Search

Your search keyword '"Todd W. Rockway"' showing total 40 results
Start Over Author "Todd W. Rockway"
40 results on '"Todd W. Rockway"'

1. Synthesis and Biological Characterization of Aryl Uracil Inhibitors of Hepatitis C Virus NS5B Polymerase: Discovery of ABT-072, a trans-Stilbene Analog with Good Oral Bioavailability

Author

Emily O. Dumas, Kent D. Stewart, Michael D. Tufano, Jill Beyer, Neeta S. Panchal, Dachun Liu, Warren M. Kati, Lisa E. Hernandez, Todd W. Rockway, John K. Pratt, John T. Randolph, Clarence J. Maring, David W A Beno, G. Koev, Donner Pamela L, Yaya Liu, Motter Christopher E, Kenton L. Longenecker, Lynn Colletti, Rolf Wagner, Rubina Mondal, A. Chris Krueger, Hock B. Lim, and Akhteruzzaman Molla

Subjects
0301 basic medicine, Hepatitis C virus, Hepacivirus, 030106 microbiology, Administration, Oral, Biological Availability, Chemistry Techniques, Synthetic, Viral Nonstructural Proteins, Pharmacology, medicine.disease_cause, Permeability, Cytosine, 03 medical and health sciences, chemistry.chemical_compound, Pharmacokinetics, Stilbenes, Drug Discovery, medicine, Humans, Potency, Tissue Distribution, Dosing, Enzyme Inhibitors, Sulfonamides, biology, Chemistry, Dihydrouracil, Stereoisomerism, Uracil, biology.organism_classification, Bioavailability, 030104 developmental biology, Molecular Medicine
Abstract

ABT-072 is a non-nucleoside HCV NS5B polymerase inhibitor that was discovered as part of a program to identify new direct-acting antivirals (DAAs) for the treatment of HCV infection. This compound was identified during a medicinal chemistry effort to improve on an original lead, inhibitor 1, which we described in a previous publication. Replacement of the amide linkage in 1 with a trans-olefin resulted in improved compound permeability and solubility and provided much better pharmacokinetic properties in preclinical species. Replacement of the dihydrouracil in 1 with an N-linked uracil provided better potency in the genotype 1 replicon assay. Results from phase 1 clinical studies supported once-daily oral dosing with ABT-072 in HCV infected patients. A phase 2 clinical study that combined ABT-072 with the HCV protease inhibitor ABT-450 provided a sustained virologic response at 24 weeks after dosing (SVR24) in 10 of 11 patients who received treatment.

Published
2018
Full Text
View/download PDF

2. Discovery of fluorobenzimidazole HCV NS5A inhibitors

Author

Nelson Lissa T, Tatyana Dekhtyar, DeAnne Stolarik, Thomas Reisch, Warren M. Kati, Donner Pamela L, Tami Pilot-Matias, Sachin V. Patel, Rolf Wagner, Preethi Krishnan, Douglas K. Hutchinson, Todd W. Rockway, Neeta Mistry, David W A Beno, Rubina Mondal, Clarence J. Maring, John T. Randolph, and Charles A. Flentge

Subjects
0301 basic medicine, Benzimidazole, Genotype, Halogenation, viruses, Hepacivirus, 030106 microbiology, Clinical Biochemistry, HCV genotypes, Pharmaceutical Science, Viral Nonstructural Proteins, Antiviral Agents, 01 natural sciences, Biochemistry, Mice, 03 medical and health sciences, chemistry.chemical_compound, Dogs, Drug Discovery, Animals, Humans, HCV NS5A Inhibitor, Replicon, NS5A, Molecular Biology, biology, 010405 organic chemistry, Organic Chemistry, virus diseases, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Hepatitis C, Virology, digestive system diseases, In vitro, Orders of magnitude (mass), Rats, 0104 chemical sciences, chemistry, Molecular Medicine, Benzimidazoles
Abstract

Research toward a next-generation HCV NS5A inhibitor has identified fluorobenzimidazole analogs that demonstrate potent, broad-genotype in vitro activity against HCV genotypes 1-6 replicons as well as HCV NS5A variants that are orders of magnitude less susceptible to inhibition by first-generation NS5A inhibitors in comparison to wild-type replicons. The fluorobenzimidazole inhibitors have improved pharmacokinetic properties in comparison to non-fluorinated benzimidazole analogs. Discovery of these inhibitors was facilitated by exploring SAR in a structurally simplified inhibitor series.

Published
2016
Full Text
View/download PDF

3. Highlights of the Structure-Activity Relationships of Benzimidazole Linked Pyrrolidines Leading to the Discovery of the Hepatitis C Virus NS5A Inhibitor Pibrentasvir (ABT-530)

Author

Ryan G. Keddy, Warren M. Kati, Tami Pilot-Matias, Nelson Lissa T, DeAnne Stolarik, Tatyana Dekhtyar, Rubina Mondal, Thomas Reisch, A. Chris Krueger, Hutchinson Douglas K, Donner Pamela L, John T. Randolph, Wenqing Gao, David A. Betebenner, Clarence J. Maring, Preethi Krishnan, Neeta S. Panchal, Christine A. Collins, Todd W. Rockway, Yi Gao, Teresa I. Ng, David W A Beno, John K. Pratt, Dachun Liu, Sachin V. Patel, Charles A. Flentge, Mark A. Matulenko, and Rolf Wagner

Subjects
Pyrrolidines, Genotype, viruses, Hepatitis C virus, Hepacivirus, medicine.disease_cause, Virus Replication, Antiviral Agents, Virus, 03 medical and health sciences, chemistry.chemical_compound, Mice, Structure-Activity Relationship, 0302 clinical medicine, Interferon, Drug Discovery, medicine, Animals, Tissue Distribution, NS5A, biology, Chemistry, Ribavirin, virus diseases, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Virology, digestive system diseases, Ombitasvir, Pibrentasvir, 030220 oncology & carcinogenesis, Drug Design, Molecular Medicine, 030211 gastroenterology & hepatology, Benzimidazoles, medicine.drug
Abstract

Curative interferon and ribavirin sparing treatments for hepatitis C virus (HCV)-infected patients require a combination of mechanistically orthogonal direct acting antivirals. A shared component of these treatments is usually an HCV NS5A inhibitor. First generation FDA approved treatments, including the component NS5A inhibitors, do not exhibit equivalent efficacy against HCV virus genotypes 1-6. In particular, these first generation NS5A inhibitors tend to select for viral drug resistance. Ombitasvir is a first generation HCV NS5A inhibitor included as a key component of Viekira Pak for the treatment of patients with HCV genotype 1 infection. Since the launch of next generation HCV treatments, functional cure for genotype 1-6 HCV infections has been achieved, as well as shortened treatment duration across a wider spectrum of genotypes. In this paper, we show how we have modified the anchor, linker, and end-cap architecture of our NS5A inhibitor design template to discover a next generation NS5A inhibitor pibrentasvir (ABT-530), which exhibits potent inhibition of the replication of wild-type genotype 1-6 HCV replicons, as well as improved activity against replicon variants demonstrating resistance against first generation NS5A inhibitors.

