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1. Safety, tolerability, and pharmacokinetics of single‐ and multiple‐dose administration of islatravir (MK‐8591) in adults without HIV

Author

Randolph P. Matthews, Wendy Ankrom, Evan Friedman, Deanne Jackson Rudd, Yang Liu, Robin Mogg, Deborah Panebianco, Inge De Lepeleire, Magdalena Petkova, Jay A. Grobler, Selwyn Aubrey Stoch, and Marian Iwamoto

Subjects
Therapeutics. Pharmacology, RM1-950, Public aspects of medicine, RA1-1270
Abstract

Abstract Islatravir (MK‐8591) is a nucleoside analogue in development for the treatment and prevention of HIV‐1. Two phase 1 trials were conducted during initial evaluation of islatravir: rising single doses (Study 1) and rising multiple doses (Study 2) of oral islatravir in male and female participants without HIV (aged 18–60 years). Safety, tolerability, and pharmacokinetics of islatravir (plasma) and islatravir‐triphosphate (peripheral blood mononuclear cells) were assessed. In Study 1, 24 participants, assigned to 1 of 3 panels, received alternating single doses of islatravir in a fasted state from 5 mg to 400 mg, or placebo, over 3 dosing periods; a 30 mg dose was additionally assessed following a high‐fat meal. In Study 2, 8 participants per dose received 3 once‐weekly doses of 10, 30, or 100 mg islatravir or placebo in a fasted state. For each panel in both trials, 6 participants received active drug and 2 received placebo. Islatravir was generally well‐tolerated, with no serious adverse events or discontinuations due to adverse events. Islatravir was rapidly absorbed (median time to maximum plasma concentration 0.5 hours); plasma half‐life was 49–61 h; intracellular islatravir‐triphosphate half‐life was 118–171 h. Plasma exposure increased in an approximately dose‐proportional manner; there was no meaningful food effect. There was a modest degree of intracellular islatravir‐triphosphate accumulation after multiple weekly dosing. After single oral doses of islatravir greater than or equal to 5 mg, intracellular islatravir‐triphosphate levels were comparable to levels associated with efficacy in preclinical studies. These results warrant continued clinical investigation of islatravir.

Published
2021
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4. Safety and Pharmacokinetics of Islatravir in Individuals with Severe Renal Insufficiency

Author

Randolph P. Matthews, Youfang Cao, Munjal Patel, Vanessa L. Weissler, Arinjita Bhattacharyya, Inge De Lepeleire, Stefanie Last, Juan C. Rondon, Ryan Vargo, S. Aubrey Stoch, and Marian Iwamoto

Subjects
Pharmacology, Infectious Diseases, Deoxyadenosines, Area Under Curve, Leukocytes, Mononuclear, Humans, Reverse Transcriptase Inhibitors, Pharmacology (medical), Renal Insufficiency, Kidney
Abstract

Islatravir (MK-8591) is a high-potency reverse transcriptase translocation inhibitor in development for the treatment of HIV-1 infection. Data from preclinical and clinical studies suggest that ~30% to 60% of islatravir is excreted renally and that islatravir is not a substrate of renal transporters. To assess the impact of renal impairment on the pharmacokinetics of islatravir, an open-label phase 1 trial was conducted with individuals with severe renal insufficiency (RI). A single dose of islatravir 60 mg was administered orally to individuals with severe RI (estimated glomerular filtration rate [eGFR]30 mL/min/1.73 m

Published
2022

5. Single Oral Doses of MK-8507, a Novel Non-Nucleoside Reverse Transcriptase Inhibitor, Suppress HIV-1 RNA for a Week

Author

Martin Daumer, Wendy Ankrom, Deanne Jackson Rudd, Yang Liu, Dirk Schürmann, Jörg Hofmann, Marian Iwamoto, Inge De Lepeleire, Christian Keicher, Evan J. Friedman, Martine Robberechts, Andrea K. Schaeffer, S. Aubrey Stoch, Jay A. Grobler, Bhargava Kandala, and Saijuan Zhang

Subjects
Adult, Combination therapy, Adolescent, Anti-HIV Agents, antiretroviral, HIV Infections, Pharmacology, HIV-1 infection, MK-8507, Nucleoside Reverse Transcriptase Inhibitor, Young Adult, Pharmacokinetics, medicine, Potency, Humans, Pharmacology (medical), Reverse-transcriptase inhibitor, business.industry, treatment-naive, Clinical Science, Middle Aged, Viral Load, pharmacokinetics and pharmacodynamics, Reverse transcriptase, CD4 Lymphocyte Count, Regimen, Infectious Diseases, Tolerability, phase 1, HIV-1, RNA, RNA, Viral, Reverse Transcriptase Inhibitors, business, medicine.drug
Abstract

Background MK-8507 is a novel HIV-1 non-nucleoside reverse transcriptase inhibitor being developed for treatment of HIV-1 infection. MK-8507 has high antiviral potency in vitro and pharmacokinetic (PK) properties that support once-weekly dosing. Setting A phase 1, open-label, proof-of-concept study was conducted in treatment-naive adults with HIV-1 infection to assess monotherapy antiviral activity. Methods In 3 sequential panels, participants aged 18-60 years with baseline plasma HIV-1 RNA ≥10,000 copies/mL and CD4+ T-cell count >200/mm3 received a single oral dose of 40, 80, or 600 mg MK-8507 in the fasted state. Participants were assessed for HIV-1 RNA for at least 7 days, PK for 14 days, and safety and tolerability for 21 days post dose. Results A total of 18 participants were enrolled (6 per panel). The mean 7-day post-dose HIV-1 RNA reduction ranged from ∼1.2 to ∼1.5 log10 copies/mL across the doses assessed. One patient had a viral rebound associated with emergence of a F227C reverse transcriptase variant (per chain-termination method sequencing) 14 days post dose; this variant was found in a second participant by ultra-deep sequencing as an emerging minority variant. MK-8507 PK were generally dose-proportional and similar to observations in participants without HIV-1 infection in prior studies; mean MK-8507 half-life was 56-69 hours in this study. MK-8507 was generally well tolerated at all doses. Conclusions The robust antiviral activity, PK, and tolerability of MK-8507 support its continued development as part of a complete once-weekly oral regimen for HIV-1 treatment; combination therapy could mitigate the emergence of resistance-associated variants.

Published
2021

6. The PET tracer [

Author

Wenping, Li, Yuchuan, Wang, Talakad G, Lohith, Zhizhen, Zeng, Ling, Tong, Robert, Mazzola, Kerry, Riffel, Patricia, Miller, Mona, Purcell, Marie, Holahan, Hyking, Haley, Liza, Gantert, David, Hesk, Sumei, Ren, John, Morrow, Jason, Uslaner, Arie, Struyk, Jenny Miu-Chun, Wai, Michael T, Rudd, David M, Tellers, Thomas, McAvoy, Guy, Bormans, Michel, Koole, Koen, Van Laere, Kim, Serdons, Jan, de Hoon, Ruben, Declercq, Inge, De Lepeleire, Maria B, Pascual, Paolo, Zanotti-Fregonara, Meixiang, Yu, Victoria, Arbones, Joseph C, Masdeu, Amy, Cheng, Azher, Hussain, Tjerk, Bueters, Matt S, Anderson, Eric D, Hostetler, and Anthony S, Basile

Subjects
Alzheimer Disease, Positron-Emission Tomography, Acetylcholinesterase, Animals, Humans, Macaca mulatta, Receptors, Muscarinic
Abstract

Positron emission tomography (PET) ligands play an important role in the development of therapeutics by serving as target engagement or pharmacodynamic biomarkers. Here, we describe the discovery and translation of the PET tracer [

Published
2022

7. The PET tracer [C-11]MK-6884 quantifies M4 muscarinic receptor in rhesus monkeys and patients with Alzheimer's disease

Author

Wenping Li, Yuchuan Wang, Talakad G. Lohith, Zhizhen Zeng, Ling Tong, Robert Mazzola, Kerry Riffel, Patricia Miller, Mona Purcell, Marie Holahan, Hyking Haley, Liza Gantert, David Hesk, Sumei Ren, John Morrow, Jason Uslaner, Arie Struyk, Jenny Miu-Chun Wai, Michael T. Rudd, David M. Tellers, Thomas McAvoy, Guy Bormans, Michel Koole, Koen Van Laere, Kim Serdons, Jan de Hoon, Ruben Declercq, Inge De Lepeleire, Maria B. Pascual, Paolo Zanotti-Fregonara, Meixiang Yu, Victoria Arbones, Joseph C. Masdeu, Amy Cheng, Azher Hussain, Tjerk Bueters, Matt S. Anderson, Eric D. Hostetler, and Anthony S. Basile

