Your search keyword '"John P. Umland"' showing total 17 results

1. Quantitative Contribution of Six Major Transporters to the Hepatic Uptake of Drugs: 'SLC-Phenotyping' Using Primary Human Hepatocytes

Author

John P. Umland, Yi-an Bi, Soraya Eatemadpour, Hui Zhang, Manthena V.S. Varma, David A. Tess, Mark A. West, Emi Kimoto, Laurie Tylaska, Sarah Lazzaro, Chester Costales, Renato J. Scialis, Larry M. Tremaine, A. David Rodrigues, Sumathy Mathialagan, and Bo Feng

Subjects

0301 basic medicine, Quinidine, Liver cytology, Quantitative proteomics, Peptide, Pharmacology, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Drug Interactions, Solute Carrier Proteins, chemistry.chemical_classification, biology, HEK 293 cells, Biological Transport, Transporter, In vitro, Organic anion-transporting polypeptide, HEK293 Cells, Phenotype, 030104 developmental biology, Liver, Pharmaceutical Preparations, chemistry, Hepatocytes, biology.protein, Molecular Medicine, Hydroxymethylglutaryl-CoA Reductase Inhibitors, Rifampin, 030217 neurology & neurosurgery, medicine.drug

Abstract

Hepatic uptake transporters [solute carriers (SLCs)], including organic anion transporting polypeptide (OATP) 1B1, OATP1B3, OATP2B1, sodium-dependent taurocholate cotransporting polypeptide (NTCP), and organic anion (OAT2) and organic cation (OCT1) transporters, play a key role in determining the systemic and liver exposure of chemically diverse drugs. Here, we established a phenotyping approach to quantify the contribution of the six SLCs, and passive diffusion, to the overall uptake using plated human hepatocytes (PHHs). First, selective inhibitor conditions were identified by screening about 20 inhibitors across the six SLCs using single-transfected human embryonic kidney 293 cells. Data implied rifamycin SV (20 µM) inhibits three OATPs, while rifampicin (5 µM) inhibits OATP1B1/1B3 only. Further, hepatitis B virus myristoylated-preS1 peptide (0.1 µM), quinidine (100 µM), and ketoprofen (100-300 µM) are relatively selective against NTCP, OCT1, and OAT2, respectively. Second, using these inhibitory conditions, the fraction transported (ft ) by the individual SLCs was characterized for 20 substrates with PHH. Generally, extended clearance classification system class 1A/3A (e.g., warfarin) and 1B/3B compounds (e.g., statins) showed predominant OAT2 and OATP1B1/1B3 contribution, respectively. OCT1-mediated uptake was prominent for class 2/4 compounds (e.g., metformin). Third, in vitro ft values were corrected using quantitative proteomics data to obtain "scaled ft " Fourth, in vitro-in vivo extrapolation of the scaled OATP1B1/1B3 ft was assessed, leveraging statin clinical drug-drug interaction data with rifampicin as the perpetrator. Finally, we outlined a novel stepwise strategy to implement phenotypic characterization of SLC-mediated hepatic uptake for new molecular entities and drugs in a drug discovery and development setting.

Published

2019

2. Mechanistic insights on clearance and inhibition discordance between liver microsomes and hepatocytes when clearance in liver microsomes is higher than in hepatocytes

Author

Manthena V.S. Varma, Ravi Visswanathan, David A. Tess, Caitlin Jagla, George Chang, JianHua Liu, Rhys M. Jones, Christopher Keefer, Li Di, John P. Umland, Nathaniel Johnson, Heather Eng, Michael J. Banker, R. Scott Obach, Keith Riccardi, Jillian Racich, Samantha Jordan, Anthony Carlo, Jonathan J. Novak, Jackie Carey, Julie Cianfrogna, and Sarah Lazzaro

Subjects

Metabolic Clearance Rate, Chemistry, CYP3A, Pharmaceutical Science, Biological Transport, Transporter, 02 engineering and technology, Metabolism, Pharmacology, 021001 nanoscience & nanotechnology, 030226 pharmacology & pharmacy, In vitro, Kinetics, 03 medical and health sciences, 0302 clinical medicine, Liver, In vivo, Hepatocytes, Microsomes, Liver, Microsome, Humans, Efflux, 0210 nano-technology, human activities, IC50