Published
2018

4. Aryl uracil inhibitors of hepatitis C virus NS5B polymerase: Synthesis and characterization of analogs with a fused 5,6-bicyclic ring motif

Author

Kenton L. Longenecker, G. Koev, A. Chris Krueger, Jill Beyer, Dachun Liu, John T. Randolph, Kent D. Stewart, Rolf Wagner, Warren M. Kati, Donner Pamela L, David W A Beno, Hutchinson Douglas K, Rubina Mondal, Yaya Liu, Todd W. Rockway, Hock B. Lim, Akhteruzzaman Molla, Clarence J. Maring, Charles A. Flentge, Christopher E. Motter, and David A. Degoey

Subjects
Stereochemistry, Hepatitis C virus, Clinical Biochemistry, Pharmaceutical Science, Hepacivirus, Viral Nonstructural Proteins, medicine.disease_cause, Biochemistry, Ns5b polymerase, Bridged Bicyclo Compounds, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, medicine, Animals, Enzyme Inhibitors, Uracil, Molecular Biology, NS5B, Bicyclic molecule, Aryl, Organic Chemistry, RNA-Dependent RNA Polymerase, Rats, chemistry, Replicon cell, Molecular Medicine
Abstract

The synthesis and structure–activity relationships of a novel aryl uracil series which contains a fused 5,6-bicyclic ring unit for HCV NS5B inhibition is described. Several analogs display replicon cell culture potencies in the low nanomolar range along with excellent rat pharmacokinetic values.

Published
2013
Full Text
View/download PDF

5. Mechanistic Study of HCV Polymerase Inhibitors at Individual Steps of the Polymerization Reaction

Author

Ron Pithawalla, Wen W. Jiang, Todd W. Rockway, Sudthida Vasavanonda, Warren M. Kati, Kevin Harris, John Pratt, Yaya Liu, and Rakesh Tripathi

Subjects
Electrophoresis, Time Factors, Polymers, Hepatitis C virus, Allosteric regulation, Viral Nonstructural Proteins, Benzothiadiazines, medicine.disease_cause, Biochemistry, Protein Structure, Secondary, Substrate Specificity, medicine, Humans, Polymerase, chemistry.chemical_classification, biology, Heparin, Active site, RNA, Templates, Genetic, Small molecule, Kinetics, Enzyme, chemistry, Catalytic cycle, biology.protein, RNA, Viral, Benzimidazoles, Protein Binding
Abstract

Little is known about the mechanism of HCV polymerase-catalyzed nucleotide incorporation and the individual steps employed by this enzyme during a catalytic cycle. In this paper, we applied various biochemical tools and examined the mechanism of polymerase catalysis. We found that formation of a productive RNA-enzyme complex is the slowest step followed by RNA dissociation and initiation of primer strand synthesis. Various groups have reported several classes of small molecule inhibitors of hepatitis C virus NS5B polymerase; however, the mechanism of inhibition for many of these inhibitors is not clear. We undertook a series of detailed mechanistic studies to characterize the mechanisms of inhibition for these HCV polymerase inhibitors. We found that the diketoacid derivatives competitively bind to the elongation NTP pocket in the active site and inhibit both the initiation and elongation steps of polymerization. While both benzimidazoles and benzothiadiazines are noncompetitive with respect to the active site elongation NTP pocket, benzothiadiazine compounds competitively bind to the initiation pocket in the active site and inhibit only the initiation step of de novo RNA polymerization. The benzimidazoles bind to the thumb allosteric pocket and inhibit the conformational changes during RNA synthesis. We also observed a cross interaction between the thumb allosteric pocket and the initiation pocket using inhibitor-inhibitor cross competition studies. This information will be very important in designing combination therapies using two small molecule drugs to treat hepatitis C virus.

Published
2006
Full Text
View/download PDF

6. Mutations Conferring Resistance to a Hepatitis C Virus (HCV) RNA-Dependent RNA Polymerase Inhibitor Alone or in Combination with an HCV Serine Protease Inhibitor In Vitro

Author

Vincent S. Stoll, Clarence J. Maring, Teresa Ng, Tatyana Dekhtyar, Todd W. Rockway, Sherie Masse, Pam Donner, Gennadiy Koev, Liangjun Lu, Akhteruzzaman Molla, Tami Pilot-Matias, Rubina Mondal, Kent D. Stewart, John K. Pratt, Hongmei Mo, and Ron Pithawalla

Subjects
Models, Molecular, Serine Proteinase Inhibitors, viruses, Hepatitis C virus, RNA-dependent RNA polymerase, Hepacivirus, Biology, medicine.disease_cause, Antiviral Agents, Cell Line, chemistry.chemical_compound, RNA polymerase, Drug Resistance, Viral, medicine, Pharmacology (medical), Protease inhibitor (pharmacology), Replicon, Enzyme Inhibitors, Pharmacology, NS3, Binding Sites, Molecular Structure, virus diseases, biochemical phenomena, metabolism, and nutrition, RNA-Dependent RNA Polymerase, Virology, Molecular biology, digestive system diseases, NS2-3 protease, Infectious Diseases, chemistry, RNA Polymerase Inhibitor, Mutation, RNA, Viral, Protein Binding
Abstract

Compounds A-782759 (an N -1-aza-4-hydroxyquinolone benzothiadiazine) and BILN-2061 are specific anti-hepatitis C virus (HCV) agents that inhibit the RNA-dependent RNA polymerase and the NS3 serine protease, respectively. Both compounds display potent activity against HCV replicons in tissue culture. In order to characterize the development of resistance to these anti-HCV agents, HCV subgenomic 1b-N replicon cells were cultured with A-782759 alone or in combination with BILN-2061 at concentrations 10 times above their corresponding 50% inhibitory concentrations in the presence of neomycin. Single substitutions in the NS5B polymerase gene (H95Q, N411S, M414L, M414T, or Y448H) resulted in substantial decreases in susceptibility to A-782759. Similarly, replicons containing mutations in the NS5B polymerase gene (M414L or M414T), together with single mutations in the NS3 protease gene (A156V or D168V), conferred high levels of resistance to both A-782759 and BILN-2061. However, the A-782759-resistant mutants remained susceptible to nucleoside and two other classes of nonnucleoside NS5B polymerase inhibitors, as well as interferon. In addition, we found that the frequency of replicons resistant to both compounds was significantly lower than the frequency of resistance to the single compound. Furthermore, the dually resistant mutants displayed significantly reduced replication capacities compared to the wild-type replicon. These findings provide strategic guidance for the future treatment of HCV infection.

Published
2005
Full Text
View/download PDF

7. Identification of Novel Binding Interactions in the Development of Potent, Selective 2-Naphthamidine Inhibitors of Urokinase. Synthesis, Structural Analysis, and SAR of N-Phenyl Amide 6-Substitution

Author

Xumiao Zhao, Kent D. Stewart, Moshe Weitzberg, Michael D. Wendt, Vincent L. Giranda, Todd W. Rockway, Robert A. Mantei, Geyer Andrew George, Vicki L. Nienaber, Vered Klinghofer, and Mcclellan William J

Subjects
Models, Molecular, Stereochemistry, medicine.drug_class, Amidines, Substituent, Carboxamide, Naphthalenes, Crystallography, X-Ray, Amidine, Structure-Activity Relationship, chemistry.chemical_compound, Amide, Drug Discovery, medicine, Humans, Structure–activity relationship, Phenyl group, Binding site, Binding Sites, Molecular Structure, Urokinase-Type Plasminogen Activator, chemistry, Solvents, Molecular Medicine, Salt bridge, Protein Binding
Abstract