Subjects
General Medicine
Abstract

Positron emission tomography (PET) ligands play an important role in the development of therapeutics by serving as target engagement or pharmacodynamic biomarkers. Here, we describe the discovery and translation of the PET tracer [11C]MK-6884 from rhesus monkeys to patients with Alzheimer’s disease (AD). [3H]MK-6884/[11C]MK-6884 binds with high binding affinity and good selectivity to an allosteric site on M4 muscarinic cholinergic receptors (M4Rs) in vitro and shows a regional distribution in the brain consistent with M4R localization in vivo. The tracer demonstrates target engagement of positive allosteric modulators of the M4R (M4 PAMs) through competitive binding interactions. [11C]MK-6884 binding is enhanced in vitro by the orthosteric M4R agonist carbachol and indirectly in vivo by the acetylcholinesterase inhibitor donepezil in rhesus monkeys and healthy volunteers, consistent with its pharmacology as a highly cooperative M4 PAM. PET imaging of [11C]MK-6884 in patients with AD identified substantial regional differences quantified as nondisplaceable binding potential (BPND) of [11C]MK-6884. These results suggest that [11C]MK-6884 is a useful target engagement biomarker for M4 PAMs but may also act as a sensitive probe of neuropathological changes in the brains of patients with AD. ispartof: SCIENCE TRANSLATIONAL MEDICINE vol:14 issue:627 ispartof: location:United States status: published

Published
2022

9. Safety, tolerability, and pharmacokinetics of single- and multiple-dose administration of islatravir (MK-8591) in adults without HIV

Author

Deborah Panebianco, Magdalena Petkova, Deanne Jackson Rudd, Robin Mogg, Inge De Lepeleire, Jay A. Grobler, Evan J. Friedman, Wendy Ankrom, Selwyn Aubrey Stoch, Marian Iwamoto, Randolph P. Matthews, and Yang Liu

Subjects
Drug, Adult, Male, Adolescent, Anti-HIV Agents, media_common.quotation_subject, Administration, Oral, RM1-950, Pharmacology, Placebo, General Biochemistry, Genetics and Molecular Biology, Article, Young Adult, Pharmacokinetics, Double-Blind Method, Medicine, Humans, Dosing, General Pharmacology, Toxicology and Pharmaceutics, Adverse effect, media_common, Meal, Nucleoside analogue, Deoxyadenosines, Dose-Response Relationship, Drug, business.industry, General Neuroscience, Research, General Medicine, Articles, Middle Aged, Healthy Volunteers, Tolerability, Leukocytes, Mononuclear, Female, Therapeutics. Pharmacology, Public aspects of medicine, RA1-1270, business, medicine.drug, Half-Life
Abstract

Islatravir (MK‐8591) is a nucleoside analogue in development for the treatment and prevention of HIV‐1. Two phase 1 trials were conducted during initial evaluation of islatravir: rising single doses (Study 1) and rising multiple doses (Study 2) of oral islatravir in male and female participants without HIV (aged 18–60 years). Safety, tolerability, and pharmacokinetics of islatravir (plasma) and islatravir‐triphosphate (peripheral blood mononuclear cells) were assessed. In Study 1, 24 participants, assigned to 1 of 3 panels, received alternating single doses of islatravir in a fasted state from 5 mg to 400 mg, or placebo, over 3 dosing periods; a 30 mg dose was additionally assessed following a high‐fat meal. In Study 2, 8 participants per dose received 3 once‐weekly doses of 10, 30, or 100 mg islatravir or placebo in a fasted state. For each panel in both trials, 6 participants received active drug and 2 received placebo. Islatravir was generally well‐tolerated, with no serious adverse events or discontinuations due to adverse events. Islatravir was rapidly absorbed (median time to maximum plasma concentration 0.5 hours); plasma half‐life was 49–61 h; intracellular islatravir‐triphosphate half‐life was 118–171 h. Plasma exposure increased in an approximately dose‐proportional manner; there was no meaningful food effect. There was a modest degree of intracellular islatravir‐triphosphate accumulation after multiple weekly dosing. After single oral doses of islatravir greater than or equal to 5 mg, intracellular islatravir‐triphosphate levels were comparable to levels associated with efficacy in preclinical studies. These results warrant continued clinical investigation of islatravir.

Published
2021

10. Safety, pharmacokinetics, and antiretroviral activity of islatravir (ISL, MK-8591), a novel nucleoside reverse transcriptase translocation inhibitor, following single-dose administration to treatment-naive adults infected with HIV-1: an open-label, phase 1b, consecutive-panel trial

Author

Inge De Lepeleire, Evan J. Friedman, Marian Iwamoto, Jörg Hofmann, Randolph P. Matthews, Jay A. Grobler, Saijuan Zhang, S. Aubrey Stoch, Deanne Jackson Rudd, Christian Keicher, Dirk Schürmann, Andreas Hüser, and Martine Robberechts

Subjects
Drug, Adult, Male, medicine.medical_specialty, Epidemiology, Anti-HIV Agents, media_common.quotation_subject, Immunology, HIV Infections, Nucleoside Reverse Transcriptase Inhibitor, Young Adult, Pharmacokinetics, Virology, Internal medicine, medicine, Humans, Dosing, Adverse effect, media_common, Deoxyadenosines, business.industry, Middle Aged, Reverse transcriptase, Infectious Diseases, Tolerability, HIV-1, Reverse Transcriptase Inhibitors, Female, business, Nucleoside
Abstract

Summary Background Islatravir (also known as ISL and MK-8591) is a unique nucleoside reverse transcriptase translocation inhibitor in clinical development for treatment of people with HIV-1 infection. In preclinical studies, intracellular islatravir-triphosphate exhibits a long half-life and prolonged virological effects. In this study, we aimed to assess islatravir safety, pharmacokinetics, and antiretroviral activity in treatment-naive adults with HIV-1 infection. Methods This open-label, consecutive-panel, phase 1b trial was done at Charite Research Organisation (Berlin, Germany) and included men and women (aged 18–60 years, inclusive) with HIV-1 infection who were ART naive. Participants were required to have plasma HIV-1 RNA counts of at least 10 000 copies per mL within 30 days before the trial treatment phase, without evidence of resistance to nucleoside reverse transcriptase inhibitors. Participants were enrolled in one of five consecutive dosing panels, receiving a single oral dose of islatravir (0·5–30 mg). The primary outcomes were safety and tolerability of islatravir and change from baseline in HIV-1 plasma RNA; secondary outcomes were islatravir plasma and islatravir-triphosphate intracellular pharmacokinetics. We obtained descriptive safety and pharmacokinetics statistics, and estimated efficacy results from a longitudinal data analysis model. This study is registered with ClinicalTrials.gov , NCT02217904 , and EudraCT, 2014-002192-28. Findings Between Sept 17, 2015, and May 11, 2017, we enrolled 30 participants (six per panel). Islatravir was generally well tolerated. 27 (90%) participants had 60 adverse events after receipt of drug, of which 21 (35%) were deemed to be drug related. The most common (n>1) drug-related adverse events were headache (in nine [30%] participants) and diarrhoea (in two [7%]). No serious adverse events were reported, and no participants discontinued due to an adverse event. Plasma islatravir pharmacokinetics and intracellular islatravir-triphosphate pharmacokinetics were approximately dose proportional. The islatravir-triphosphate intracellular half-life was 78·5–128·0 h. Least-squares mean HIV-1 RNA at 7 days after dose decreased from 1·67 log10 copies per mL (95% CI 1·42–1·92) at 10 mg dose to 1·20 log10 copies per mL (0·95–1·46) at 0·5 mg dose. No genetic changes consistent with development of viral resistance were detected. Interpretation Single doses of islatravir as low as 0·5 mg significantly suppressed HIV-1 RNA by more than 1·0 log at day 7 in treatment-naive adults with HIV-1 infection and were generally well tolerated, supporting the further development of islatravir as a flexible-dose treatment for individuals with HIV-1 infection. Funding Merck Sharp & Dohme Corp, a subsidiary of Merck & Co Inc, Kenilworth, NJ, USA.