Abstract

Human liver microsomes (HLM) and human hepatocytes (HHEP) are two common in vitro systems used in metabolic stability and inhibition studies. The comparison between the assays using the two systems can provide mechanistic insights on the interplay of metabolism, passive permeability and transporters. This study investigated the critical factors impacting the unbound intrinsic clearance (CLint,u) and IC50 of CYP3A inhibition between HLM and HHEP. The HLM/HHEP CLint,u ratio and HHEP/HLM IC50 ratio are inversely correlated to passive permeability, but have no correlation with P-gp efflux ratio. Cofactor-supplemented permeabilized HHEP (MetMax™) collapses the IC50 differences between HHEP and HLM. P-gp inhibitor, encequidar, shows minimal impact on CLint,u and IC50 in HHEP. This is the first study that is able to separately investigate the effects of passive permeability and efflux transport. These data collectively show that passive permeability plays a critical role in metabolism and enzyme inhibition in HHEP, while P-gp efflux has a minor role. This may be due to low functional P-gp activity in suspension HHEP under the assay conditions. Low passive permeability may limit metabolism and enzyme inhibition in HHEP, leading to lower CLint,u and higher IC50 in HHEP compared to HLM. When liver microsomes give higher CLint,u than hepatocytes, microsomes are more predictive of in vivo clearance than hepatocytes.

Published

2020

3. In Vitro-In Vivo Extrapolation of Key Transporter Activity at the Blood-Brain Barrier

Author

Anthony Carlo, Bo Feng, Mark A. West, Jennifer L. Liras, Nandini Chaturbhai Patel, Thomas Y. K. Lau, Travis T. Wager, Matthew D. Troutman, Patrick Trapa, John P. Umland, and Tristan S. Maurer

Subjects

Abcg2, Pharmaceutical Science, ATP-binding cassette transporter, Blood–brain barrier, Proteomics, 030226 pharmacology & pharmacy, Cell Line, Madin Darby Canine Kidney Cells, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, Dogs, In vivo, medicine, Animals, ATP Binding Cassette Transporter, Subfamily B, Member 1, Pharmacology, biology, Chemistry, Brain, Transporter, Biological Transport, In vitro, Rats, medicine.anatomical_structure, Blood-Brain Barrier, 030220 oncology & carcinogenesis, Biophysics, biology.protein, Efflux

Abstract

Understanding the quantitative implications of P-glycoprotein and breast cancer resistance protein efflux is a key hurdle in the design of effective, centrally acting or centrally restricted therapeutics. Previously, a comprehensive physiologically based pharmacokinetic model was developed to describe the in vivo unbound brain-to-plasma concentration ratio as a function of efflux activity measured in vitro. In the present work, the predictive utility of this framework was examined through application to in vitro and in vivo data generated on 133 unique compounds across three preclinical species. Two approaches were examined for the scaling of efflux activity to in vivo, namely relative expression as determined by independent proteomics measurements and relative activity as determined via fitting the in vivo neuropharmacokinetic data. The results with both approaches indicate that in vitro efflux data can be used to accurately predict the degree of brain penetration across species within the context of the proposed physiologically based pharmacokinetic framework.

Published

2018

4. Development of a new permeability assay using low‐efflux MDCKII cells

Author

Hui Zhang, Russ Smith, Caroline A. Lee, Manthena V.S. Varma, Matthew D. Troutman, Charles J. Rotter, James Federico, Theodore E. Liston, Sarah Kempshall, Katherine S. Fenner, Ralph E. Davidson, Xun Zhang, John P. Umland, Carrie Whitney-Pickett, Li Di, Bo Feng, Yurong Lai, Ayman El-Kattan, Eric L. Reyner, and David F. Gebhard

Subjects

biology, Pharmaceutical Science, ATP-binding cassette transporter, Transporter, Endogeny, Cell Separation, Cell sorting, Flow Cytometry, Real-Time Polymerase Chain Reaction, Permeability, Intestinal absorption, Cell Line, Cell biology, Dogs, Intestinal Absorption, Biochemistry, Tandem Mass Spectrometry, Cell culture, biology.protein, Animals, Humans, ATP Binding Cassette Transporter, Subfamily B, Member 1, Efflux, Chromatography, Liquid, P-glycoprotein

