysteine Endopeptidases, Kinetics, Enzyme, chemistry, Enzyme inhibitor, Drug Design, biology.protein, Molecular Medicine, Oligopeptides

Abstract

Tripeptide-derived molecules incorporating C-terminal ketone electrophiles were evaluated as reversible inhibitors of the cysteine-containing human rhinovirus 3C protease (3CP). An optimized example of such compounds displayed potent 3CP inhibition activity (Ki=0.0045 μM) and in vitro antiviral properties (EC50=0.34 μM) when tested against HRV serotype-14.

Published

2000

18. Structure-Based Design, Synthesis, and Biological Evaluation of Irreversible Human Rhinovirus 3C Protease Inhibitors. 3. Structure−Activity Studies of Ketomethylene-Containing Peptidomimetics

Author

Ru Zhou, Thomas J. Prins, David A. Matthews, Peter S. Dragovich, Stephen T. Worland, James W. Meador, Amy K. Patick, Clifford E. Ford, Rose Ann Ferre, and Shella A. Fuhrman

Subjects

Rhinovirus, Picornain 3C, Stereochemistry, Peptidomimetic, Peptide, Cysteine Proteinase Inhibitors, Antiviral Agents, Chemical synthesis, Cell Line, Structure-Activity Relationship, Viral Proteins, chemistry.chemical_compound, Drug Discovery, Peptide synthesis, Humans, Structure–activity relationship, chemistry.chemical_classification, biology, Molecular Mimicry, 3C Viral Proteases, Dipeptides, Ketones, Cysteine Endopeptidases, Enzyme, chemistry, Enzyme inhibitor, Drug Design, biology.protein, Molecular Medicine

Abstract

The structure-based design, chemical synthesis, and biological evaluation of various ketomethylene-containing human rhinovirus (HRV) 3C protease (3CP) inhibitors are described. These compounds are comprised of a peptidomimetic binding determinant and an ethyl propenoate Michael acceptor moiety which forms an irreversible covalent adduct with the active site cysteine residue of the 3C enzyme. The ketomethylene-containing inhibitors typically display slightly reduced 3CP inhibition activity relative to the corresponding peptide-derived molecules, but they also exhibit significantly improved antiviral properties. Optimization of the ketomethylene-containing compounds is shown to provide several highly active 3C protease inhibitors which function as potent antirhinoviral agents (EC90 =1 microM) against multiple virus serotypes in cell culture.

Published

1999

19. Structure-Based Design, Synthesis, and Biological Evaluation of Irreversible Human Rhinovirus 3C Protease Inhibitors. 2. Peptide Structure−Activity Studies

Author

Babine Robert E, Edward L. Brown, David A. Matthews, Susan L. Binford, Stephen T. Worland, Shella A. Fuhrman, Amy K. Patick, James E. V. Harr, Reich Siegfried Heinz, Joseph T. Marakovits, Thomas J. Prins, Caroline A. Lee, Wallace Michael B, Peter S. Dragovich, Littlefield Ethel S, and Dorothy M. DeLisle, James W. Meador, Rose Ann Ferre, Clifford E. Ford, Ru Zhou, Stephen E. Webber, and Jayashree Tikhe

Subjects

Rhinovirus, Picornain 3C, Stereochemistry, Drug Evaluation, Preclinical, Peptide, Tripeptide, Cysteine Proteinase Inhibitors, Crystallography, X-Ray, Antiviral Agents, Chemical synthesis, Structure-Activity Relationship, Viral Proteins, chemistry.chemical_compound, Drug Discovery, Humans, Structure–activity relationship, Cell Line, Transformed, chemistry.chemical_classification, Binding Sites, Dipeptide, biology, 3C Viral Proteases, Cysteine Endopeptidases, chemistry, Enzyme inhibitor, Drug Design, biology.protein, Molecular Medicine, Oligopeptides

Abstract

The structure-based design, chemical synthesis, and biological evaluation of various peptide-derived human rhinovirus (HRV) 3C protease (3CP) inhibitors are described. These compounds are comprised of an ethyl propenoate Michael acceptor moiety and a tripeptidyl binding determinant. The systematic modification of each amino acid residue present in the binding determinant as well as the N-terminal functionality is described. Such modifications are shown to provide irreversible HRV-14 3CP inhibitors with anti-3CP activities (kobs/[I]) ranging from 60 to 280 000 M-1 s-1 and antiviral EC50's which approach 0.15 microM. An optimized inhibitor which incorporates several improvements identified by the structure-activity studies is also described. This molecule displays very rapid irreversible inhibition of HRV-14 3CP (kobs/[I] = 800 000 M-1 s-1) and potent antiviral activity against HRV-14 in cell culture (EC50 = 0.056 microM). A 1.9 A crystal structure of an S-alkylthiocarbamate-containing inhibitor complexed with HRV-2 3CP is also detailed.