Published
2019

11. Pharmacokinetic Interactions between the Hepatitis C Virus Inhibitors Elbasvir and Grazoprevir and HIV Protease Inhibitors Ritonavir, Atazanavir, Lopinavir, and Darunavir in Healthy Volunteers

Author

Wendy W. Yeh, Iain P. Fraser, Christine Fandozzi, Jennifer Talaty, Anna Mitselos, Marian Iwamoto, Xiaoyan Chu, Monika Martinho, Corinne Vandermeulen, Luzelena Caro, Xiaobi Huang, Zifang Guo, Jean Francois Denef, Katherine Dunnington, William D. Hanley, Deborah Panebianco, Jan de Hoon, Inge De Lepeleire, Joan R. Butterton, Hwa-Ping Feng, Lihong Du, Patricia Jumes, William L. Marshall, and Robert Valesky

Subjects
Cyclopropanes, Male, viruses, HIV Infections, Hepacivirus, Viral Nonstructural Proteins, Pharmacology, Lopinavir, 0302 clinical medicine, immune system diseases, HIV Protease Inhibitor, Drug Interactions, Pharmacology (medical), 030212 general & internal medicine, Darunavir, Sulfonamides, Imidazoles, Intracellular Signaling Peptides and Proteins, virus diseases, Middle Aged, Hepatitis C, Healthy Volunteers, Infectious Diseases, Grazoprevir, Female, 030211 gastroenterology & hepatology, medicine.drug, Adult, Elbasvir, Atazanavir Sulfate, Antiviral Agents, Young Adult, 03 medical and health sciences, Quinoxalines, medicine, Humans, Protease inhibitor (pharmacology), Benzofurans, Ritonavir, business.industry, HIV Protease Inhibitors, biochemical phenomena, metabolism, and nutrition, Amides, Atazanavir, HIV-1, Carbamates, business
Abstract

The combination of the hepatitis C virus (HCV) nonstructural protein 5A (NS5A) inhibitor elbasvir and the NS3/4A protease inhibitor grazoprevir is a potent, once-daily therapy indicated for the treatment of chronic HCV infection in individuals coinfected with human immunodeficiency virus (HIV). We explored the pharmacokinetic interactions of elbasvir and grazoprevir with ritonavir and ritonavir-boosted HIV protease inhibitors in three phase 1 trials. Drug-drug interaction trials with healthy participants were conducted to evaluate the effect of ritonavir on the pharmacokinetics of grazoprevir (n = 10) and the potential two-way pharmacokinetic interactions of elbasvir (n = 30) or grazoprevir (n = 39) when coadministered with ritonavir-boosted atazanavir, lopinavir, or darunavir. Coadministration of ritonavir with grazoprevir increased grazoprevir exposure; the geometric mean ratio (GMR) for grazoprevir plus ritonavir versus grazoprevir alone area under the concentration-time curve from 0 to 24 h (AUC0-24) was 1.91 (90% confidence interval [CI]; 1.31 to 2.79). Grazoprevir exposure was markedly increased with coadministration of atazanavir-ritonavir, lopinavir-ritonavir, and darunavir-ritonavir, with GMRs for grazoprevir AUC0-24 of 10.58 (90% CI, 7.78 to 14.39), 12.86 (90% CI, 10.25 to 16.13), and 7.50 (90% CI, 5.92 to 9.51), respectively. Elbasvir exposure was increased with coadministration of atazanavir-ritonavir, lopinavir-ritonavir, and darunavir-ritonavir, with GMRs for elbasvir AUC0-24 of 4.76 (90% CI, 4.07 to 5.56), 3.71 (90% CI, 3.05 to 4.53), and 1.66 (90% CI, 1.35 to 2.05), respectively. Grazoprevir and elbasvir had little effect on atazanavir, lopinavir, and darunavir pharmacokinetics. Coadministration of elbasvir-grazoprevir with atazanavir-ritonavir, lopinavir-ritonavir, or darunavir-ritonavir is contraindicated, owing to an increase in grazoprevir exposure. Therefore, HIV treatment regimens without HIV protease inhibitors should be considered for HCV/HIV-coinfected individuals who are being treated with elbasvir-grazoprevir. ispartof: ANTIMICROBIAL AGENTS AND CHEMOTHERAPY vol:63 issue:4 ispartof: location:United States status: published

Published
2019

12. IL-17-high asthma with features of a psoriasis immunophenotype

Author

Jörgen Östling, Marleen van Geest, James P.R. Schofield, Zala Jevnikar, Susan Wilson, Jonathan Ward, Rene Lutter, Dominick E. Shaw, Per S. Bakke, Massimo Caruso, Sven-Erik Dahlen, Stephen J. Fowler, Ildikó Horváth, Norbert Krug, Paolo Montuschi, Marek Sanak, Thomas Sandström, Kai Sun, Ioannis Pandis, Charles Auffray, Ana R. Sousa, Yike Guo, Ian M. Adcock, Peter Howarth, Kian Fan Chung, Jeanette Bigler, Peter J. Sterk, Paul J. Skipp, Ratko Djukanović, Outi Vaarala, I.M. Adcock, H. Ahmed, C. Auffray, P. Bakke, A.T. Bansal, F. Baribaud, S. Bates, E.H. Bel, J. Bigler, H. Bisgaard, M.J. Boedigheimer, K. Bønnelykke, J. Brandsma, P. Brinkman, E. Bucchioni, D. Burg, A. Bush, M. Caruso, A. Chaiboonchoe, P. Chanez, K.F. Chung, C.H. Compton, J. Corfield, A. D'Amico, S.E. Dahlen, B. De Meulder, R. Djukanovic, V.J. Erpenbeck, D. Erzen, K. Fichtner, N. Fitch, L.J. Fleming, E. Formaggio, S.J. Fowler, U. Frey, M. Gahlemann, T. Geiser, Y. Guo, S. Hashimoto, J. Haughney, G. Hedlin, P.W. Hekking, T. Higenbottam, J.M. Hohlfeld, C. Holweg, I. Horváth, P. Howarth, A.J. James, R. Knowles, A.J. Knox, N. Krug, D. Lefaudeux, M.J. Loza, R. Lutter, A. Manta, S. Masefield, A. Mazein, A. Meiser, R.J.M. Middelveld, M. Miralpeix, P. Montuschi, N. Mores, C.S. Murray, J. Musial, D. Myles, L. Pahus, I. Pandis, S. Pavlidis, P. Powell, G. Praticò, M. Puig N. Rao, J. Riley, A. Roberts, G. Roberts, A. Rowe, T. Sandström, W. Seibold, A. Selby, D.E. Shaw, R. Sigmund, F. Singer, P.J. Skipp, A.R. Sousa, P.J. Sterk, K. Sun, B. Thornton, W.M. van Aalderen, M. van Geest, J. Vestbo, N.H. Vissing, A.H. Wagener, S.S. Wagers, Z. Weiszhart, C.E. Wheelock, S.J. Wilson, Antonios Aliprantis, David Allen, Kjell Alving, P. Badorrek, David Balgoma, S. Ballereau, Clair Barber, Manohara Kanangana Batuwitage, A. Bautmans, A. Bedding, A.F. Behndig, Jorge Beleta, A. Berglind, A. Berton, Grazyna Bochenek, Armin Braun, D. Campagna, Leon Carayannopoulos, C. Casaulta, Romanas Chaleckis, B. Dahlén, imothy Davison, Jorge De Alba, Inge De Lepeleire, Tamara Dekker, Ingrid Delin, P. Dennison, Annemiek Dijkhuis, Paul Dodson, Aleksandra Draper, K. Dyson, Jessica Edwards, L. El Hadjam, Rosalia Emma, Magnus Ericsson, C. Faulenbach, Breda Flood, G. Galffy, Hector Gallart, D. Garissi, J. Gent, M. Gerhardsson de Verdier, D. Gibeon, Cristina Gomez, Kerry Gove, Neil Gozzard, E. Guillmant-Farry, E. Henriksson, Lorraine Hewitt, U. Hoda, Richard Hu, Sile Hu, X. Hu, E. Jeyasingham, K. Johnson, N. Jullian, Juliette Kamphuis, Erika J. Kennington, Dyson Kerry, G. Kerry, M. Klüglich, Hugo Knobel, Johan Kolmert, J.R. Konradsen, Maxim Kots, Kosmas Kretsos, L. Krueger, Scott Kuo, Maciej Kupczyk, Bart Lambrecht, A.-S. Lantz, Christopher Larminie, L.X. Larsson, P. Latzin, N. Lazarinis, N. Lemonnier, Saeeda Lone-Latif, L.A. Lowe, Alexander Manta, Lisa Marouzet, Jane Martin, Caroline Mathon, L. McEvoy, Sally Meah, A. Menzies-Gow, Leanne Metcalf, Maria Mikus, Philip Monk, Shama Naz, K. Nething, Ben Nicholas, U. Nihlén, Peter Nilsson, R. Niven, B. Nordlund, S. Nsubuga, Antonio Pacino, Susanna Palkonen, J. Pellet, Giorgio Pennazza, Anne Petrén, Sandy Pink, C. Pison, Anthony Postle, Malayka Rahman-Amin, Lara Ravanetti, Emma Ray, Stacey Reinke, Leanne Reynolds, K. Riemann, Martine Robberechts, J.P. Rocha, C. Rossios, Kirsty Russell, Michael Rutgers, G. Santini, Marco Santoninco, M. Saqi, Corinna Schoelch, S. Scott, N. Sehgal, Marcus Sjödin, Barbara Smids, Caroline Smith, Jessica Smith, Katherine M. Smith, P. Söderman, A. Sogbessan, F. Spycher, Doroteya Staykova, S. Stephan, J. Stokholm, K. Strandberg, M. Sunther, M. Szentkereszty, L. Tamasi, K. Tariq, John-Olof Thörngren, Jonathan Thorsen, S. Valente, Marianne van de Pol, C.M. van Drunen, Jonathan Van Eyll, Jenny Versnel, Anton Vink, C. von Garnier, A. Vyas, Frans Wald, Samantha Walker, Kristiane Wetzel, Coen Wiegman, Siân Williams, Xian Yang, Elizabeth Yeyasingham, W. Yu Amgen, W. Zetterquist, Z. Zolkipli, A.H. Zwinderman, Publica, Pediatric surgery, Amsterdam Reproduction & Development (AR&D), Pulmonology, AII - Inflammatory diseases, Experimental Immunology, Ear, Nose and Throat, Epidemiology and Data Science, APH - Methodology, and Commission of the European Communities