Abstract

Permeability is an important property of drug candidates. The Madin-Darby canine kidney cell line (MDCK) permeability assay is widely used and the primary concern of using MDCK cells is the presence of endogenous transporters of nonhuman origin. The canine P-glycoprotein (Pgp) can interfere with permeability and transporter studies, leading to less reliable data. A new cell line, MDCKII-LE (low efflux), has been developed by selecting a subpopulation of low-efflux cells from MDCKII-WT using an iterative fluorescence-activated cell sorting technique with calcein-AM as a Pgp and efflux substrate. MDCKII-LE cells are a subpopulation of MDCKII cells with over 200-fold lower canine Pgp mRNA level and fivefold lower protein level than MDCKII-WT. MDCKII-LE cells showed less functional efflux activity than MDCKII-WT based on efflux ratios. Notably, MDCKII-MDR1 showed about 1.5-fold decreased expression of endogenous canine Pgp, suggesting that using the net flux ratio might not completely cancel out the background endogenous transporter activities. MDCKII-LE cells offer clear advantages over the MDCKII-WT by providing less efflux transporter background signals and minimizing interference from canine Pgp. The MDCKII-LE apparent permeability values well differentiates compounds from high to medium/low human intestinal absorption and can be used for Biopharmaceutical Classification System. The MDCKII-LE permeability assay (4-in-1 cassette dosing) is high throughput with good precision, reproducibility, robustness, and cost-effective.

Published

2011

5. Species Independence in Brain Tissue Binding Using Brain Homogenates

Author

Matthew D. Troutman, John P. Umland, Li Di, Theodore E. Liston, Dennis O. Scott, Youping Huang, Zhen J Lin, and George Chang

Subjects

Pharmacology, Wistar Han, Strain (chemistry), Guinea Pigs, Central nervous system, Brain, Pharmaceutical Science, Brain tissue, Anatomy, Biology, Molecular biology, Beagle, Rats, Macaca fascicularis, Mice, Dogs, medicine.anatomical_structure, Species Specificity, Hartley Guinea Pig, medicine, Animals, Humans, Statistical analysis, Linear correlation

Abstract

Species independence of brain tissue binding was assessed with a large number of structurally diverse compounds using equilibrium dialysis with brain homogenates of seven species and strains (Wistar Han rat, Sprague-Dawley rat, CD-1 mouse, Hartley guinea pig, beagle dog, cynomolgus monkey, and human). The results showed that the fractions unbound of the seven species and strains were strongly correlated with correlation coefficients ranging from 0.93 to 0.99. The cross-species/strain correlations were not significantly different from the interassay correlation with the same species. The linear correlation between Wistar Han and other species had a slope close to 1 and an intercept near 0. Based on orthogonal statistical analysis, no correction is needed for extrapolation of fraction unbound from Wistar Han rat to the other species or strains. Hence, brain tissue binding of Wistar Han rat can be used to obtain binding of other species and strains in drug discovery.

Published

2011

6. A new chemical tool for exploring the role of the PDE4D isozyme in leukocyte function

Author

John B. Cheng, Ajith V. Kamath, Douglas A. Fisher, Kelvin Lam, R. J. Chambers, Joann D. Pillar, Tessa A. Castleberry, Kristin Abrams, David Nettleton, John P. Umland, J.T. Shirley, C R Turner, Anthony Marfat, Alissa L. Sheils, and E. D. Salter

Subjects

Niacinamide, Phosphodiesterase Inhibitors, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Isozyme, chemistry.chemical_compound, Drug Discovery, Leukocytes, medicine, Molecular Biology, Rolipram, chemistry.chemical_classification, Nicotinamide, Chemotaxis, Organic Chemistry, respiratory system, Eosinophil, Cyclic Nucleotide Phosphodiesterases, Type 4, Eosinophils, Isoenzymes, Enzyme, medicine.anatomical_structure, chemistry, Mechanism of action, 3',5'-Cyclic-AMP Phosphodiesterases, Molecular Medicine, medicine.symptom, Function (biology), medicine.drug

Abstract

Nicotinamide (2) is a potent and selective inhibitor of the PDE4D isozyme and as a chemical tool selectively blocks eosinophil mediator release and chemotaxis thus linking the role of PDE4D to eosinophil function.