Published

1998

20. Tripeptide Aldehyde Inhibitors of Human Rhinovirus 3C Protease: Design, Synthesis, Biological Evaluation, and Cocrystal Structure Solution of P1 Glutamine Isosteric Replacements

Author

J W Meador rd, K. Okano, Rose Ann Ferre, Edward L. Brown, Y Xin, Stephanie Webber, Susan L. Binford, Stephen T. Worland, Shella A. Fuhrman, R. A. Love, David A. Matthews, Clifford E. Ford, Amy K. Patick, Thomas F. Hendrickson, T L Little, and Reich Siegfried Heinz

Subjects

Models, Molecular, Rhinovirus, Molecular model, Picornain 3C, Protein Conformation, medicine.drug_class, Stereochemistry, Isostere, Glutamine, Molecular Conformation, Carboxamide, Tripeptide, Cysteine Proteinase Inhibitors, Crystallography, X-Ray, Antiviral Agents, Cocrystal, Viral Proteins, chemistry.chemical_compound, Amide, Drug Discovery, Peptide synthesis, medicine, Humans, Cell Line, Transformed, Binding Sites, Chemistry, 3C Viral Proteases, Cysteine Endopeptidases, Drug Design, Molecular Medicine, Oligopeptides, HeLa Cells

Abstract

The investigation of tripeptide aldehydes as reversible covalent inhibitors of human rhinovirus (HRV) 3C protease (3CP) is reported. Molecular models based on the apo crystal structure of HRV-14 3CP and other trypsin-like serine proteases were constructed to approximate the binding of peptide substrates, generate transition state models of P1-P1' amide cleavage, and propose novel tripeptide aldehydes. Glutaminal derivatives have limitations since they exist predominantly in the cyclic hemiaminal form. Therefore, several isosteric replacements for the P1 carboxamide side chain were designed and incorporated into the tripeptide aldehydes. These compounds were found to be potent inhibitors of purified HRV-14 3CP with Kis ranging from 0.005 to 0.64 microM. Several have low micromolar antiviral activity when tested against HRV-14-infected H1-HeLa cells. The N-acetyl derivative 3 was also shown to be active against HRV serotypes 2, 16, and 89. High-resolution cocrystal structures of HRV-2 3CP, covalently bound to compounds 3, 15, and 16, were solved. These cocrystal structures were analyzed and compared with our original HRV-14 3CP-substrate and inhibitor models.

Published

1998

21. Design, Synthesis, and Evaluation of Nonpeptidic Inhibitors of Human Rhinovirus 3C Protease

Author

Edward L. Brown, Susan L. Binford, Amy K. Patick, Shella A. Fuhrman, Rose Ann Ferre, D. M. Delisle, R. A. Love, Jayashree Tikhe, Stephen E. Webber, James W. Meador, Thomas F. Hendrickson, David A. Matthews, Stephen T. Worland, and Clifford E. Ford

Subjects

Magnetic Resonance Spectroscopy, Molecular model, Picornain 3C, medicine.drug_class, Stereochemistry, Carboxamide, Antiviral Agents, Chemical synthesis, Mass Spectrometry, Viral Proteins, chemistry.chemical_compound, Drug Discovery, medicine, Humans, Protease Inhibitors, Chymotrypsin, Molecular Structure, biology, Isatin, 3C Viral Proteases, Proteolytic enzymes, Active site, Cysteine Endopeptidases, chemistry, biology.protein, Thermodynamics, Molecular Medicine, HeLa Cells