Subjects
0301 basic medicine, Male, URINARY-EXCRETION, Allergy, Neutrophils, Inflammatory bowel disease, Cohort Studies, DOUBLE-BLIND, 0302 clinical medicine, Immunology and Allergy, POPULATION, Interleukin-13, Interleukin-17, psoriasis, BRODALUMAB, Up-Regulation, IL-17, Phenotype, 1107 Immunology, Biomarker (medicine), Female, Interleukin 17, medicine.symptom, Life Sciences & Biomedicine, ENDOTYPES, Signal Transduction, EXPRESSION, Adult, Settore BIO/14 - FARMACOLOGIA, Immunology, PHENOTYPES, Bronchi, 03 medical and health sciences, INFLAMMATION, Psoriasis, medicine, Humans, Interleukin 8, Asthma, U-BIOPRED Study Group, Science & Technology, business.industry, Gene Expression Profiling, biomarkers, Epithelial Cells, asthma, bronchial brushings, medicine.disease, bronchial biopsies, Neutrophilia, 030104 developmental biology, 030228 respiratory system, EXACERBATION, CELLS, Sputum, business, Transcriptome, Biomarkers
Abstract

Background The role of IL-17 immunity is well established in patients with inflammatory diseases, such as psoriasis and inflammatory bowel disease, but not in asthmatic patients, in whom further study is required. Objective We sought to undertake a deep phenotyping study of asthmatic patients with upregulated IL-17 immunity. Methods Whole-genome transcriptomic analysis was performed by using epithelial brushings, bronchial biopsy specimens (91 asthmatic patients and 46 healthy control subjects), and whole blood samples (n = 498) from the Unbiased Biomarkers for the Prediction of Respiratory Disease Outcomes (U-BIOPRED) cohort. Gene signatures induced in vitro by IL-17 and IL-13 in bronchial epithelial cells were used to identify patients with IL-17–high and IL-13–high asthma phenotypes. Results Twenty-two of 91 patients were identified with IL-17, and 9 patients were identified with IL-13 gene signatures. The patients with IL-17–high asthma were characterized by risk of frequent exacerbations, airway (sputum and mucosal) neutrophilia, decreased lung microbiota diversity, and urinary biomarker evidence of activation of the thromboxane B2 pathway. In pathway analysis the differentially expressed genes in patients with IL-17-high asthma were shared with those reported as altered in psoriasis lesions and included genes regulating epithelial barrier function and defense mechanisms, such as IL1B, IL6, IL8, and β-defensin. Conclusion The IL-17–high asthma phenotype, characterized by bronchial epithelial dysfunction and upregulated antimicrobial and inflammatory response, resembles the immunophenotype of psoriasis, including activation of the thromboxane B2 pathway, which should be considered a biomarker for this phenotype in further studies, including clinical trials targeting IL-17.

Published
2019

13. Rhinovirus challenge in asthmatics and healthy volunteers to evaluate the safety and appropriate dose of a GMP human rhinovirus 16 preparation for challenge studies in mild-moderate asthmatics taking ICS

Author

Norbert Krug, Jens M. Hohlfeld, Antonios Aliprantis, Leonidas Carayannopoulos, An Bautmans, Martine Robberechts, Inge De Lepeleire, Holger Ziehr, Dave Singh, Zuzana Diamant, Shan Yang, Neil Fitch, Bob Thornton, Peter J. Sterk, Rene Lutter And The U-Biopred Study Group, and Publica

Subjects
medicine.medical_specialty, Evening, business.industry, Common cold, medicine.disease, medicine.disease_cause, Gastroenterology, Tolerability, Internal medicine, Healthy volunteers, medicine, Nasal administration, Rhinovirus, business, Morning, Asthma
Abstract

Introduction: Rhinovirus (RV) infection is the most important trigger for asthma exacerbation. However, no GMP grade RV preparation and established protocols are available for human RV challenge studies. Aim: To establish safety and tolerability of a new GMP grade U-BIOPRED human RV16 (RV16UB) and to identify an appropriate dose to study biomarkers in asthmatics following RV challenge. Methods: Study 1: Single doses of 10, 100 and 1000 TCID50 of RV16UB were administered intranasally in healthy subjects (n=18) and 10 and 100 TCID50 in mild-moderate asthmatics on ICS control therapy (n=18), taking LABA and not taking LABA. Study 2: Single doses of 100 TCID50 were given to asthmatics on ICS not taking LABA (n=23) and changes from baseline in lung function, Asthma Control Diary (ACD), Common Cold Symptoms Score (CSS) and FeNO were determined (time weighted average days 1-7; TWA1-7). Results: Study 1: All doses of RV16UB were well tolerated in asthma and controls. A dose of 100 TCID50 induced cold symptoms and detectable viral RNA titers in most asthmatics. Study 2: Following challenge with 100 TCID50 morning and evening TWA1-7 FEV1 were significantly reduced by -1.7% and – 2.1% respectively. Max. FEV1 drop post challenge was 6.8%. TWA1-7 ACD and CSS were significantly increased after challenge (2.7 and 4.0 respectively). No significant changes in FeNO were found. Conclusion: A dose of 100 TCID50 of RV16UB was safe in asthmatics and induced a small, but significant reduction in FEV1 (-2%). Significant increases in ACD and CSS were found. Changes in biomarkers are under investigation.