Published

2006

7. Characterization of chemokine CCR3 agonist-mediated eosinophil recruitment in the Brown-Norway rat

Author

Kudlacz Elizabeth M, Catharine J. Andresen, Carrie A Whitney, John P. Umland, and John B. Cheng

Subjects

Pharmacology, Eotaxin, medicine.medical_specialty, Eosinophil cationic protein, Chemokine, biology, CCR3, respiratory system, Eosinophil, Cell aggregation, Endocrinology, medicine.anatomical_structure, Internal medicine, medicine, biology.protein, Major basic protein, Eosinophilia, medicine.symptom

Abstract

The ability of various C-C chemokines to elicit tissue eosinophil infiltration following intradermal injection or peripheral blood eosinophilia following intravenous injection were compared in the Brown-Norway rat. Eotaxin (0.1–3 μg site−1) of human and murine origin produced equivalent, dose-dependent increases in eosinophil peroxidase activity in rat dermis 4 h post-injection. Human eotaxin-2 was equipotent with human eotaxin in terms of dermal eosinophil recruitment. Other human CCR3 agonists, such as MCP-3, RANTES and MCP-4 failed to increase dermal eosinophil peroxidase activity at doses up to 1 μg site−1 whereas the latter did produce a small effect at 3 μg site−1. Consistent with observations in vivo, human eotaxin displaced [125I]-eotaxin from rat spleen membranes more potently (IC50=2 nM) than did MCP-4 (IC50=500 nM). RANTES did not compete with the radiolabelled chemokine at concentrations up to 1 μM. Human eotaxin (5 μg) administered intravenously increased circulating eosinophils ∼3 fold whereas MCP-4 (5 μg, i.v.) increased circulating monocytes ∼3 fold without affecting eosinophil numbers. Dexamethasone pretreatment inhibited eotaxin-induced dermal eosinophil influx only at a steroid dose (0.1 mg kg−1, s.c.) which significantly reduced circulating eosinophil numbers. The steroid also reduced eosinophilia in peripheral blood resulting from systemic eotaxin administration (5 μg, i.v.). These data suggest differences in rat CCR3 relative to other species as surmised from a distinctive rank order of chemokine potency. In addition to its chemotactic effects eotaxin, but not MCP-4, promotes eosinophil recruitment into the circulation. One of the mechanisms by which glucocorticoids, such as dexamethasone, acutely inhibits eotaxin-induced dermal eosinophil influx is to diminish the circulating numbers of these cells available for tissue recruitment. British Journal of Pharmacology (1999) 128, 788–794; doi:10.1038/sj.bjp.0702835

Published

1999

8. Discovery of micromolar PDE IV inhibitors that exhibit much reduced affinity for the [3H]rolipram binding site: 3-norbornyloxy-4-methoxyphenylmethylene oxindoles

Author

John P. Umland, Anthony Marfat, James F. Eggier, Sally C. Marshall, J.T. Shirley, Enrique Vazquez, Kelvin Cooper, Jeanene E. Tickner, Hiroko Masamune, and John B. Cheng

Subjects

Stereochemistry, Chemistry, Structural similarity, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Phosphodiesterase, Biochemistry, In vitro, Drug Discovery, medicine, Molecular Medicine, Binding site, Molecular Biology, Rolipram, medicine.drug

Abstract

The synthesis and the in vitro properties of a novel series of potent and selective phosphodiesterase type IV (PDE IV) inhibitors is described. Despite bearing structural similarity to rolipram, several of these compounds have much reduced affinity for the [3H]rolipram binding site.