Abstract

The design, synthesis, and biological evaluation of reversible, nonpeptidic inhibitors of human rhinovirus (HRV) 3C protease (3CP) are reported. A novel series of 2,3-dioxindoles (isatins) were designed that utilized a combination of protein structure-based drug design, molecular modeling, and structure-activity relationship (SAR). The C-2 carbonyl of isatin was envisioned to react in the active site of HRV 3CP with the cysteine responsible for catalytic proteolysis, thus forming a stabilized transition state mimic. Molecular-modeling experiments using the apo crystal structure of human rhinovirus-serotype 14 (HRV-14) 3CP and a peptide substrate model allowed us to design recognition features into the P1 and P2 subsites, respectively, from the 5- and 1-positions of isatin. Attempts to optimize recognition properties in the P1 subsite using SAR at the 5-position were performed. In addition, a series of ab initio calculations were carried out on several 5-substituted isatins to investigate the stability of sulfide adducts at C-3. The inhibitors were prepared by general synthetic methods, starting with commercially available 5-substituted isatins in nearly every case. All compounds were tested for inhibition of purified HRV-14 3CP. Compounds 8, 14, and 19 were found to have excellent selectivity for HRV-14 3CP compared to other proteolytic enzymes, including chymotrypsin and cathepsin B. Selected compounds were assayed for antiviral activity against HRV-14-infected HI-HeLa cells. A 2.8 A cocrystal structure of derivative 19 covalently bound to human rhinovirus-serotype 2 (HRV-2) 3CP was solved and revealed that the isatin was situated in essentially the same conformation as modeled.

Published

1996

22. Novel isoquinolone PDK1 inhibitors discovered through fragment-based lead discovery

Author

Ping Chen, Laura Lingardo, Rose Ann Ferre, John Charles Kath, Qiyue Hu, M. Catherine Johnson, Jiangli Yan, Jacques Ermolieff, Samantha Elizabeth Greasley, and Gordon Alton

Subjects

Protein-Serine-Threonine Kinases, Ligand efficiency, Binding Sites, Drug discovery, Kinase, Stereochemistry, Fragment-based lead discovery, Drug Evaluation, Preclinical, Pyruvate Dehydrogenase Acetyl-Transferring Kinase, Hydrogen Bonding, Plasma protein binding, Biology, Protein Serine-Threonine Kinases, Crystallography, X-Ray, Ligands, Magnetic Resonance Imaging, Peptide Fragments, Computer Science Applications, High-Throughput Screening Assays, Drug Discovery, Humans, Physical and Theoretical Chemistry, PI3K/AKT/mTOR pathway, Protein Binding

Abstract

Phosphoinositide-dependent kinase-1 (PDK1) is a critical enzyme in the PI3K/AKT pathway and to the activation of AGC family protein kinases, including S6K, SGK, and PKC. Dysregulation of this pathway plays a key role in cancer cell growth, survival and tumor angiogenesis. As such, inhibitors of PDK1 offer the promise of a new therapeutic modality for cancer treatment. Fragment based drug screening has recently become a viable entry point for hit identification. In this work, NMR spectroscopy fragment screening of PDK1 afforded novel chemotypes as orthogonal starting points from HTS screening hits. Compounds identified as hits by NMR spectroscopy were tested in a biochemical assay, and fragments with activity in both assays were clustered. The Pfizer compound file was mined via substructure and 2D similarity search, and the chemotypes were prioritized by ligand efficiency (LE), SAR mining, chemical attractiveness, and chemical enablement of promising vectors. From this effort, an isoquinolone fragment hit, 5 (IC(50) 870 μM, LE = 0.39), was identified as a novel, ligand efficient inhibitor of PDK1 and a suitable scaffold for further optimization. Initially in the absence of crystallographic data, a fragment growing approach efficiently explored four vectors of the isoquinolone scaffold via parallel synthesis to afford a compound with crystallographic data, 16 (IC(50) 41.4 μM, LE = 0.33). Subsequent lead optimization efforts provided 24 (IC(50) 1.8 μM, LE = 0.42), with greater than fivefold selectivity against other key pathway kinases.