Published
2018

14. Quantification, Variability, and Reproducibility of Basal Skeletal Muscle Glucose Uptake in Healthy Humans Using 18F-FDG PET/CT

Author

Jan de Hoon, Michael Klimas, Manu Chakravarthy, Christophe Deroose, Ruben Declercq, Inge De Lepeleire, Corinne Vandermeulen, Andrey Postnov, Justin Dennie, Olivier Gheysens, Koen Van Laere, and Lori A. Mixson

Subjects
Adult, Male, Intraclass correlation, Glucose uptake, Coefficient of variation, Insulin resistance, Fluorodeoxyglucose F18, Image Processing, Computer-Assisted, medicine, Humans, Radiology, Nuclear Medicine and imaging, Muscle, Skeletal, Tomography, Emission-Computed, Single-Photon, Reproducibility, business.industry, Reproducibility of Results, Skeletal muscle, Blood flow, medicine.disease, Healthy Volunteers, medicine.anatomical_structure, Basal (medicine), Positron-Emission Tomography, Female, Radiopharmaceuticals, Nuclear medicine, business
Abstract

The quantification and variability of skeletal muscle glucose utilization (SMGU) in healthy subjects under basal (low insulin) conditions are poorly known. This information is essential early in clinical drug development to effectively interrogate novel pharmacologic interventions that modulate glucose uptake. The aim of this study was to determine test–retest characteristics and variability of SMGU within and between healthy subjects under basal conditions. Furthermore, different kinetic modeling strategies were evaluated to find the best-fitting model to assess SMGU studied by 18F-FDG. Methods: Six healthy male volunteers underwent 2 dynamic 18F-FDG PET/CT scans with an interval of 24 h. Subjects were admitted to the clinical unit to minimize variability in daily activities and food intake and restrict physical activity. 18F-FDG PET/CT scans of gluteal and quadriceps muscle area were obtained with arterial input. Regions of interest were drawn over the muscle area to obtain time–activity curves and standardized uptake values (SUVs) between 60 and 90 min. Spectral analysis of the data and kinetic modeling was performed using 2-tissue-irreversible (2T3K), 2-tissue-reversible, and 3-tissue-sequential-irreversible (3T5KS) models. Reproducibility was assessed by intraclass correlation coefficients (ICCs) and within-subject coefficient of variation (WSCV). Results: SUVs in gluteal and quadriceps areas were 0.56 ± 0.09 and 0.64 ± 0.07. ICCs (with 90% confidence intervals in parentheses) were 0.88 (0.64–0.96) and 0.96 (0.82–0.99), respectively, for gluteal and quadriceps muscles, and WSCV for gluteal and quadriceps muscles was 2.2% and 3.6%, respectively. The rate of glucose uptake into muscle was 0.0016 ± 0.0004 mL/mL⋅min, with an ICC of 0.94 (0.93–0.95) and WSCV of 6.6% for the 3T5KS model, whereas an ICC of 0.98 (0.92–1.00) and WSCV of 2.8% was obtained for the 2T3K model. 3T5KS demonstrated the best fit to the measured experimental points. Conclusion: Minimal variability in skeletal muscle glucose uptake was observed under basal conditions in healthy subjects. SUV measurements and rate of glucose uptake values were reproducible, with an average WSCV of less than 5%. Compared with SUV, the 3-tissue model adds information about kinetics between blood, intra- and intercellular compartments, and phosphorylation that may highlight the exact mechanisms of metabolic changes after pharmacologic intervention.

Published
2015

15. Characterizing the PK/PD relationship for inhibition of capsaicin-induced dermal vasodilatation by MK-3207, an oral calcitonin gene related peptide receptor antagonist

Author

Rebecca L. Blanchard, John Palcza, Jan de Hoon, Kristien Van Dyck, Inge De Lepeleire, William S. Denney, Adrianna Gipson, Steve Vermeersch, Tae H. Han, M. Gail Murphy, Chi-Chung Li, William P. Kennedy, and Marleen Depré

Subjects
Pharmacology, medicine.medical_specialty, education.field_of_study, Telcagepant, Chemistry, Population, TRPV1, Antagonist, Calcitonin gene-related peptide, Calcitonin gene-related peptide receptor antagonist, Endocrinology, Internal medicine, medicine, Pharmacology (medical), Receptor, education, PK/PD models
Abstract

Aims Calcitonin gene related peptide (CGRP) receptor antagonists are effective acute migraine treatments. A capsaicin-induced dermal vasodilatation (CIDV) model has been developed to provide target-engagement information in healthy volunteers. In the model, CGRP release is provoked after dermal capsaicin application, by activating transient receptor potential vanilloid-type-1 (TRPV1) receptors at peripheral sensory nerves. Laser Doppler imaging is used to quantify CIDV and subsequent inhibition by CGRP receptor antagonists. We sought to evaluate a CGRP receptor antagonist, MK-3207, in the biomarker model and to assess the predictability of the CIDV response to migraine clinical efficacy. Methods An integrated population pharmacokinetic/pharmacodynamic (PK/PD) model was developed to describe the exposure−response relationship for CIDV inhibition by CGRP and TRPV1 receptor antagonists. MK-3207 dose−response predictions were made based on estimated potency from the PK/PD model and mean plasma concentrations observed at the doses investigated. Results The results suggested that a 20 mg dose of MK-3207 (EC50 of 1.59 nm) would be required to attain the peripheral CIDV response at a target level that was shown previously to correlate with 2 h clinical efficacy based on phase 3 telcagepant clinical data, and that a plateau of the dose−response would be reached around 40–100 mg. These predictions provided a quantitative rationale for dose selection in a phase 2 clinical trial of MK-3207 and helped with interpretation of the efficacy results from the trial. Conclusions The integrated CIDV PK/PD model provides a useful platform for characterization of PK/PD relationships and predictions of dose−response relationships to aid in future development of CGRP and TRPV1 receptor antagonists.

Published
2015

16. U-BIOPRED clinical adult asthma clusters linked to a subset of sputum -omics

Author

Hugo H. Knobel, Koos Zwinderman, Anton Vink, Laurie Pahus, Elisabeth H. Bel, Wim van Aalderenm, Massimo Caruso, Marianne A. van de Pol, Lorraine Hewitt, David Balgoma, Jilaiha Gent, Paul Skipp, Sally Meah, Grazyna Bochenek, Martina Gahlemann, Xugang Hu, Graham Roberts, Stephen J. Fowler, Aleksandra Draper, Jon R Konradsen, Craig E. Wheelock, Philips Monk, Roelinde Middelveld, Päivi Söderman, Stelios Pavlidis, João P. Carvalho da Purfição Rocha, Caroline Smith, Alan J. Knox, Doroteya Staykova, Ildiko Horvath, Nadia Mores, Christophe von Garnier, Frans Wald, Uruj Hoda, Giuseppe Santini, Anne Petrén, Thomas Sandström, Alexander Mazein, Tamara Dekker, Ana R. Sousa, Andrea Maiser, Zsoka Weiszhart, Wolfgang Seibold, Susanna Palkonnen, Johan Kolmert, Cristina Gómez, Marco Sentoninco, Nancy Peffer, Anna James, Ingrid Delin, Montse Miralpeix, Antonios Aliprantis, Annemiek Dijkhuis, Amanda Roberts, Clare S. Murray, Lara Ravanetti, Yike Guo, Jenny Versnel, Richard Hu, Saeeda Lone-Satif, Jonathan Ward, Martine Robberechts, René Lutter, Linn Krueger, Antonio Pacino, Arnaldo D'Amico, Jans Hohlfeld, Scott Wagers, Neil Fitch, Pippa Powel, Matthew J. Loza, Karin Strandberg, Damijan Erzen, H. Ahmed, Per Bakke, Neil Gozzard, David Gibeon, Arianne Wagerner, Kerry Gove, Siân Williams, Ann Berglind, Rosalia Emma, Bob Thornton, Val Hudson, Elizabeth Yeyashingham, John Haughney, Ann-Sofie Lantz, Kjell Alving, Bart N. Lambrecht, Marek Sanak, Lilla Tamasi, Nadja Hawwa Vissing, Katja Nething, Barbro Dahlén, Jacek Musiał, Pim de Boer, Marcus O.D. Sjödin, Sarah Masefield, Marleen van Geest, Maciej Kupczyk, Peter H. Howarth, Alix Berton, Peter J. Sterk, David Myles, Peter Nilsson, Emma Ray, Ian M. Adcock, Pascal Chanez, Christos Rossios, Paolo Montuschi, Inge De Lepeleire, Armin Braun, Juliette Kamphuis, Davide Campagna, Salvatore Valente, Kees van Drunen, Urs Frey, Philipp Badorek, Ralf Sigmund, Malayka Rahman-Amin, Maria Mikus, James P.R. Schofield, Simone Hashimoto, Marton Szentkereszty, Gabriella Galffy, Lisa Marouzet, Barbara Smids, L. Larsson, Louise Fleming, Corinna Schoelch, Leanne Metcalf, Ashley Woosdcock, Anthony D. Postle, Maxim Kots, Sven-Erik Dahlén, J. M. Edwards, J.C. Smith, Gunilla Hedlin, Breda Flood, Veit J. Erpenbeck, Wen Yu, Susan J. Wilson, Jeanette Bigler, Jorge De Alba, Leon Carayannopoulos, Kristiane Wetzel, Klaus Fichtner, Paul Brinkman, Cecile T.J. Holweg, David Supple, Romanas Chaleckis, Coen Wiegman, Anthony Rowe, Hans Bisgaard, Annelie F. Behndig, Joost Brandsma, Richard G. Knowles, Jorge Beleta, Scott Kuo, Katherine M. Smith, Sandy Pink, Pieter-Paul Hekking, An Bautmans, Ben Nicholas, Kathrin Riemann, Michael Rutgers, Leanne Reynolds, Adesimbo Sogbesan, Dominic Burg, Aruna T. Bansal, Ulf Nihlen, Dyson Kerry, Ioannis Pandis, Julie Corfield, Björn Nordlund, Shama Naz, Wilhelm Zetterquist, Diane Lefaudeux, Xian Yang, Clair Barber, Kirsty E. Russell, Andrew Menzies-Gow, Dominic E. Shaw, Patrick Dennison, Elisabeth Henriksson, John G. Matthews, Tim Higgenbottam, Ratko Djukanovic, Charles Auffray, Kai Sun, Amphun Chaiboonchoe, Jonathan Thorsen, Nikos Lazarinis, Samantha Walker, John-Olof Thörngren, Frédéric Baribaud, Florian Singer, Klaus Bøonnelykke, John H. Riley, Magnus Ericsson, Sile Hu, Jørgen Vestbo, Bertrand De Meulder, Kamran Tariq, Maria Gerhardsson de Verdier, Stacey N. Reinke, Navin Rao, Trevor Garret, Norbert Krug, Michael Boedigheimer, Chris Compton, Cornelia Faulenbach, Hector Gallart, Matthias Klüglich, Caroline Mathon, Giorgio Pennazza, Kian Fan Chung, Thomas Geiser, Jörgen Östling, Courtney Coleman, Erika Kennington, Nora Adriaens, Jane Martin, Medical Research Council (MRC), Commission of the European Communities, National Institute for Health Research, AII - Inflammatory diseases, Pulmonology, AII - Amsterdam institute for Infection and Immunity, Graduate School, Experimental Immunology, Ear, Nose and Throat, APH - Methodology, Epidemiology and Data Science, ARD - Amsterdam Reproduction and Development, and Publica