Published

1995

9. Synthesis and in vitro profile of a novel series of catechol benzimidazoles. The discovery of potent, selective phosphodiesterase type IV inhibitors with greatly attenuated affinity for the [3H]rolipram binding site

Author

Kelvin Cooper, Anthony Marfat, Jeenene E. Tickner, James F. Eggler, Hiroko Masamune, Allen J. Duplantier, Sally C. Marshall, John B. Cheng, Kenneth G. Kraus, John P. Umland, and J.T. Shirley

Subjects

Catechol, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Phosphodiesterase, Inhibitory postsynaptic potential, Biochemistry, In vitro, chemistry.chemical_compound, chemistry, Biological property, Drug Discovery, medicine, Molecular Medicine, heterocyclic compounds, sense organs, Binding site, Molecular Biology, Rolipram, medicine.drug

Abstract

The synthesis and biological properties of a novel series of potent and selective phosphodiesterase type IV (PDE IV) inhibitors are described. These catechol benzimidazoles were designed from rolipram and initial compounds reflected a similarly high affinity for the [ 3 H]rolipram b binding site (500 to 1000X greater affinity for the [ 3 H]rolipram binding site over the PDE IV inhibitory site). However, SAR studies on the 3-alkoxy position revealed that this [ 3 H]rolipram binding site affinity could be attenuated, while potentiating the PDE IV inhibitory activity. This resulted in the 2-indanyl analog 13 which is a potent, selective PDE IV inhibitor with a 15X differential in favor of PDE IV binding.

Published

1995

10. Development of a high-speed, multiplexed sample-delivery instrument for LC-MS/MS bioanalysis

Author

Matthew D. Troutman, John P. Umland, Mary Piotrowski, Veronica Zelesky, Kevin M. Whalen, Jason Gobey, James Federico, Hui Zhang, Theodore E. Liston, Brendon Kapinos, Carrie Funk, Walter Mitchell, Mike West, John S. Janiszewski, and Richard P. Schneider

Subjects

Bioanalysis, Instrument control, business.industry, Computer science, Clinical Biochemistry, Sample (statistics), Nanotechnology, General Medicine, Multiplexing, Mass Spectrometry, Analytical Chemistry, High-Throughput Screening Assays, Medical Laboratory Technology, Software, Pharmaceutical Preparations, Lc ms ms, Drug Interactions, Delivery system, General Pharmacology, Toxicology and Pharmaceutics, business, Computer hardware, Chromatography, High Pressure Liquid

Abstract

Background: The number of new chemical entities and types of in vitro and in vivo samples that require bioanalysis in drug discovery is large and diverse. In addition, method development time is limited as data turnaround is the highest priority. These circumstances require that a well-defined set of bioanalysis options be available in short timeframes to triage samples for analysis. Method: The Apricot Designs Dual Arm (ADDA) instrument is an LC–MS/MS sample delivery system that features a flexible hardware design coupled with software automation to enhance throughput in LC–MS/MS bioanalysis drug discovery. The instrument can perform high-throughput LC–MS/MS (8–10 s/sample) for screening and in vitro bioanalysis, as well as multiplexed LC for traditional gradient or isocratic LC approaches. The instrument control software is designed to integrate with DiscoveryQuant™ software (AB Sciex) and a global database of MS/MS conditions. Conclusion: Development of the sample delivery platform and its application in high-throughput and gradient LC will be described.

Published

2012

11. Impact of recovery on fraction unbound using equilibrium dialysis

Author

Tristan S. Maurer, Li Di, John P. Umland, and Patrick Trapa

Subjects

Nonspecific binding, Chromatography, Chemistry, Pharmaceutical Science, Brain, Fraction (chemistry), Blood Proteins, Models, Biological, Rats, Pharmaceutical Preparations, Tissue binding, Drug Discovery, Animals, Humans, Equilibrium dialysis, Computer Simulation, Solubility, Rats, Wistar, Dialysis (biochemistry), Dialysis, Protein Binding

Abstract

Historically, recovery had been used to evaluate the data quality of plasma protein binding or tissue binding obtained from equilibrium dialysis assays. Low recovery was often indicative of high nonspecific binding, instability, or low solubility. This study showed that, when equilibrium was fully established in the dialysis assay, low recovery due to nonspecific binding had no impact on the determination of fraction unbound. The conclusion was supported by the principles of the equilibrium dialysis assay, experimental data, and mathematic simulations. The results suggested that the use of recovery as an acceptance criterion for the equilibrium dialysis assay in drug discovery was too restrictive, and introduced the additional burden of repeating studies unnecessarily.