Published

2011

23. ChemInform Abstract: Design, Synthesis, and Evaluation of Nonpeptidic Inhibitors of Human Rhinovirus 3C Protease

Author

R. A. Love, Stephen T. Worland, D. M. Delisle, Jayashree Tikhe, Edward L. Brown, Susan L. Binford, Thomas F. Hendrickson, Rose Ann Ferre, Shella A. Fuhrman, David A. Matthews, James W. Meador, Clifford E. Ford, Amy K. Patick, and Stephen E. Webber

Subjects

Chymotrypsin, medicine.diagnostic_test, biology, Molecular model, Stereochemistry, Isatin, Proteolysis, Proteolytic enzymes, Active site, General Medicine, chemistry.chemical_compound, Protein structure, chemistry, medicine, biology.protein, Cysteine

Abstract

The design, synthesis, and biological evaluation of reversible, nonpeptidic inhibitors of human rhinovirus (HRV) 3C protease (3CP) are reported. A novel series of 2,3-dioxindoles (isatins) were designed that utilized a combination of protein structure-based drug design, molecular modeling, and structure-activity relationship (SAR). The C-2 carbonyl of isatin was envisioned to react in the active site of HRV 3CP with the cysteine responsible for catalytic proteolysis, thus forming a stabilized transition state mimic. Molecular-modeling experiments using the apo crystal structure of human rhinovirus-serotype 14 (HRV-14) 3CP and a peptide substrate model allowed us to design recognition features into the P1 and P2 subsites, respectively, from the 5- and 1-positions of isatin. Attempts to optimize recognition properties in the P1 subsite using SAR at the 5-position were performed. In addition, a series of ab initio calculations were carried out on several 5-substituted isatins to investigate the stability of sulfide adducts at C-3. The inhibitors were prepared by general synthetic methods, starting with commercially available 5-substituted isatins in nearly every case. All compounds were tested for inhibition of purified HRV-14 3CP. Compounds 8, 14, and 19 were found to have excellent selectivity for HRV-14 3CP compared to other proteolytic enzymes, including chymotrypsin and cathepsin B. Selected compounds were assayed for antiviral activity against HRV-14-infected HI-HeLa cells. A 2.8 A cocrystal structure of derivative 19 covalently bound to human rhinovirus-serotype 2 (HRV-2) 3CP was solved and revealed that the isatin was situated in essentially the same conformation as modeled.

Published

2010

24. The crystal structure of the RNA-dependent RNA polymerase from human rhinovirus: a dual function target for common cold antiviral therapy

Author

Robert A, Love, Karen A, Maegley, Xiu, Yu, Rose Ann, Ferre, Laura K, Lingardo, Wade, Diehl, Hans E, Parge, Peter S, Dragovich, and Shella A, Fuhrman

Subjects

Models, Molecular, Protein Folding, Rhinovirus, Sequence Homology, Amino Acid, Molecular Sequence Data, Humans, Amino Acid Sequence, Cloning, Molecular, Crystallography, X-Ray, RNA-Dependent RNA Polymerase

Abstract

Human rhinoviruses (HRV), the predominant members of the Picornaviridae family of positive-strand RNA viruses, are the major causative agents of the common cold. Given the lack of effective treatments for rhinoviral infections, virally encoded proteins have become attractive therapeutic targets. The HRV genome encodes an RNA-dependent RNA polymerase (RdRp) denoted 3Dpol, which is responsible for replicating the viral genome and for synthesizing a protein primer used in the replication. Here the crystal structures for three viral serotypes (1B, 14, and 16) of HRV 3Dpol have been determined. The three structures are very similar to one another, and to the closely related poliovirus (PV) 3Dpol enzyme. Because the reported PV crystal structure shows significant disorder, HRV 3Dpol provides the first complete view of a picornaviral RdRp. The folding topology of HRV 3Dpol also resembles that of RdRps from hepatitis C virus (HCV) and rabbit hemorrhagic disease virus (RHDV) despite very low sequence homology.

Published

2004

25. Structure-based design, synthesis, and biological evaluation of irreversible human rhinovirus 3C protease inhibitors. 8. Pharmacological optimization of orally bioavailable 2-pyridone-containing peptidomimetics

Author

Hiep T. Luu, Zhen Ping Wu, Theodore O. Johnson, Jia Liu, Bennett Chaplin Borer, Tove Tuntland, Junhua Tao, Caroline A. Lee, Fausto Maldonado, Amy K. Patick, Sylvie K. Sakata, Thomas J. Prins, Naresh K. Nayyar, Rose Ann Ferre, Michael Mohajeri, Peter W. Rose, Maha B. Kosa, David A. Matthews, Kevin Scott Mcgee, Leora S. Zalman, Steven Lee, Peter S. Dragovich, Ellen Y. Wu, Bo Liu, Shella A. Fuhrman, Ye Hua, Elena Z. Dovalsantos, Paul A. Rejto, Ru Zhou, Mark Christopher Guzman, Ming Guo, Edward L. Brown, Minerva R. Batugo, James W. Meador, Lijian Chen, Andreas Liese, Moran Terence Jarold, and Jean-Paul R. Gleeson