The preparation and assessment of biological activity of 6-substituted 2-naphthamidine inhibitors of the serine protease urokinase plasminogen activator (uPA, or urokinase) is described. 2-Naphthamidine was chosen as a starting point based on synthetic considerations and on modeling of substituent vectors. Phenyl amides at the 6-position were found to improve binding; replacement of the amide with other two-atom linkers proved ineffective. The phenyl group itself is situated near the S1' subsite; substitutions off of the phenyl group accessed S1' and other distant binding regions. Three new points of interaction were defined and explored through ring substitution. A solvent-exposed salt bridge with the Asp60A carboxylate was formed using a 4-alkylamino group, improving affinity to K(i) = 40 nM. Inhibitors also accessed two hydrophobic regions. One interaction is characterized by a tight hydrophobic fit made with a small dimple largely defined by His57 and His99; a weaker, less specific interaction involves alkyl groups reaching into the broad prime-side protein binding region near Val41 and the Cys42-Cys58 disulfide, displacing water molecules and leading to small gains in activity. Many inhibitors accessed two of these three regions. Affinities range as low as K(i) = 6 nM, and many compounds had K(i)100 nM, while moderate to excellent selectivity was gained versus four of five members of a panel of relevant serine proteases. Also, some selectivity against trypsin was generated via the interaction with Asp60A. X-ray structures of many of these compounds were used to inform our inhibitor design and to increase our understanding of key interactions. In combination with our exploration of 8-substitution patterns, we have identified a number of novel binding interactions for uPA inhibitors.

Published
2003
Full Text
View/download PDF

8. Inhibitors of the Protease Domain of Urokinase-Type Plasminogen Activator

Author

Vincent L. Giranda, Vicki L. Nienaber, and Todd W. Rockway

Subjects
Models, Molecular, Pharmacology, Serine protease, Urokinase, Proteases, Protease, biology, Chemistry, Plasmin, medicine.medical_treatment, Protein degradation, Urokinase-Type Plasminogen Activator, Protein Structure, Tertiary, Urokinase receptor, Biochemistry, Drug Discovery, biology.protein, medicine, Animals, Humans, Protease Inhibitors, Plasminogen activator, medicine.drug
Abstract

Human urokinase-type plasminogen activator (uPA or uPA) has been implicated in the regulation and control of basement membrane and interstitial protein degradation. Since Urokinase plays a role in tissue remodeling, it may be responsible, in part, for the disease progression of cancer. Inhibitors of urokinase may then be useful in the treatment of cancer by retarding tumor growth and metastasis. Urokinase is a multidomain protein, two regions of the protein are most responsible for the observed proteolytic activity in cancer disease and progression. The N-terminal domain or ATF binds to a Urokinase receptor (uPAR) on the cell surface and the C-terminal serine protease domain, then, activates plasminogen to plasmin, beginning a cascade of events leading to the progression of cancer. Investigations of urokinase inhibition has been an area of ongoing research for the past 3 decades. It began with the discovery of small natural and unnatural amino acid derivatives or peptide analogs which exhibited weak inhibition of uPA. The last decade has seen the generation of several classes of potent and selective Urokinase inhibitor directed to the serine protease domain of the protein which have shown potential anti-cancer effects. The availability of structural information of enzyme-inhibitor complexes either by nuclear magnetic spectroscopy (NMR) or crystallography has allowed a detailed analysis of inhibitor protein interactions that contribute to observed inhibitor potency. Structural studies of specific inhibitor-uPA complexes will be discussed as well as the contributions of specific inhibitor protein interactions that are important for overall inhibitor potency. These data were used to discover a class of urokinase inhibitor based on the 2-Naphthamidine template that exhibits potent urokinase inhibition and excellent selectivity for urokinase over similar trypsin family serine proteases.

Published
2002
Full Text
View/download PDF

9. Probing Inhibitors Binding to Human Urokinase Crystals by Raman Microscopy: Implications for Compound Screening

Author

Kerry M. Swift, Todd W. Rockway, Vicki L. Nienaber, Moshe Weitzberg, Edmund D. Matayoshi, Jian Dong, and Paul R. Carey

Subjects
biology, Chemistry, Stereochemistry, Active site, Biochemistry, Amidine, chemistry.chemical_compound, Crystallography, symbols.namesake, Molecular vibration, Functional group, biology.protein, symbols, Moiety, Raman microscope, Raman spectroscopy, Single crystal
Abstract

Inhibition of urokinase activity represents a promising target for antimetastatic therapy for several types of tumor. The present study sets out to investigate the potential of Raman spectroscopy for defining the molecular details of inhibitor binding to this enzyme, with emphasis on single crystal studies. It is demonstrated that high quality Raman spectra from a series of five inhibitors bound individually to the active site of human urokinase can be obtained in situ from urokinase single crystals in hanging drops by using a Raman microscope. After recording the spectrum of the free crystal, a solution of inhibitor containing an amidine functional group on a naphthalene ring was added, and the spectrum of the crystal−inhibitor complex was obtained. The resulting difference Raman spectrum contained only vibrational modes due to bound inhibitor, originating from the protonated group, i.e., the amidinium moiety, as well as naphthalene ring modes and features from other functionalities that made up each inh...

Published
2001
Full Text
View/download PDF

10. Species Specificity of Amidine-Based Urokinase Inhibitors

Author

Richard S. Smith, Xumiao Zhao, Aparna V. Sarthy, Vicki L. Nienaber, Kent D. Stewart, Moshe Weitzberg, K. I. Hulkower, Christopher C Butler, Vered Klinghofer, Vincent L. Giranda, Todd W. Rockway, Paul G. Richardson, Sarah A. Dorwin, Michael D. Wendt, and Tom Mcgonigal

Subjects
Serine Proteinase Inhibitors, Molecular Sequence Data, Amidines, Antineoplastic Agents, Thiophenes, Naphthalenes, Crystallography, X-Ray, Biochemistry, Amiloride, Carcinoma, Lewis Lung, Mice, Species Specificity, Tumor Cells, Cultured, medicine, Animals, Humans, Potency, Amino Acid Sequence, Binding site, chemistry.chemical_classification, Serine protease, Urokinase, Binding Sites, Sequence Homology, Amino Acid, biology, Blood Proteins, Urokinase-Type Plasminogen Activator, Blood proteins, Amino acid, Enzyme, chemistry, biology.protein, Sequence Alignment, medicine.drug
Abstract

Inhibition of the proteolytic activity of urokinase has been shown to inhibit the progression of tumors in rodent models and is being investigated for use in human disease. Understanding the rodent/human species-specificity of urokinase inhibitors is therefore critical for interpretation of rodent cancer progression models that use these inhibitors. We report here studies with a panel of 11 diverse urokinase inhibitors in both human and mouse enzymatic assays. Inhibitors such as amiloride, B428, and naphthamidine, that occupy only the S1 subsite pocket were found to be nearly equipotent between the human and the murine enzymes. Inhibitors that access additional, more distal, pockets were significantly more potent against the human enzyme but there was no corresponding potency increase against the murine enzyme. X-ray crystallographic structures of these compounds bound to the serine protease domain of human urokinase were solved and examined in order to explain the human/mouse potency differences. The differences in inhibitor potency could be attributed to four amino acid residues that differ between murine and human urokinases: 60, 99, 146, and 192. These residues are Asp, His, Ser, and Gln in human and Gln, Tyr, Glu, and Lys in mouse, respectively. Compounds bearing a cationic group that interacts with residue 60 will preferentially bind to the human enzyme because of favorable electrostatic interactions. The hydrogen bonding to residue 192 and steric considerations with residues 99 and 146 also contribute to the species specificity. The nonparallel human/mouse enzyme inhibition observations were extended to a cell-culture assay of urokinase-activated plasminogen-mediated fibronectin degradation with analogous results. These studies will aid the interpretation of in vivo evaluation of urokinase inhibitors.