Published

2011

12. Pharmacokinetic-pharmacodynamic modelling of the effect of Moxifloxacin on QTc prolongation in telemetered cynomolgus monkeys

Author

Xian Chen, Bernard Fermini, William P. Gorczyca, Sunny Z. Sun, Mark Holbrook, Ying Zhang, Piet H. van der Graaf, John P. Umland, and Kenny J. Watson

Subjects

ERG1 Potassium Channel, Patch-Clamp Techniques, hERG, Moxifloxacin, Action Potentials, Administration, Oral, Dofetilide, Torsades de pointes, Pharmacology, Toxicology, Transfection, QT interval, Cell Line, Electrocardiography, In vivo, Oral administration, medicine, Animals, Humans, Telemetry, Aza Compounds, biology, business.industry, Blood Proteins, medicine.disease, Ether-A-Go-Go Potassium Channels, Blockade, Disease Models, Animal, Long QT Syndrome, Macaca fascicularis, biology.protein, Quinolines, business, medicine.drug, Fluoroquinolones, Protein Binding

Abstract

Introduction Delayed ventricular repolarisation is manifested electrocardiographically in a prolongation of the QT interval. Such prolongation can lead to potentially fatal Torsades de Pointes. Moxifloxacin is a fluoroquinolone antibiotic which has been associated with QT prolongation and, as a result, is recommended by the regulatory authorities as a positive control in thorough QT studies performed to evaluate the potential of new chemical entities to induce QT prolongation in humans. The sensitivity of the cynomolgus monkey as a quantitative preclinical predictor of the PK–QT c relationship is discussed. Methods Cardiovascular monitoring was performed in the telemetered cynomolgus monkey for 22 h following oral administration of Moxifloxacin (10, 30 and 90 mg/kg) or placebo. QT c was derived using an individual animal correction factor (ICAF): RR-I = QT-I − (RR-550) ⁎ (IACF). A PKPD analysis was performed to quantify the increase in placebo-adjusted QT c elicited by administration of Moxifloxacin. In addition, the rate of onset of hERG channel blockade of Moxifloxacin was compared to Dofetilide by whole cell patch clamp technique in HEK-293 cells stably expressing the hERG channels. Results Moxifloxacin induced a dose dependent increase in QT c . A maximum increase of 28 ms was observed following administration of 90 mg/kg Moxifloxacin. The corresponding maximum free systemic exposure was 18 μM. Interrogation of the PK–QT c relationship indicated a direct relationship between the systemic exposure of Moxifloxacin and increased QT c . A linear PKPD model was found to describe this relationship whereby a 1.5 ms increase in QT c was observed for every 1 μM increase in free systemic exposure. Discussion The exposure dependent increases in QT c observed following oral administration of Moxifloxacin to the cynomolgus monkey are in close agreement with those previously reported in human subjects. A direct effect linear relationship was found to be conserved in both species. As a result of the quantitative agreement in both species, the utility of the telemetered cynomolgus monkey as a preclinical predictor of QT c prolongation is exemplified. Furthermore, the rate of onset of hERG channel blockade observed in patch clamp offers a mechanistic insight into the relative rates of channel blockade observed in vivo with both Moxifloxacin and Dofetilide.

Published

2010

13. ChemInform Abstract: Biarylcarboxamide Inhibitors of Phosphodiesterase IV and Tumor Necrosis Factor-α

Author

E. R. Pettipher, Allen J. Duplantier, K. L. Johnson, Kenneth G. Kraus, R. J. Chambers, T. A. Hibbs, John B. Cheng, Anthony Marfat, E. D. Salter, John P. Umland, T. H. Jenkinson, J.T. Shirley, V. L. Cohan, and David B. Damon

Subjects

Phosphodiesterase IV, chemistry.chemical_compound, Mediator, chemistry, Rheumatoid arthritis, medicine, Cyclic adenosine monophosphate, Tumor necrosis factor alpha, General Medicine, Pharmacology, medicine.disease, Tumor necrosis factor α, Intracellular

Abstract

Tumor necrosis factor-α (TNF-α) has been implicated as a key mediator in the progression of rheumatoid arthritis. Inhibitors of phosphodiesterase IV (PDE IV) have been shown to inhibit the production of TNF-α by elevating intracellular levels of cyclic adenosine monophosphate (cAMP). Our efforts in a series of biarylcarboxamides have led to the identification of 8j (CP-353,164) as a potent inhibitor of PDE IV and TNF-α production.