Subjects

Male, Magnetic Resonance Spectroscopy, Picornain 3C, Rhinovirus, Peptidomimetic, Stereochemistry, Pyridones, Biological Availability, In Vitro Techniques, Chemical synthesis, Antiviral Agents, Structure-Activity Relationship, Viral Proteins, Dogs, Oral administration, Drug Discovery, Animals, Humans, Protease Inhibitors, chemistry.chemical_classification, biology, 3C Viral Proteases, Biological activity, Blood Proteins, Blood proteins, Cysteine Endopeptidases, Macaca fascicularis, Enzyme, chemistry, Solubility, Enzyme inhibitor, Drug Design, biology.protein, Hepatocytes, Microsomes, Liver, Molecular Medicine, Indicators and Reagents, Caco-2 Cells, Half-Life, Protein Binding

Abstract

The optimization of the pharmacokinetic performance of various 2-pyridone-containing human rhinovirus (HRV) 3C protease (3CP) inhibitors following oral administration to either beagle dogs or CM-monkeys is described. The molecules described in this work are composed of a 2-pyridone-containing peptidomimetic binding determinant and an alpha,beta-unsaturated ester Michael acceptor moiety which forms an irreversible covalent adduct with the active site cysteine residue of the 3C enzyme. Modification of the ester contained within these compounds is detailed along with alteration of the P(2) substituent present in the peptidomimetic portion of the inhibitors. The pharmacokinetics of several inhibitors in both dogs and monkeys are described (7 h plasma concentrations after oral administration) along with their human plasma stabilities, stabilities in incubations with human, dog, and monkey microsomes and hepatocytes, Caco-2 permeabilities, and aqueous solubilities. Compounds containing an alpha,beta-unsaturated ethyl ester fragment and either an ethyl or propargyl P(2) moiety displayed the most promising combination of 3C enzyme inhibition (k(obs)/[I] 170 000-223 000 M(-1) s(-1)), antiviral activity (EC(50) = 0.047-0.058 microM, mean vs seven HRV serotypes), and pharmacokinetics following oral administration (7 h dog plasma levels = 0.248-0.682 microM; 7 h CM-monkey plasma levels = 0.057-0.896 microM).

Published

2003

26. Structure-based design of a parallel synthetic array directed toward the discovery of irreversible inhibitors of human rhinovirus 3C protease

Author

Hiep T. Luu, Rose Ann Ferre, Fausto Maldonado, Peter S. Dragovich, Amy K. Patick, Skalitzky Donald James, Shella A. Fuhrman, Ye Hua, David A. Matthews, Shao Song Chu, Fora Chan, Edward L. Brown, Leora S. Zalman, Theodore O. Johnson, Eastman Brian Walter, Siegfried Reich, Michelle Yang, Stephen T. Worland, James W. Meador, and Thomas F. Hendrickson

Subjects

Picornain 3C, Rhinovirus, Stereochemistry, medicine.drug_class, Carboxamide, medicine.disease_cause, Crystallography, X-Ray, Chemical synthesis, Antiviral Agents, Structure-Activity Relationship, Viral Proteins, stomatognathic system, Drug Discovery, medicine, Structure–activity relationship, Combinatorial Chemistry Techniques, Humans, Enzyme Inhibitors, Cytotoxicity, chemistry.chemical_classification, 3C Viral Proteases, virus diseases, In vitro, Cysteine Endopeptidases, Enzyme, Biochemistry, chemistry, Molecular Medicine, HeLa Cells, Protein Binding

Abstract

Utilizing the tools of parallel synthesis and structure-based design, a new class of Michael acceptor-containing, irreversible inhibitors of human rhinovirus 3C protease (HRV 3CP) was discovered. These inhibitors are shown to inhibit HRV-14 3CP with rates of inactivation ranging from 886 to 31 400 M(-1) sec(-1). These inhibitors exhibit antiviral activity when tested against HRV-14 infected H1-HeLa cells, with EC(50) values ranging from 1.94 to 0.15 microM. No cytotoxicity was observed at the limits of the assay concentration. A crystal structure of one of the more potent inhibitors covalently bound to HRV-2 3CP is detailed. These compounds were also tested against HRV serotypes other than type 14 and were found to have highly variable activities.