Subjects
0301 basic medicine, Male, Proteomics, Allergy, Severe asthma, Severity of Illness Index, Leukocyte Count, 0302 clinical medicine, Immunology and Allergy, Medicine, CLASS DISCOVERY, 610 Medicine & health, Oligonucleotide Array Sequence Analysis, COPD, EPITHELIAL-CELLS, Middle Aged, sputum eosinophilia, Phenotype, 1107 Immunology, Cohort, Female, medicine.symptom, Life Sciences & Biomedicine, Algorithms, clustering, EXPRESSION, Adult, Settore BIO/14 - FARMACOLOGIA, Immunology, PHENOTYPES, 03 medical and health sciences, INFLAMMATION, partition-around-medoids algorithm, Severity of illness, Humans, LYN, Asthma, Aged, U-BIOPRED Study Group, Science & Technology, IDENTIFICATION, business.industry, Gene Expression Profiling, Sputum, Omics, medicine.disease, respiratory tract diseases, 030104 developmental biology, 030228 respiratory system, Exhaled nitric oxide, business, Biomarkers
Abstract

BACKGROUND: Asthma is a heterogeneous disease in which there is a differential response to asthma treatments. This heterogeneity needs to be evaluated so that a personalised management approach can be provided.OBJECTIVES: We stratified patients with moderate-to-severe asthma based on clinico-physiological parameters and performed an -omics analysis of sputum.METHODS: Partition-around-medoid clustering was applied to a training set of 266 asthma participants from the European U-BIOPRED adult cohort using 8 pre-specified clinic-physiological variables. This was repeated in a separate validation set of 152 asthmatics. The clusters were compared based on sputum proteomic and transcriptomic data.RESULTS: Four reproducible and stable clusters of asthmatics were identified. The training set cluster T1 consists of well-controlled moderate-to-severe asthmatics, while cluster T2 is a group of late-onset severe asthmatics with history of smoking and chronic airflow obstruction. Cluster T3 is similar to cluster T2 in terms of chronic airflow obstruction but is composed of non-smokers. Cluster T4 is predominantly composed of obese female uncontrolled severe asthmatics with increased exacerbations, but with normal lung function. The validation set exhibited similar clusters, demonstrating reproducibility of the classification. There were significant differences in sputum proteomics and transcriptomics between the clusters. The severe asthma clusters, T2, T3 and T4, had higher sputum eosinophilia than T1 with no differences in sputum neutrophil counts, exhaled nitric oxide and serum IgE levels.CONCLUSION: Clustering based on clinico-physiological parameters yielded 4 stable and reproducible clusters that associate with different pathobiological pathways.CLINICAL IMPLICATIONS: The definition of four distinct clusters of asthma linked to different pathobiological pathways provides a better template for the phenotyping and personalised treatment of severe asthma, where high unmet needs remain.CAPSULE SUMMARY: Unsupervised clustering of asthma on clinical features alone has led to the definition of four phenotypes. Sputum 'omics' analysis has revealed different biological pathways pointing towards potential new treatments.

Published
2017

17. Characterization of the novel GlyT1 PET tracer [18F]MK-6577 in humans

Author

Michel Koole, Terence G. Hamill, Marleen Depré, Cyrille Sur, Koen Van Laere, Anne Van Hecken, Aniket Joshi, Inge De Lepeleire, Jan de Hoon, Sandra M. Sanabria-Bohórquez, and Guy Bormans

Subjects
education.field_of_study, medicine.diagnostic_test, business.industry, Population, Biology, Effective dose (pharmacology), Reuptake, Glycine transporter, Cellular and Molecular Neuroscience, In vivo, Positron emission tomography, medicine, Dosimetry, Potency, Nuclear medicine, business, education
Abstract

Decreased glutamatergic neurotransmission is hypothesized to be involved in the pathophysiology of schizophrenia. Inhibition of glycine transporter Type-1 (GlyT1) reuptake is expected to increase the glutamatergic neurotransmission and may serve as treatment for cognitive and negative symptoms of schizophrenia. In this article, we present human data from a novel GlyT1 PET tracer, [(18) F]MK-6577. In the process of developing a GlyT1 inhibitor therapeutic, a PET tracer can assist in determining the dose with a high probability of sufficiently testing the mechanism of action. This article reports the human PET studies with [(18) F]MK-6577 for measuring GlyT1 receptor availability at baseline in normal human subjects and occupancy with a GlyT1 inhibitor, MK-2637. Studies were also performed to measure radiation burden and the baseline test-retest (T-RT) variability of the tracer. The effective dose from sequential whole-body dosimetry scans in three male subjects was estimated to be 24.5 ± 2.9 µSV/MBq (mean ± SD). The time-activity curves from T-RT scans modeled satisfactorily using a two tissue compartmental model. The tracer uptake was highest in the pons (VT = 6.7 ± 0.9, BPND = 4.1 ± 0.43) and lowest in the cortex (VT = 2.1 ± 0.5, BPND = 0.60 ± 0.23). VT T-RT variability measured in three subjects was

Published
2014

18. IC-P-150: [C-11]MK-6884 PET: CHARACTERIZING BRAIN M4 RECEPTORS IN HEALTHY ELDERLY VOLUNTEERS AND ACETYLCHOLINESTERASE INHIBITORS-TREATED AD PATIENTS

Author

Wenping Li, Kim Serdons, Paolo Zanotti-Fregonara, Amy Cheng, Michel Koole, Eric D. Hostetler, Koen Van Laere, Meixiang Yu, Joseph C. Masdeu, Guy Bormans, Yuchuan Wang, Anthony S. Basile, Maria Belen Pascual, Talakad G. Lohith, Jan de Hoon, Victoria Arbones, Ruben Declercq, Inge De Lepeleire, and Matt S. Anderson