Published

2010

14. Strategic Use of Plasma and Microsome Binding To Exploit in Vitro Clearance in Early Drug Discovery

Author

Stefanus J. Steyn, John P. Umland, Dennis O. Scott, and George Chang

Subjects

Nonspecific binding, End point, Chemistry, Drug discovery, Organic Chemistry, Drug Discovery, Microsome, Context (language use), Metabolic stability, Pharmacology, Biochemistry, In vitro, ADME

Abstract

Apparent intrinsic clearance (CLia) determined from microsomal stability assays is a cornerstone in drug discovery. Categorical bins are routinely applied to this end point to facilitate analysis. However, such bins ignore the interdependent nature of apparent intrinsic microsome clearance on several ADME parameters. Considering CLia as a determinant for both metabolic stability and potential dose is more appropriate. In this context with proper accounting for nonspecific binding to microsomes and plasma, consideration of compounds with higher CLia may be warranted. The underlying benefit is the potential increase in the number of hits or chemical diversity for evaluation during the early stages of programs.

Published

2010

15. High throughput ADME screening: practical considerations, impact on the portfolio and enabler of in silico ADME models

Author

Mark J. Cole, John P. Umland, Matt D. Troutman, Mike West, Veronica Zelesky, Kevin M. Whalen, Cornelis E.C.A. Hop, Kelly Jenkins, Suzanne Krueger, John R. Soglia, Walter Mitchell, Stefan J. Steyn, Theodore E. Liston, Ralph E. Davidson, John S. Janiszewski, James Federico, Rebecca Lebowitz, David B. Duignan, Mark Snyder, Sabrina X. Zhao, and Christine Taylor

Subjects

Pharmacology, Quality Control, Drug-Related Side Effects and Adverse Reactions, Chemistry, Drug discovery, In silico, Clinical Biochemistry, Drug Evaluation, Preclinical, Computational biology, Combinatorial chemistry, Pharmaceutical Preparations, Animals, Humans, Computer Simulation, Pharmacokinetics, Throughput (business), ADME

Abstract

Evaluation and optimization of drug metabolism and pharmacokinetic data plays an important role in drug discovery and development and several reliable in vitro ADME models are available. Recently higher throughput in vitro ADME screening facilities have been established in order to be able to evaluate an appreciable fraction of synthesized compounds. The ADME screening process can be dissected in five distinct steps: (1) plate management of compounds in need of in vitro ADME data, (2) optimization of the MS/MS method for the compounds, (3) in vitro ADME experiments and sample clean up, (4) collection and reduction of the raw LC-MS/MS data and (5) archival of the processed ADME data. All steps will be described in detail and the value of the data on drug discovery projects will be discussed as well. Finally, in vitro ADME screening can generate large quantities of data obtained under identical conditions to allow building of reliable in silico models.

Published

2008

16. Impaired inflammatory and pain responses in mice lacking an inducible prostaglandin E synthase

Author

Karamjeet Pandher, Thomas J. Carty, Per-Johan Jakobsson, Marsha L. Roach, Brian M. Naiman, John D. McNeish, Demetrius Carter, Jeffrey L. Stock, John E. Hambor, Colleen P. Gibbons, Catherine E. Trebino, Sipra Saha, Nathalie A. Thomas, Becky A. Durtschi, Laurent P. Audoly, John P. Umland, Jose R. Perez, Jean Martin Lapointe, and Timothy S. Wachtmann

Subjects

Male, Arthritis, Prostaglandin, Pain, Inflammation, Pharmacology, Prostaglandin E synthase, Dinoprostone, Pathogenesis, Arthritis, Rheumatoid, chemistry.chemical_compound, Mice, Medicine, Animals, Humans, Hypersensitivity, Delayed, Prostaglandin-E Synthases, Mice, Knockout, Multidisciplinary, biology, business.industry, Macrophages, Lipid signaling, medicine.disease, Arthritis, Experimental, Intramolecular Oxidoreductases, chemistry, Mice, Inbred DBA, Rheumatoid arthritis, Immunology, biology.protein, Commentary, lipids (amino acids, peptides, and proteins), Female, medicine.symptom, Inflammation Mediators, business