Published
2001
Full Text
View/download PDF

11. Synthesis and SAR of novel 1,1-dialkyl-2(1H)-naphthalenones as potent HCV polymerase inhibitors

Author

Sherie Masse, Daniel P. Larson, Debra Montgomery, Dale J. Kempf, Warren M. Kati, Todd W. Rockway, Akhter Molla, Yaya Liu, Todd D. Bosse, Hongmei Mo, Doug K. Hutchinson, Tim Middleton, Gennadiy Koev, Rolf Wagner, and Wen Jiang

Subjects
Genotype, Stereochemistry, Hepatitis C virus, Hepacivirus, Clinical Biochemistry, Pharmaceutical Science, Naphthalenes, medicine.disease_cause, Biochemistry, Chemical synthesis, Virus, Structure-Activity Relationship, Drug Discovery, medicine, Enzyme Inhibitors, Molecular Biology, Polymerase, chemistry.chemical_classification, biology, Bicyclic molecule, Organic Chemistry, DNA-Directed RNA Polymerases, biology.organism_classification, Enzyme, chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine
Abstract

A series of gem -dialkyl naphthalenone derivatives with varied alkyl substitutions were synthesized and evaluated according to their structure–activity relationship. This investigation led to the discovery of potent inhibitors of the hepatitis C virus at low nanomolar concentrations in both enzymatic and cell-based HCV genotype 1a assays.

Published
2008
Full Text
View/download PDF

13. Inhibitors of HCV NS5B polymerase: synthesis and structure-activity relationships of N-alkyl-4-hydroxyquinolon-3-yl-benzothiadiazine sulfamides

Author

Tim Middleton, Dale J. Kempf, Rong Zhang, Todd W. Rockway, Warren M. Kati, John K. Pratt, Darold L. Madigan, Hongmei Mo, Keith F. McDaniel, Clarence J. Maring, Sherie Masse, Wen W. Jiang, Akhteruzzaman Molla, A. Chris Krueger, Dachun Liu, Yaya Liu, and Debra Montgomery

Subjects
Stereochemistry, Hepatitis C virus, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Viral Nonstructural Proteins, medicine.disease_cause, Benzothiadiazines, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, medicine, Structure–activity relationship, Enzyme Inhibitors, Molecular Biology, Polymerase, chemistry.chemical_classification, Sulfonamides, biology, Molecular Structure, Chemistry, Organic Chemistry, Enzyme, Enzyme inhibitor, Benzothiadiazine, Lactam, biology.protein, Molecular Medicine
Abstract

Substituted N-alkyl-4-hydroxyquinolon-3-yl-benzothiadiazine sulfamides were investigated as inhibitors of genotype 1 HCV polymerase. Structure-activity relationship patterns for this class of compounds are discussed.

Published
2006

14. Inhibitors of HCV NS5B polymerase: synthesis and structure-activity relationships of N-1-benzyl and N-1-[3-methylbutyl]-4-hydroxy-1,8-naphthyridon-3-yl benzothiadiazine analogs containing substituents on the aromatic ring

Author

Dachun Liu, Tim Middleton, Akhteruzzaman Molla, Sherie Masse, Rong Zhang, Dale J. Kempf, Debra Montgomery, David A. Betebenner, John K. Pratt, Todd W. Rockway, Clarence J. Maring, Warren M. Kati, David W A Beno, Wen W. Jiang, and Keith F. McDaniel

Subjects
Genotype, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Viral Nonstructural Proteins, Benzothiadiazines, Virus Replication, Biochemistry, Chemical synthesis, Hydrocarbons, Aromatic, chemistry.chemical_compound, Inhibitory Concentration 50, Structure-Activity Relationship, Drug Discovery, Structure–activity relationship, Enzyme Inhibitors, Naphthyridines, Molecular Biology, chemistry.chemical_classification, biology, Bicyclic molecule, Chemistry, Organic Chemistry, Nucleotidyltransferase, RNA-Dependent RNA Polymerase, Enzyme, Benzothiadiazine, Enzyme inhibitor, biology.protein, Lactam, Molecular Medicine
Abstract

A series of non-nucleoside HCV NS5B polymerase inhibitors based on the N-1-benzyl or N-1-[3-methylbutyl]-4-hydroxy-1,8-naphthyridon-3-yl benzothiadiazine core substituted in the D-ring aromatic moiety have been prepared and evaluated. Aromatic substituents extending from position 7 of the D-ring exhibited excellent potency against both genotypes 1a and 1b.

Published
2006

15. Naphthamidine urokinase plasminogen activator inhibitors with improved pharmacokinetic properties

Author

Xumiao Zhao, Kent D. Stewart, Dalton Christopher R, Daryl R. Sauer, Vicki L. Nienaber, Jennifer J. Bouska, Milan Bruncko, Moshe Weitzberg, Vincent L. Giranda, Todd W. Rockway, Robert A. Mantei, Jane Gong, Vered Klinghofer, Mcclellan William J, Joseph F. Dellaria, Kaminski Michele A, Geyer Andrew George, and Wendt Michael D

Subjects
chemistry.chemical_classification, Models, Molecular, biology, Chemistry, Urokinase Plasminogen Activator, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Naphthalenes, Biochemistry, Urokinase-Type Plasminogen Activator, In vitro, Substrate Specificity, Plasminogen Inactivators, Enzyme, Pharmacokinetics, U-plasminogen activator, Enzyme inhibitor, Drug Discovery, biology.protein, Molecular Medicine, Substrate specificity, Molecular Biology
Abstract

A series of non-amide-linked 6-substituted-2-naphthamidine urokinase plasminogen activator (uPA) inhibitors are described. These compounds possess excellent binding activities and selectivities with significantly improved pharmacokinetic profiles versus previously described amide-linked inhibitors.

Published
2004

16. Interaction with the S1 beta-pocket of urokinase: 8-heterocycle substituted and 6,8-disubstituted 2-naphthamidine urokinase inhibitors

Author

Geyer Andrew George, Moshe Weitzberg, Kent D. Stewart, Vicki L. Nienaber, Vincent L. Giranda, Michael D. Wendt, Todd W. Rockway, Robert A. Mantei, Vered Klinghofer, Xumiao Zhao, and Mcclellan William J

Subjects
Serine Proteinase Inhibitors, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Naphthalenes, Biochemistry, Sulfone, chemistry.chemical_compound, Amide, Drug Discovery, Hydrolase, medicine, Molecular Biology, Serine protease, chemistry.chemical_classification, Urokinase, biology, Activator (genetics), Organic Chemistry, Blood Proteins, Urokinase-Type Plasminogen Activator, Enzyme, chemistry, biology.protein, Molecular Medicine, Selectivity, medicine.drug
Abstract

Several 8-substituted 2-naphthamidine-based inhibitors of the serine protease urokinase plasminogen activator (uPA) are described. Direct attachment of five-membered saturated or unsaturated rings improved inhibitor performance; substitution with sulfones further improved binding profiles. Combination of these substituents or of previously described NH-linked heteroaromatic rings with 6-phenyl amide substituents provided further enhancements to potency and selectivity.