Subjects
Epidemiology, business.industry, Health Policy, Healthy elderly, Pharmacology, Acetylcholinesterase, Psychiatry and Mental health, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Developmental Neuroscience, chemistry, Medicine, Neurology (clinical), Geriatrics and Gerontology, Receptor, business
Published
2019

19. 11C-MK-8278 PET as a Tool for Pharmacodynamic Brain Occupancy of Histamine 3 Receptor Inverse Agonists

Author

Anne Van Hecken, Sandra M. Sanabria-Bohórquez, David P. Mozley, Guy Bormans, Donald Burns, K. Cerchio, Lingling Han, Koenraad Van Laere, Terence G. Hamill, Marleen Depré, Inge De Lepeleire, Richard Hargreaves, John J. Renger, Robert Iannone, Michel Koole, Jan de Hoon, and John Plalcza

Subjects
Adult, Male, Administration, Oral, Pharmacology, Ligands, Histamine agonist, Histamine Agonists, Young Adult, chemistry.chemical_compound, Imaging, Three-Dimensional, Pharmacokinetics, Radioligand, Animals, Humans, Receptors, Histamine H3, Medicine, Spiro Compounds, Radiology, Nuclear Medicine and imaging, Carbon Radioisotopes, Radiometry, Benzofurans, business.industry, Brain, Reproducibility of Results, Human brain, Macaca mulatta, Effective dose (pharmacology), medicine.anatomical_structure, chemistry, Positron-Emission Tomography, Autoreceptor, Radiopharmaceuticals, Histamine H3 receptor, business, Histamine
Abstract

The histamine 3 (H3) receptor is a presynaptic autoreceptor in the central nervous system that regulates the synthesis and release of histamine and modulates the release of other major neurotransmitters. H3 receptor inverse agonists (IAs) may be efficacious in the treatment of various central nervous system disorders, including excessive daytime sleepiness, attention deficit hyperactivity disorder, Alzheimer disease, ethanol addiction, and obesity. Methods: Using PET and a novel high-affinity and selective radioligand 11C-MK-8278, we studied the tracer biodistribution, quantification, and brain H3 receptor occupancy (RO) of MK-0249 and MK-3134, 2 potential IA drugs targeting cerebral H3 receptors, in 6 healthy male subjects (age, 19–40 y). The relationship among H3 IA dose, time on target, and peripheral pharmacokinetics was further investigated in 15 healthy male volunteers (age, 18–40 y) with up to 3 PET scans and 3 subjects per dose level. Results: The mean effective dose for 11C-MK-8278 was 5.4 ± 1.1 μSv/MBq. Human brain kinetics showed rapid high uptake and fast washout. Binding potential values can be assessed using the pons as a reference region, with a test–retest repeatability of 7%. Drug RO data showed low interindividual variability per dose (mean RO SD, 2.1%), and a targeted 90% RO can be reached for both IAs at clinically feasible doses. Conclusion:11C-MK-8278 is a useful novel PET radioligand for determination of human cerebral H3 receptor binding and allows highly reproducible in vivo brain occupancy of H3-targeting drugs, hereby enabling the evaluation of novel compounds in early development to select doses and schedules.

Published
2013

20. In Vivo Quantification of Calcitonin Gene-Related Peptide Receptor Occupancy by Telcagepant in Rhesus Monkey and Human Brain Using the Positron Emission Tomography Tracer [11C]MK-4232

Author

Harold G. Selnick, Mangay Williams, Patricia Miller, Guy Bormans, Hong Fan, Tom Reynders, Koen Van Laere, Cyrille Sur, Ruben Declercq, Rebecca L. Blanchard, Zhizhen Zeng, Eric D. Hostetler, Mona Purcell, Tjibbe de Groot, Sandra Sanabria-Bohorquez, Liza Gantert, Anne Van Hecken, Jan de Hoon, Steven N. Gallicchio, Eugene E. Marcantonio, Inge Derdelinckx, Stacey O'Malley, Stefanie A. Kane, Aniket D. Joshi, Inge De Lepeleire, Richard Hargreaves, Jacquelynn J. Cook, Ian M. Bell, Kerry Riffel, Christopher A. Salvatore, William P. Kennedy, Chi-Chung Li, and Jeffrey L. Evelhoch

Subjects
Adult, Male, Agonist, medicine.medical_specialty, medicine.drug_class, Migraine Disorders, Central nervous system, Calcitonin gene-related peptide, Young Adult, Calcitonin gene-related peptide receptor antagonist, Species Specificity, Calcitonin Gene-Related Peptide Receptor Antagonists, Internal medicine, medicine, Animals, Humans, Spiro Compounds, Tissue Distribution, Carbon Radioisotopes, Pharmacology, Analgesics, Neurogenic inflammation, Telcagepant, Molecular Structure, Chemistry, Imidazoles, Brain, Azepines, Human brain, Middle Aged, Macaca mulatta, Endocrinology, medicine.anatomical_structure, Calcitonin, Positron-Emission Tomography, Molecular Medicine, Acetanilides, Female, Radiopharmaceuticals, Protein Binding
Abstract

Calcitonin gene-related peptide (CGRP) is a potent neuropeptide whose agonist interaction with the CGRP receptor (CGRP-R) in the periphery promotes vasodilation, neurogenic inflammation and trigeminovascular sensory activation. This process is implicated in the cause of migraine headaches, and CGRP-R antagonists in clinical development have proven effective in treating migraine-related pain in humans. CGRP-R is expressed on blood vessel smooth muscle and sensory trigeminal neurons and fibers in the periphery as well as in the central nervous system. However, it is not clear what role the inhibition of central CGRP-R plays in migraine pain relief. To this end, the CGRP-R positron emission tomography (PET) tracer [(11)C]MK-4232 (2-[(8R)-8-(3,5-difluorophenyl)-6,8-[6-(11)C]dimethyl-10-oxo-6,9-diazaspiro[4.5]decan-9-yl]-N-[(2R)-2'-oxospiro[1,3-dihydroindene-2,3'-1H-pyrrolo[2,3-b]pyridine]-5-yl]acetamide) was discovered and developed for use in clinical PET studies. In rhesus monkeys and humans, [(11)C]MK-4232 displayed rapid brain uptake and a regional brain distribution consistent with the known distribution of CGRP-R. Monkey PET studies with [(11)C]MK-4232 after intravenous dosing with CGRP-R antagonists validated the ability of [(11)C]MK-4232 to detect changes in CGRP-R occupancy in proportion to drug plasma concentration. Application of [(11)C]MK-4232 in human PET studies revealed that telcagepant achieved only low receptor occupancy at an efficacious dose (140 mg PO). Therefore, it is unlikely that antagonism of central CGRP-R is required for migraine efficacy. However, it is not known whether high central CGRP-R antagonism may provide additional therapeutic benefit.

Published
2013

21. Evaluation of [18F]MK-0911, a positron emission tomography (PET) tracer for opioid receptor-like 1 (ORL1), in rhesus monkey and human

Author

Hisashi Ohta, Sandra M. Sanabria-Bohórquez, Michael F. Egan, Satoshi Ozaki, Guy Bormans, Kerry Riffel, William Cho, Marleen Depré, Shailendra Patel, Wai-Si Eng, Jacquelynn J. Cook, Tom Reynders, Raymond E. Gibson, Stephen Krause, Koen Van Laere, Christine Ryan, Sheng Bi, Stacey O'Malley, Osamu Okamoto, Eric D. Hostetler, Richard Hargreaves, Hiroshi Kawamoto, Aniket Joshi, Inge De Lepeleire, Tjibbe de Groot, H. Donald Burns, and Jan de Hoon

Subjects
Volume of distribution, medicine.diagnostic_test, Chemistry, medicine.drug_class, Cognitive Neuroscience, Antagonist, Human brain, Pharmacology, Nociceptin receptor, medicine.anatomical_structure, Neurology, Positron emission tomography, Opioid receptor, medicine, Receptor, Neuroscience, Preclinical imaging
Abstract