Abstract

Prostaglandin (PG)E 2 is a potent mediator of pain and inflammation, and high levels of this lipid mediator are observed in numerous disease states. The inhibition of PGE 2 production to control pain and to treat diseases such as rheumatoid arthritis to date has depended on nonsteroidal antiinflammatory agents such as aspirin. However, these agents inhibit the synthesis of all prostanoids. To produce biologically active PGE 2 , PGE synthases catalyze the isomerization of PGH 2 into PGE 2 . Recently, several PGE synthases have been identified and cloned, but their role in inflammation is not clear. To study the physiological role of the individual PGE synthases, we have generated by targeted homologous recombination a mouse line deficient in microsomal PGE synthase 1 (mPGES1) on the inbred DBA/1lacJ background. mPGES1-deficient (mPGES1 -/- ) mice are viable and fertile and develop normally compared with wild-type controls. However, mPGES1 -/- mice displayed a marked reduction in inflammatory responses compared with mPGES1 +/+ mice in multiple assays. Here, we identify mPGES1 as the PGE synthase that contributes to the pathogenesis of collagen-induced arthritis, a disease model of human rheumatoid arthritis. We also show that mPGES1 is responsible for the production of PGE 2 that mediates acute pain during an inflammatory response. These findings suggest that mPGES1 provides a target for the treatment of inflammatory diseases and pain associated with inflammatory states.

Published

2003

17. Biarylcarboxylic acids and -amides: inhibition of phosphodiesterase type IV versus [3H]rolipram binding activity and their relationship to emetic behavior in the ferret

Author

R. J. Chambers, Hiroko Masamune, David B. Damon, John W. Watson, J.T. Shirley, M. S. Biggers, Kelvin Cooper, Anthony Marfat, James F. Eggler, J.S. Pillar, John B. Cheng, John P. Umland, Kenneth G. Kraus, and Allen J. Duplantier

Subjects

Phosphodiesterase Inhibitors, Vomiting, Allosteric regulation, Guinea Pigs, Pharmacology, Benzoates, Mice, Structure-Activity Relationship, Drug Discovery, medicine, Potency, Structure–activity relationship, Animals, Humans, Binding site, IC50, Rolipram, Binding Sites, biology, Chemistry, Phosphoric Diester Hydrolases, Ferrets, Brain, Smooth muscle contraction, Pyrrolidinones, Cyclic Nucleotide Phosphodiesterases, Type 4, Biochemistry, Enzyme inhibitor, 3',5'-Cyclic-AMP Phosphodiesterases, biology.protein, Molecular Medicine, medicine.drug

Abstract

In addition to having desirable inhibitory effects on inflammation, anaphylaxis, and smooth muscle contraction, PDE-IV inhibitors also produce undesirable side effects including nausea and vomiting. In general, compounds that inhibit PDE-IV also potently displace [3H]rolipram from a high-affinity binding site in rat cortex. While this binding site has not been identified, it has been proposed to be an allosteric binding site on the PDE-IV enzyme. Preliminary studies have suggested that the emetic potency of PDE-IV inhibitors is correlated with affinity for the brain rolipram binding site rather than potency at inhibiting PDE-IV enzyme activity. Efforts to eliminate the emetic potential of PDE-IV inhibitors were directed toward developing compounds with decreased [3H]rolipram binding affinity while retaining PDE-IV potency. Thus, a novel series of 4-(3-alkoxy-4-methoxyphenyl)benzoic acids and their corresponding carboxamides were prepared and evaluated for their PDE-IV inhibitory and rolipram binding site properties. Modification of the catechol ether moiety led to phenylbutoxy and phenylpentoxy analogues that provided the desired activity profile. Specifically, 4-[3-(5-phenylpentoxy)-4-methoxyphenyl]-2-methylbenzoic acid, 18, was found to exhibit potent PDE-IV inhibitory activity (IC50 0.41 microM) and possessed 400 times weaker activity than rolipram for the [3H]rolipram binding site. In vivo, compound 18 was efficacious in the guinea pig aerosolized antigen induced airway obstruction assay (ED50 8.8 mg/kg, po) and demonstrated a significant reduction in emetic side effects (ferret, 20% emesis at 30 mg/kg, po).

Published

1996