Published
2004

17. Inhibition of human immunodeficiency virus type I integrase by naphthamidines and 2-aminobenzimidazoles

Author

Todd W. Rockway, Hongmei Mo, Tim Middleton, William E. Kohlbrenner, Xueheng Cheng, Debra Montgomery, Hock Ben Lim, Hua Tang, Warren M. Kati, Akhteruzzaman Molla, and Liangjun Lu

Subjects
Benzimidazole, Genes, Viral, Integrase inhibitor, HIV Integrase, In Vitro Techniques, Naphthalenes, Virus, Cell Line, chemistry.chemical_compound, Virology, Humans, HIV Integrase Inhibitors, Pharmacology, biology, Base Sequence, Molecular Structure, Integrases, biology.organism_classification, Recombinant Proteins, Integrase, genomic DNA, chemistry, Lentivirus, DNA, Viral, biology.protein, HIV-1, Benzimidazoles, DNA
Abstract

Retroviral integrases catalyze two of the steps of insertion of proviral DNA into the host genomic DNA. Inhibitors that target the second step, strand transfer into the host DNA, have been demonstrated to have antiviral activity in cell culture. We describe two classes of HIV-1 integrase inhibitors that block strand transfer, one based on a naphthamidine core and one on a benzimidazole core. While the naphthamidine compounds showed some propensity to interact with the DNA substrate, both classes were shown to bind directly to integrase. The naphthamidine compounds showed activity in cell culture, and a direct effect on integrase was indicated by an increase in 2-LTR products in the presence of a naphthamidine compound. These two classes of compounds represent potential starting points for the development of new classes of integrase inhibitors.

Published
2003

18. Pyridone-containing farnesyltransferase inhibitors: synthesis and biological evaluation

Author

Wen-Zhen Gu, Saul H. Rosenberg, Le Wang, Todd W. Rockway, Robert A. Mantei, Joy Bauch, Haiying Zhang, Hing L. Sham, Lisa A. Hasvold, Stephen L. Gwaltney, Stephen A. Fakhoury, Nelson Lissa T, Weibo Wang, Nan-Horng Lin, Qun Li, Kennan C. Marsh, Jerome Cohen, and Gerard M. Sullivan

Subjects
Pyridones, Farnesyltransferase, Clinical Biochemistry, Pharmaceutical Science, Antineoplastic Agents, Biochemistry, Chemical synthesis, Structure-Activity Relationship, In vivo, Cell Line, Tumor, Drug Discovery, Animals, Farnesyltranstransferase, Humans, Enzyme Inhibitors, Molecular Biology, Biological evaluation, chemistry.chemical_classification, Farnesyl-diphosphate farnesyltransferase, Alkyl and Aryl Transferases, biology, Molecular Structure, Organic Chemistry, In vitro, Enzyme, chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine, Cell Division
Abstract

Farnesyltransferase inhibitors (FTIs) have been developed as potential anti-cancer agents due to their efficacy in blocking malignant growth in a variety of murine models of human tumors. To that end, we have developed a series of pyridone farnesyltransferase inhibitors with potent in vitro and cellular activity. The synthesis, SAR and biological properties of these compounds will be discussed.

Published
2003

19. Inhibitors of the proteolytic activity of urokinase type plasminogen activator

Author

Vincent L. Giranda and Todd W. Rockway

Subjects
Pharmacology, Urokinase, Research groups, Plasmin, business.industry, Hydrolysis, Cancer, medicine.disease, Urokinase-Type Plasminogen Activator, Urokinase receptor, Tissue remodeling, Drug Discovery, medicine, Cancer research, Animals, Humans, Protease Inhibitors, business, Plasminogen activator, medicine.drug, Peptide Hydrolases
Abstract

Urokinase type plasminogen activator (uPA) activates plasminogen to plasmin and is often associated with diseases where tissue remodeling is essential (e.g. cancer, macular degeneration, atherosclerosis). We discuss some of the mechanisms of uPA action in diseases, and evidence that some of the early uPA inhibitors can modulate the progression of these diseases. Recently, a number of research groups have discovered, with the aid of structure-based design, a new generation of uPA inhibitors. These inhibitors are much more potent and selective than their predecessors. We will review this progress here, and give particular attention to the structural rationale associated with these observed increases in potency and selectivity.

Published
2003

20. Identification of novel inhibitors of urokinase via NMR-based screening

Author

Philip J. Hajduk, Richard D. Smith, Jean M. Severin, Stephen W. Fesik, Boyd Steven A, Vicki L. Nienaber, David G. Nettesheim, Don J. Davidson, and Todd W. Rockway

Subjects
Urokinase, Models, Molecular, Magnetic Resonance Spectroscopy, Bicyclic molecule, biology, Molecular model, Blood clotting, Chemistry, Stereochemistry, Crystallography, X-Ray, Urokinase-Type Plasminogen Activator, Inhibitory potency, Structure-Activity Relationship, Biochemistry, Enzyme inhibitor, Drug Discovery, biology.protein, medicine, Molecular Medicine, Moiety, Benzimidazoles, Enzyme Inhibitors, Electrostatic interaction, medicine.drug
Abstract

Using an NMR-based screen, a novel class of urokinase inhibitors were identified that contain a 2-aminobenzimidazole moiety. The inhibitory potency of this family of inhibitors is similar to that of inhibitors containing a guanidine or amidine group. However, unlike previously described guanidino- or amidino-based inhibitors which have pK(a) values greater than 9.0, urokinase inhibitors containing a 2-aminobenzimidazole have pK(a) values of 7.5. Thus, 2-aminobenzimidazoles may have improved pharmacokinetic properties which could increase the bioavailability of inhibitors which contain this moiety. A crystal structure of one of the lead inhibitors, 2-amino-5-hydroxybenzimidazole, complexed with urokinase reveals the electrostatic and hydrophobic interactions that stabilize complex formation and suggests nearby subsites that may be accessed to increase the potency of this new series of urokinase inhibitors.

Published
2000

21. The Design and Synthesis of Long-Acting Oxytocin Antagonists Substituted in Positions 2, 7, and 8

Author

Jan Hlaváček, Victor J. Hruby, Todd W. Rockway, James Ormberg, and W. Y. Chan

Subjects
Peptide analog, Long acting, Oxytocin, Stereochemistry, Chemistry, medicine, Oxytocin receptor, medicine.drug
Abstract

The design of oxytocin antagonists (for reviews, see Hruby and Mosberg, 1982; Hruby and Smith, 1987; Hruby et al., 1990; Lebl, 1987; Manning and Sawyer, 1989; Sawyer and Manning, 1985) has increasingly involved a search for structural changes that would enhance both in vivo potency and increase duration of action. The discovery of Shulz and du Vigneaud (1966, 1967) and Jost et al. (1961) that substituting more bulky amino acids in either position 1 (penicillamine) or position 2 (O-methyltyrosine) produced oxytocin antagonists has led to numerous further investigations into the structural and conformational requirements important for antagonism at the uterine oxytocin receptor (Hruby, 1985; Hruby et al., 1990; Manning and Sawyer, 1989; Meraldi et al., 1975, 1977). Since these pioneering studies, many important, more potent antagonists have been reported, particularly by the groups of Manning et al., Melin et al., Lebl et al., and Hruby et al. (Hruby and Smith, 1987; Lebl, 1987; Manning and Sawyer, 1985) primarily by incorporating appropriate amino acid substitutions into positions 1, 2, 4, 7, and 8, including linear analogs (Manning et al., 1987).