Published

2002

27. Structure-based design, synthesis, and biological evaluation of irreversible human rhinovirus 3C protease inhibitors. 4. Incorporation of P1 lactam moieties as L-glutamine replacements

Author

Ru Zhou, Stephen E. Webber, Thomas J. Prins, Joseph T. Marakovits, Rose Ann Ferre, Edward L. Brown, Caroline A. Lee, James E. V. Harr, Peter S. Dragovich, Tove Tuntland, Benjamin J. Burke, Amy K. Patick, Clifford E. Ford, Shella A. Fuhrman, Paul A. Rejto, Thomas F. Hendrickson, Maha Kosa, Stephen T. Worland, James W. Meador, and David A. Matthews

Subjects

Models, Molecular, Proteases, Picornain 3C, Lactams, Rhinovirus, Peptidomimetic, Stereochemistry, Glutamine, Phenylalanine, Drug Evaluation, Preclinical, Cysteine Proteinase Inhibitors, Crystallography, X-Ray, Chemical synthesis, Antiviral Agents, Cell Line, chemistry.chemical_compound, Structure-Activity Relationship, Viral Proteins, Drug Discovery, Structure–activity relationship, Humans, biology, Molecular Mimicry, 3C Viral Proteases, Valine, Isoxazoles, Pyrrolidinones, Cysteine Endopeptidases, chemistry, Enzyme inhibitor, Drug Design, Lactam, biology.protein, Molecular Medicine, Oligopeptides, Cysteine

Abstract

The structure-based design, chemical synthesis, and biological evaluation of various human rhinovirus (HRV) 3C protease (3CP) inhibitors which incorporate P1 lactam moieties in lieu of an L-glutamine residue are described. These compounds are comprised of a tripeptidyl or peptidomimetic binding determinant and an ethyl propenoate Michael acceptor moiety which forms an irreversible covalent adduct with the active site cysteine residue of the 3C enzyme. The P1-lactam-containing inhibitors display significantly increased 3CP inhibition activity along with improved antirhinoviral properties relative to corresponding L-glutamine-derived molecules. In addition, several lactam-containing compounds exhibit excellent selectivity for HRV 3CP over several other serine and cysteine proteases and are not appreciably degraded by a variety of biological agents. One of the most potent inhibitors (AG7088, mean antirhinoviral EC90 approximately 0.10 microM, n = 46 serotypes) is shown to warrant additional preclinical development to explore its potential for use as an antirhinoviral agent.

Published

1999

28. Structure-based design, synthesis, and biological evaluation of irreversible human rhinovirus 3C protease inhibitors. 1. Michael acceptor structure-activity studies

Author

Peter S. Dragovich, Stephen E. Webber, Robert E. Babine, Shella A. Fuhrman, Amy K. Patick, David A. Matthews, Caroline A. Lee, Siegfried H. Reich, Thomas J. Prins, Joseph T. Marakovits, Ethel S. Littlefield, Ru Zhou, Jayashree Tikhe, Clifford E. Ford, Michael B. Wallace, James W. Meador, Rose Ann Ferre, Edward L. Brown, Susan L. Binford, James E. V. Harr, Dorothy M. DeLisle, and Stephen T. Worland

Subjects

Binding Sites, Rhinovirus, Protein Conformation, 3C Viral Proteases, Cysteine Proteinase Inhibitors, Crystallography, X-Ray, Antiviral Agents, Rats, Rats, Sprague-Dawley, Cysteine Endopeptidases, Structure-Activity Relationship, Viral Proteins, Drug Stability, Drug Design, Drug Discovery, Molecular Medicine, Animals, Humans, Oligopeptides, Cell Line, Transformed, HeLa Cells

Abstract

The structure-based design, chemical synthesis, and biological evaluation of peptide-derived human rhinovirus (HRV) 3C protease (3CP) inhibitors are described. These compounds incorporate various Michael acceptor moieties and are shown to irreversibly bind to HRV serotype 14 3CP with inhibition activities (kobs/[I]) ranging from 100 to 600 000 M-1 s-1. These inhibitors are also shown to exhibit antiviral activity when tested against HRV-14-infected H1-HeLa cells with EC50's approaching 0.50 microM. Extensive structure-activity relationships developed by Michael acceptor alteration are reported along with the evaluation of several compounds against HRV serotypes other than 14. A 2.0 A crystal structure of a peptide-derived inhibitor complexed with HRV-2 3CP is also detailed.

Published

1998

29. Structure of human rhinovirus 3C protease reveals a trypsin-like polypeptide fold, RNA-binding site, and means for cleaving precursor polyprotein

Author

Brad Condon, H.E. McElroy, C.L. Gribskov, Gregg Budahazi, Stephen T. Worland, David A. Matthews, Ward W. Smith, Wes Slsson, Jesus Ernesto Villafranca, Rose Ann Ferre, and Cheryl Ann Janson

Subjects

Models, Molecular, Proteases, Protein Folding, Picornain 3C, Rhinovirus, Molecular Sequence Data, Beta sheet, General Biochemistry, Genetics and Molecular Biology, Substrate Specificity, Viral Proteins, medicine, Animals, Humans, Trypsin, Amino Acid Sequence, Binding Sites, biology, Molecular Structure, Sequence Homology, Amino Acid, 3C Viral Proteases, Active site, RNA, Cysteine protease, Cysteine Endopeptidases, Biochemistry, biology.protein, Cattle, Oxyanion hole, medicine.drug

Abstract

The structure of human rhinovirus-14 3C protease (3Cpro) has been determined at 2.3 A resolution and refined to an R factor of 0.22. This cysteine protease folds into two topologically equivalent six-stranded beta barrels and in this sense is similar to trypsin-like serine proteases. However, there are differences in the lengths and positioning of individual beta strands as well as in loops connecting elements of secondary structure. The catalytic residues Cys-146, His-40, and Glu-71 are positioned as in serine proteases, but the oxyanion hole is moved 1-1.2 A away. Residues that bind to the 5' noncoding region of rhinovirus genomic RNA are located on the opposite side of the molecule from the active site. Interactions between individual 3Cpro molecules in the crystal lattice suggest a model for intermolecular proteolytic cleavage of the 3CD polyprotein.

Published

1994

30. 2.3 A crystal structure of the catalytic domain of DNA polymerase beta

Author

Jay F. Davies, Zuzana Hostomska, Rose Ann Ferre, Zdenek Hostomsky, and Robert Almassy

Subjects

Models, Molecular, DNA polymerase, Stereochemistry, Molecular Sequence Data, DNA polymerase beta, Crystallography, X-Ray, General Biochemistry, Genetics and Molecular Biology, Catalysis, Protein Structure, Secondary, chemistry.chemical_compound, Aspartic acid, Moiety, Animals, Thymine Nucleotides, Amino Acid Sequence, Peptide sequence, Polymerase, Manganese, biology, DNA Polymerase I, Peptide Fragments, Protein Structure, Tertiary, Rats, chemistry, Biochemistry, biology.protein, Beta protein, DNA polymerase I, Protein Binding

Abstract

The crystal structure of the catalytic domain of rat DNA polymerase beta (pol beta) has been determined at 2.3 A resolution and refined to an R factor of 0.22. The mixed alpha/beta protein has three subdomains arranged in an overall U shape reminiscent of other polymerase structures. The folding topology of pol beta, however, is unique. Two divalent metals bind near three aspartic acid residues implicated in the catalytic activity. In the presence of Mn2+ and dTTP, interpretable electron density is seen for two metals and the triphosphate, but not the deoxythymidine moiety. The principal interaction of the triphosphate moiety is with the bound divalent metals.

Published

1994

31. Corrigendum to 'Thioether benzenesulfonamide inhibitors of carbonic anhydrases II and IV: Structure-based drug design, synthesis, and biological evaluation' [Bioorg. Med. Chem. 18 (2010) 3307]

Author

Samantha Elizabeth Greasley, Eric L. Reyner, D.A. Rewolinski, Thomas A. Pauly, Wesley K. M. Chong, Martha A. Ornelas, Seiji Nukui, Dac M. Dinh, James W. Meador, Robert L. Paz, Rose Ann Ferre, Morena N. Shaw, and William F. Vernier

Subjects

Drug, Stereochemistry, media_common.quotation_subject, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, chemistry.chemical_compound, Design synthesis, Thioether, chemistry, Drug Discovery, Molecular Medicine, Structure based, Molecular Biology, Biological evaluation, media_common

Published

2010