Published
1994
Full Text
View/download PDF

23. HPLC and PDMS analysis of cleavage products aid in the design of small, stable ANP analogues

Author

Todd W. Rockway, Thomas W. von Geldern, Alexander M. Buko, William H. Holleman, Carol A. Marselle, Terry J. Opgenorth, Steven K. Davidsen, Steven P. Cepa, and Edward M. Devine

Subjects
Male, Stereochemistry, Proteolysis, Molecular Sequence Data, Tripeptide, Cleavage (embryo), Kidney, Biochemistry, High-performance liquid chromatography, Mass Spectrometry, Dogs, Atrial natriuretic peptide, Drug Stability, In vivo, medicine, Animals, Amino Acid Sequence, Chromatography, High Pressure Liquid, chemistry.chemical_classification, Chromatography, medicine.diagnostic_test, In vitro, Amino acid, chemistry, Rabbits, Peptides, Atrial Natriuretic Factor, Half-Life
Abstract

The degradation of a prototypical small analogue of atrial natriuretic peptide (ANP) has been studied using HPLC and mass spectrometric techniques. These studies revealed that removal of the N-terminal amino acid was the primary catabolic event in vitro. Based on this information the N-terminus was remanufactured to provide a family of more stable analogues. Additional stabilization was provided through modification of the C-terminal tripeptide. Through dramatically more stable in vitro, these new analogues do not appear to have longer in vivo half-lives.

Published
1992

24. Small atrial natriuretic peptide analogues: design, synthesis, and structural requirements for guanylate cyclase activation

Author

M Y Chu-Moyer, E N Bush, William H. Holleman, Scott D. Lucas, Steven K. Davidsen, Todd W. Rockway, M C Johnson, T. W. von Geldern, G. P. Budzik, and E. M. Devine

Subjects
Agonist, Male, medicine.drug_class, Molecular Sequence Data, Natriuresis, Receptors, Cell Surface, Binding, Competitive, Structure-Activity Relationship, Dogs, Atrial natriuretic peptide, Drug Discovery, medicine, Structure–activity relationship, Animals, Amino Acid Sequence, Receptor, Peptide sequence, Cyclic GMP, Chemistry, GUCY1A3, Rats, Inbred Strains, Acute Kidney Injury, NPR1, NPR2, Peptide Fragments, Diuresis, Rats, Enzyme Activation, Biochemistry, Guanylate Cyclase, cardiovascular system, Molecular Medicine, Rabbits, Receptors, Atrial Natriuretic Factor, hormones, hormone substitutes, and hormone antagonists, Atrial Natriuretic Factor
Abstract

Structure/activity studies on atrial natriuretic peptide ANP (1-28) have highlighted three portions of the native molecule as necessary for its biological responses. We have linked these three regions and excised the remaining segments to produce a family of small analogues (less than half the size of the parent) which demonstrate the full range of ANP's actions. Importantly, these compounds act at both major types of ANP receptor. Two critical modifications lead to more potent analogues; both involve expanding the cyclic portion of the molecule. Further optimization of one of these modified structures leads to A68828, a full ANP agonist which shows promise as a preventative agent against acute renal failure.

Published
1992

25. Truncated atrial natriuretic factor analogs retain full agonist activity

Author

William H. Holleman, T. W. von Geldern, T. J. Opgenorth, A. M. Thomas, G. P. Budzik, E. M. Devine, D. M. Pollock, and Todd W. Rockway

Subjects
Agonist, Arginine, Physiology, Stereochemistry, medicine.drug_class, Phenylalanine, Peptide, Receptors, Cell Surface, In Vitro Techniques, Binding, Competitive, chemistry.chemical_compound, Biosynthesis, Atrial natriuretic peptide, Physiology (medical), medicine, Animals, Cyclic GMP, Pharmacology, chemistry.chemical_classification, Cell Membrane, General Medicine, Cyclic peptide, Amino acid, chemistry, Biochemistry, Adrenal Cortex, Rabbits, Receptors, Atrial Natriuretic Factor, Atrial Natriuretic Factor
Abstract

The synthesis, receptor binding, and agonist activity of a series of truncated atrial natriuretic analogs (ANF) are described. These analogs incorporate two portions of the native 28 amino peptide, the eight amino acids C-terminal to Cys7, and two amino acids from the C-terminus (phenylalanine and arginine), into disulfide-bonded cyclic peptides. The inclusion of the C-terminal amino acids converted the ANF analogs from receptor ligands to full agonists, as measured by several methods, including the stimulation of cGMP biosynthesis in endothelial cells, inhibition of aldosterone biosynthesis in rat adrenal cells, and natriuretic–hypotensive activity in vivo. The most potent analogs have cyclohexylalanine (Cha) at position 8. The lead compound (Arg6,Cha8 ANF 6–15 Phe-Arg-Cys-NH2) is a tridecapeptide that integrates the C-terminal amino acids inside the disulfide ring. This peptide, designated as A-68828, has a binding affinity of IC50 = 120 nM, approximately 1/400 of ANF 1–28. However, this analog, in vivo, is only slightly less natriuretic (1/20–1/50) than ANF 1–28. Unlike the native peptide, A-68828 is only mildly hypotensive and at the highest concentration tested reduced blood pressure less than 15 mmHg (1 mmHg = 133.322 Pa). A-68828 inhibited ACTH-induced aldosterone release to a greater extent than ANF 1–28: 100 vs. 50%. The selective natriuretic activity of A-66828, relative to ANF, suggests clinical utility for the treatment of acute renal failure.Key words: atrial natriuretic factor, renal failure, dopamine, peptide analogs, cGMP.

Published
1991

29. Conformational and dynamic considerations in the design of peptide hormone analogs

Author

James J. Knittel, Victor J. Hruby, Paul S. Darman, Todd W. Rockway, W Y Chan, Tomi K. Sawyer, Mac E. Hadley, Henry I. Mosberg, and James Ormberg

Subjects
chemistry.chemical_classification, Protein Conformation, Chemistry, Organic Chemistry, Biophysics, Peptide, Biological activity, General Medicine, Peptide hormone, Oxytocin, Biochemistry, Biomaterials, Structure-Activity Relationship, Transduction (genetics), In vivo, Animals, Amino Acid Sequence, Melanocyte-Stimulating Hormones, Receptor, Function (biology), Hormone
Abstract

Efforts to understand the chemical-physical basis for peptide hormone and neurotransmitter action requires integration of conformational parameters and biological properties. Since most peptide hormones are conformationally flexible, the question arises as to which of the manifold of conformations is of biological significance. In molecular terms, it is necessary to carefully distinguish chemical-physical features important to binding (the binding message) from those involved in transduction (the biological activity message). One approach to this involves the design, synthesis, and conformational analysis of semirigid hormone analogs. The distinction between binding and transduction can best be examined by evaluation of full biological profiles of partial agonists, antagonists, and analogs with prolonged biological activity. Using this multidisciplinary approach, we have prepared several semirigid [Pen1]-oxytocin antagonist analogs and evaluated their conformational properties and biological activities. Specific conformational features can be related to inhibitory activities in several cases. On the basis of structure–activity relationships and conformational considerations, we have designed a series of conformationally restricted cyclic and acyclic analogs of the linear peptide α-melanotropin. Some of these peptides have exceptionally prolonged in vivo activity (weeks), and others exhibit superagonist potency (10,000 times the native hormone). We have evidence that potency and prolonged activity have different structural and conformational requirements. It is suggested that potency is primarily a function of receptor recognition (the binding message), whereas prolonged activity is related to transduction (the biological activity message).

Published
1983
Full Text
View/download PDF

31. Atrial natriuretic factor: Structural requirements of the peptide for receptor binding, biological activity, and cGMP stimulation

Author

Edward M. Devine, Todd W. Rockway, Susan L. Firestone, E N Bush, G. P. Budzik, Virender K. Sarin, and William H. Holleman

Subjects
chemistry.chemical_classification, medicine.medical_specialty, Vascular smooth muscle, Aldosterone, Biological activity, Stimulation, Peptide, Peptide hormone, musculoskeletal system, Ligand (biochemistry), chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, Drug Discovery, cardiovascular system, medicine, Receptor
Abstract

The atrial natriuretic factor (ANF) family of peptides possesses diverse functional properties including smooth-muscle relaxation, inhibition of aldosterone biosynthesis, and hypotensive activities. These separate activities are most likely mediated by the binding of the peptide to specific receptors located in the target organs. The present study was initiated to more closely examine the relationship between biological activity and the requirements of the various receptors for interaction with ANF and with ANF analogs. Binding affinities (Ki) were measured in plasma membranes isolated from rabbit kidney cortex, aorta, and adrenal, and in cultured rabbit aortic vascular smooth muscle cells (VSMC) using 125I-Tyr-28-ANF (1–28) as the ligand. The VSMC were also utilized to quantitate stimulation of cGMP synthesis. Vasorelaxation (pD2) was measured in histamine-contracted rabbit aortic rings. The activities of 19 ANF (5–28) analogs were compared, and a significant correlation between pD2 and Ki (r = −.83; p < 0.01) was obtained. The (D)Phe-8 and Asn-13 analogs were exceptions to this correlation; pD2 = 7.1 and 7.2, and pKi = 6.0 and 8.1, respectively. All analogs examined possessed comparable affinities in the four receptor assays. Conversely, comparison of vasorelaxant and cGMP stimulatory activities resulted in a much larger separation of activities. Tyr-8 ANF (5–27) did not stimulate cGMP synthesis but relaxed smooth muscle (pD2 = 7.9), while ANF (7–23) was 500-fold less active than ANF (5–28) in the vasorelaxant assay (pD2 = 6.1 and 8.9, respectively) but equipotent in the cGMP system. These and other experiments suggest the presence of ANF receptor subtypes and question the causative role of cGMP for inducing vasorelaxation of histamine-constricted aortic rings.

Published
1988
Full Text
View/download PDF

32. Structure-directed discovery of potent non-peptidic inhibitors of human urokinase that access a novel binding subsite

Author

Karl A. Walter, Richard A. Smith, Todd W. Rockway, Robert A. Mantei, Sean M. Merrick, Rohinton Edalji, Michael D. Wendt, Vicki L. Nienaber, Moshe Weitzberg, Jieyi Wang, Jack Henkin, Vincent L. Giranda, Peter Magdalinos, Kent D. Stewart, Vered Klinghofer, Jean M. Severin, Xumiao Zhao, and Donald J. Davidson

Subjects
Models, Molecular, Proteases, Macromolecular Substances, medicine.medical_treatment, Naphthalenes, Protein degradation, Crystallography, X-Ray, Drug design, Substrate Specificity, Protein structure, Thrombin, Structural Biology, medicine, Humans, Enzyme Inhibitors, Urokinase, Molecular Biology, X-ray crystallography, Binding Sites, Protease, Chemistry, Inhibitors, Urokinase-Type Plasminogen Activator, Protein Structure, Tertiary, Urokinase receptor, Biochemistry, Plasminogen activator, Tumor metastasis, medicine.drug
Abstract

Background: Human urokinase-type plasminogen activator has been implicated in the regulation and control of basement membrane and interstitial protein degradation. Because of its role in tissue remodeling, urokinase is a central player in the disease progression of cancer, making it an attractive target for design of an anticancer clinical agent. Few urokinase inhibitors have been described, which suggests that discovery of such a compound is in the early stages. Towards integrating structural data into this process, a new human urokinase crystal form amenable to structure-based drug design has been used to discover potent urokinase inhibitors. Results: On the basis of crystallographic data, 2-naphthamidine was chosen as the lead scaffold for structure-directed optimization. This co-crystal structure shows the compound binding at the primary specificity pocket of the trypsin-like protease and at a novel binding subsite that is accessible from the 8-position of 2-napthamidine. This novel subsite was characterized and used to design two compounds with very different 8-substituents that inhibit urokinase with K i values of 30–40 nM. Conclusions: Utilization of a novel subsite yielded two potent urokinase inhibitors even though this site has not been widely used in inhibitor optimization with other trypsin-like proteases, such as those reported for thrombin or factor Xa. The extensive binding pockets present at the substrate-binding groove of these other proteins are blocked by unique insertion loops in urokinase, thus necessitating the utilization of additional binding subsites. Successful implementation of this strategy and characterization of the novel site provides a significant step towards the discovery of an anticancer clinical agent.

Full Text
View/download PDF

33. Active and inactive L-prolyl-L-leucyl glycinamide synthetic analogs in rat models of levodopa-treated Parkinson's disease

Author

Victor J. Hruby, Todd W. Rockway, Stuart R. Snider, and Todd C. Case

Subjects
Levodopa, Parkinson's disease, medicine.medical_treatment, Rat model, Tripeptide, Pharmacology, Motor Activity, Peptides, Cyclic, General Biochemistry, Genetics and Molecular Biology, Antiparkinson Agents, Structure-Activity Relationship, Hypokinesia, medicine, Animals, General Pharmacology, Toxicology and Pharmaceutics, Chemotherapy, Chemistry, Parkinsonism, Neuropeptides, Carbidopa, Drug Synergism, Parkinson Disease, General Medicine, Dipeptides, medicine.disease, MSH Release-Inhibiting Hormone, nervous system diseases, Rats, Drug Therapy, Combination, medicine.symptom, medicine.drug
Abstract

The tripeptide, L-prolyl-L-leucyl-glycinamide (PLG) has been shown to facilitate dopaminergic mechanisms in the brain. In the present study, we evaluated the interaction of PLG and its synthetic analogs with levodopa in two animal models of Parkinson's disease. In one experiment using rats with chronic unilateral lesions of the nigrostriatal dopamine pathway, PLG and Z-PLG potentiated the contraversive rotation elicited by levodopa with carbidopa (L/C). In a second experiment using reserpinized rats, PLG, Z-PLG and cyclo-LG potentiated L/C reversal of hypokinesia. Further studies of the PLG analogs, Z-PLG and cyclo-LG as adjunctive drugs with levodopa in the treatment of parkinsonism are warranted.

Published
1985

36. Two-dimensional NMR studies of [Pro-10] atrial natriuretic factor [7-23]

Author

Peter J. Connolly, Stephen W. Fesik, Robert T. Gampe, and Todd W. Rockway

Subjects
chemistry.chemical_classification, Magnetic Resonance Spectroscopy, Chemistry, Stereochemistry, Protein Conformation, Organic Chemistry, Biophysics, Peptide, Sequence (biology), General Medicine, Nuclear magnetic resonance spectroscopy, Biochemistry, Peptide Fragments, Biomaterials, Glycine, Proton NMR, Proline, Spectroscopy, Vicinal, Atrial Natriuretic Factor
Abstract

The conformational properties of an analog of atrial naturiuretic factor, [Pro-10] ANF(7-23), were examined in H2O, H2O/DMSO-d6 (2/1), and DMSO-d6 using two-dimensional nmr techniques. The sequence differs from the native peptide by the absence of the exocyclic N- and C-terminal residues, and the substitution of a proline for a glycine at position 10—a modification expected to reduce the conformational flexibility of this analog. The backbone proton nmr resonances were assigned from two-dimensional correlated spectroscopy (2D-COSY), relayed COSY, and 2D nuclear Overhauser enhancement (NOE) experiments, and the solution conformation was evaluated from vicinal spin–spin coupling constants and NOE data. Despite the substitution of a proline in the sequence, [Pro-10] ANF(7-23) exhibits a considerable amount of flexibility in all of the solvents employed.

Published
1988

37. Divergence of ANF analogs in smooth muscle cell cGMP response and aorta vasorelaxation: evidence for receptor subtypes

Author

G. P. Budzik, Peter J. Connolly, Susan L. Firestone, Virender K. Sarin, Todd W. Rockway, Eugene N. Bush, and William H. Holleman

Subjects
medicine.medical_specialty, Cell, Biophysics, Vasodilation, Aorta, Thoracic, Receptors, Cell Surface, Biology, In Vitro Techniques, Biochemistry, Muscle, Smooth, Vascular, Structure-Activity Relationship, Smooth muscle, medicine.artery, Internal medicine, otorhinolaryngologic diseases, medicine, Structure–activity relationship, Thoracic aorta, Animals, Receptor, Molecular Biology, Cyclic GMP, Cells, Cultured, Aorta, Cell Biology, In vitro, medicine.anatomical_structure, Endocrinology, cardiovascular system, Rabbits, Receptors, Atrial Natriuretic Factor, hormones, hormone substitutes, and hormone antagonists, Atrial Natriuretic Factor
Abstract

ANF analog potencies in stimulating smooth muscle cell cGMP were compared with the ability to relax histamine-constricted rabbit aorta in vitro. ANF[1-28], [5-28], [5-27] and Lys-11[5-28] elevated cGMP and were potent vasorelaxants. ANF[7-23] and Lys-11[7-23] were potent cGMP stimulators but 1000-fold weaker relaxants. Tyr-8[5-27] did not stimulate cGMP synthesis or antagonize the response of the other peptides, yet was a potent vasorelaxant. Crosslinking with 125I-ANF identified bands at 150 and 65 KD by SDS-PAGE. ANF[1-28], Lys-11[7-23] and Tyr-8[5-27] blocked crosslinking at low concentration despite disparate activities. These data support the existence of ANF receptor subtypes and suggest that cGMP elevation alone is not sufficient to promote atrial peptide-induced vasorelaxation.

Published
1987

38. Pharmacological, conformational and dynamic properties of cycloleucine-2 analogues of oxytocin and [1-penicillamine]oxytocin

Author

Todd W. Rockway, Victor J. Hruby, V. Viswanatha, and W. Y. Chan

Subjects
Agonist, endocrine system, medicine.medical_specialty, Magnetic Resonance Spectroscopy, medicine.drug_class, Protein Conformation, Oxytocin, Biochemistry, Oxytocin Antagonist, chemistry.chemical_compound, Structure-Activity Relationship, Internal medicine, medicine, Animals, Receptor, 1-penicillamine-oxytocin, Cycloleucine, Antagonist, In vitro, Hormones, Rats, Endocrinology, chemistry, Biological Assay, Female, hormones, hormone substitutes, and hormone antagonists, medicine.drug
Abstract

The solid phase syntheses of [2-cycloleucine] oxytocin and [1-penicillamine, 2-cycloleucine] oxytocin are reported. [1-Penicillamine, 2-cycloleucine] oxytocin is an oxytocin antagonist exhibiting no in vitro oxytocic activity. In the in vitro oxytocic assay, [1-penicillamine, 2-cycloleucine] oxytocin has a pA2 value of 6.70 +/- 0.08. [2-Cycloleucine]-oxytocin is a full oxytocin agonist exhibiting 4.9 +/- 0.5 U/mg of oxytocic activity. Neither compound possesses any measurable agonist or antagonist activity in the rat pressor assay. Carbon-13 nuclear magnetic resonance chemical shift parameters and spin-lattice relaxation times (T1) of the antagonist, [1-penicillamine, 2-cycloleucine] oxytocin, indicate that the antagonist exhibits similar conformational and dynamic properties as other oxytocin inhibitors previously studied. The carbon-13 nuclear magnetic resonance shift parameters and spin-lattice relaxation times (T1) of the oxytocin agonist, [2-cycloleucine] oxytocin, indicate that the agonist exhibits similar conformational and dynamic properties as oxytocin. These results are discussed in terms of the different receptor requirements for agonist and antagonist activities. It appears that there are different structural and conformational requirements at the 2-position for oxytocic agonist and antagonist activities.

Published
1983

39. NMR study of the solution conformation of rat atrial natriuretic factor 7-23 in sodium dodecyl sulfate micelles

Author

Edward T. Olejniczak, Stephen W. Fesik, Todd W. Rockway, and Robert T. Gampe

Subjects
chemistry.chemical_classification, Models, Molecular, Magnetic Resonance Spectroscopy, Stereochemistry, Protein Conformation, Sodium Dodecyl Sulfate, Peptide, Nuclear Overhauser effect, Biochemistry, Micelle, Peptide Fragments, Rats, NMR spectra database, Solutions, chemistry.chemical_compound, Crystallography, chemistry, Cardiovascular agent, Proton NMR, Animals, Sodium dodecyl sulfate, Protein secondary structure, Atrial Natriuretic Factor, Micelles
Abstract

The conformation of the cyclic portion (7-23) of naturally occurring rat atrial natriuretic factor, ANF(1-28), has been examined in sodium dodecyl sulfate (SDS) micelles using high-resolution NMR techniques. Evidence is presented which shows that ANF(7-23) has several regions of definable structure in SDS micelles which were not observed in earlier studies in bulk solvents. The /sup 1/H NMR resonances of ANF(7-23) in SDS micelles were assigned using sequential assignment techniques, and the conformational properties were analyzed primarily from proton-proton distances obtained from the quantitative analysis of two-dimensional nuclear Overhauser effect spectra. Three-dimensional structures consistent with the NMR data were generated by using distance geometry and constrained minimization/dynamics. Several similar but not identical structures were found which adequately satisfied the NMR constraints. Although none of the structures adopted a standard secondary structure, the conformations of three different sections of the peptide, 8-13, 14-17, and 18-21, were nearly identical in all of the predicted structures when individually superimposed.

Published
1988

40. Binding and Molecular Properties of Atrial Natriuretic Hormone (ANH) Receptors from Rabbit Aorta, Renal Cortex, and Adrenal

Author

Todd W. Rockway, Eugene N. Bush, Virender K. Sarin, W. Holleman, G. P. Budzik, Peter J. Connolly, and Edward M. Devine

Subjects
Pharmacology, medicine.medical_specialty, Endocrinology, medicine.anatomical_structure, business.industry, Internal medicine, Renal cortex, Rabbit aorta, Atrial natriuretic hormone, medicine, Cardiology and Cardiovascular Medicine, business, Receptor
Published
1986
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results