Antagonism of the central opioid receptor like-1 receptor (ORL1) has been implicated in cognition, and has been a focus of drug discovery efforts to ameliorate the cognitive deficits that remain during the stable treatment of schizophrenia with current antipsychotics. In order to facilitate dose selection for phase II clinical testing an ORL1-specific PET tracer was developed to determine drug plasma concentration versus occupancy relationships in order to ensure that the doses selected and the degree of target engagement were sufficient to ensure adequate proof of concept testing. MK-0911 is a selective, high affinity antagonist for the ORL1 receptor radiolabeled with high specific activity 18F for positron emission tomography (PET) studies. Evaluation of [18F]MK-0911 in rhesus monkey PET studies showed a pattern of brain uptake which was consistent with the known distribution of ORL1. In vitro autoradiography with [18F]MK-0911 in rhesus monkey and human brain tissue slices showed a regional distribution that was consistent with in vivo imaging results in monkey. Pre-treatment of rhesus monkeys with high doses of structurally diverse ORL1 antagonists MK-0584, MK-0337, or MK-5757 achieved blockade of [18F]MK-0911 in all gray matter regions. Baseline PET studies with [18F]MK-0911 in healthy human subjects showed tracer distribution and kinetics similar to that observed in rhesus monkey. Quantification of [18F]MK-0911 uptake in repeat human baseline PET studies showed a test–retest variability in volume of distribution (VT) averaging 3% across brain regions. Humans dosed orally with MK-5757 showed reduced [18F]MK-0911 tracer concentration in brain proportional with MK-5757 dose and plasma level. [18F]MK-0911 was useful for determining MK-5757-induced receptor occupancy of ORL1 to guide MK-5757 dose-selection for clinical proof-of-concept studies. Additionally, [18F]MK-0911 may be a useful tool for studying the pharmacology of ORL1 in various human populations and disease states.

Published
2013

22. Orexin 2 Receptor Antagonism is Sufficient to Promote NREM and REM Sleep from Mouse to Man

Author

Anthony L. Gotter, Vladimir Svetnik, Arie Struyk, Pamela L. Tannenbaum, Mark S. Forman, Nicole Calder, Susan L. Garson, John J. Renger, Christopher J. Winrow, Joanne Stevens, Anthony J. Roecker, Laura B. Rosen, W. Joseph Herring, Ka Lai Yee, Inge De Lepeleire, Xiaodong Li, Paul J. Coleman, Steven V. Fox, and Charles M. Harrell

Subjects
0301 basic medicine, Male, medicine.medical_specialty, Polysomnography, Sleep, REM, Non-rapid eye movement sleep, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Dogs, Orexin Receptors, Internal medicine, mental disorders, Medicine, Animals, Humans, Neuroscience of sleep, Sleep Stages, Multidisciplinary, medicine.diagnostic_test, Dose-Response Relationship, Drug, business.industry, musculoskeletal, neural, and ocular physiology, Sleep in non-human animals, Orexin receptor, Orexin, Rats, 030104 developmental biology, Endocrinology, Sleep Aids, Pharmaceutical, Female, Orexin Receptor Antagonists, Sleep onset, business, 030217 neurology & neurosurgery, psychological phenomena and processes
Abstract

Orexin neuropeptides regulate sleep/wake through orexin receptors (OX1R, OX2R); OX2R is the predominant mediator of arousal promotion. The potential for single OX2R antagonism to effectively promote sleep has yet to be demonstrated in humans. MK-1064 is an OX2R-single antagonist. Preclinically, MK-1064 promotes sleep and increases both rapid eye movement (REM) and non-REM (NREM) sleep in rats at OX2R occupancies higher than the range observed for dual orexin receptor antagonists. Similar to dual antagonists, MK-1064 increases NREM and REM sleep in dogs without inducing cataplexy. Two Phase I studies in healthy human subjects evaluated safety, tolerability, pharmacokinetics and sleep-promoting effects of MK-1064, and demonstrated dose-dependent increases in subjective somnolence (via Karolinska Sleepiness Scale and Visual Analogue Scale measures) and sleep (via polysomnography), including increased REM and NREM sleep. Thus, selective OX2R antagonism is sufficient to promote REM and NREM sleep across species, similarly to that seen with dual orexin receptor antagonism.

Published
2016
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23. A comparison of the natriuretic and kaliuretic effects of cicletanine and hydrochlorothiazide in prehypertensive and hypertensive humans

Author

Kristien Van Dyck, Rose Fernandez, Inge De Lepeleire, Robert M. Carey, Chan R. Beals, Shabri Mitta, Irene Nunes, John J Gildea, Amy O. Johnson-Levonas, Helen E. McGrath, Frank Wagner, Marie-Pierre Malice, Christine McCrary Sisk, Erol Wiegert, and Danielle M. Greenwalt

Subjects
Adult, Male, G-Protein-Coupled Receptor Kinase 4, Pyridines, Physiology, Natriuresis, Pharmacology, Polymorphism, Single Nucleotide, Prehypertension, Hydrochlorothiazide, Double-Blind Method, Internal Medicine, medicine, Humans, Antihypertensive Agents, Aged, Cicletanine, business.industry, Middle Aged, Kaliuresis, Hypertension, Potassium, Cardiology and Cardiovascular Medicine, business, medicine.drug
Abstract

The aim of this study was to compare the single-dose effects of thiazide-type diuretics cicletanine and hydrochlorothiazide (HCTZ), on natriuresis and kaliuresis in prehypertensive and treatment-naïve, stage 1 hypertensive patients and to explore the impact of GRK4 gene polymorphisms on thiazide-induced urinary electrolyte excretion.The study was a randomized, double-blind, placebo-controlled, three-period, four-treatment, balanced incomplete block, cross-over study in male patients assigned to treatment sequences consisting of placebo, cicletanine 50 mg, cicletanine 150 mg, and HCTZ 25 mg, doses used to treat hypertension. Cumulative urine samples were collected predosing and over 24 h after dosing in each period to compare urine electrolyte excretion profiles of potassium (UKV), sodium (UNaV), magnesium, calcium, phosphate, chloride, and pH among groups. Each treatment was administered to 18 different patients in each period, and an equal number of patients had less than and at least three GRK4 allele variants.Compared with placebo, mean UKV was significantly increased with HCTZ 25 mg (12.7 mmol/day; P ≤ 0.001), cicletanine 50 mg (4.6 mmol/day; P = 0.026), and cicletanine 150 mg (5.5 mmol/day; P = 0.011), and mean UNaV was significantly increased with HCTZ 25 mg (102.2 mmol/day; P ≤ 0.001), cicletanine 50 mg (21.7 mmol/day; P = 0.005), and cicletanine 150 mg (57.9 mmol/day; P ≤ 0.001).All treatments had more natriuresis, diuresis, and kaliuresis than placebo, and both doses of cicletanine had less kaliuresis than HCTZ. These findings suggest that cicletanine is a favorable and well tolerated option for the treatment of hypertension with an improved safety profile compared with HCTZ.

Published
2012

24. The effects of laropiprant, a selective prostaglandin D2receptor 1 antagonist, on the antiplatelet activity of clopidogrel or aspirin

Author

Lisa Ratcliffe, Amy O. Johnson-Levonas, Wen-Lin Luo, Jules I. Schwartz, Jan de Hoon, Victor Dishy, Eseng Lai, Julie Mabalot Luk, John A. Wagner, Anne Van Hecken, Waldemar Radziszewski, Walter K. Kraft, Aimee Dallob, and Inge De Lepeleire

Subjects
Aspirin, medicine.diagnostic_test, business.industry, Antagonist, Prostaglandin, Hematology, General Medicine, Pharmacology, Clopidogrel, chemistry.chemical_compound, chemistry, Bleeding time, Pharmacodynamics, medicine, business, Laropiprant, Niacin, medicine.drug
Abstract

Laropiprant (LRPT) is being developed in combination with Merck's extended-release niacin (ERN) formulation for the treatment of dyslipidemia. LRPT, an antagonist of the prostaglandin PGD2 receptor DP1, reduces flushing symptoms associated with ERN. LRPT also has affinity for the thromboxane A2 receptor TP (approximately 190-fold less potent at TP compared with DP1). Aspirin and clopidogrel are two frequently used anti-clotting agents with different mechanisms of action. Since LRPT may potentially be co-administered with either one of these agents, these studies were conducted to assess the effects of steady-state LRPT on the antiplatelet activity of steady-state clopidogrel or aspirin. Bleeding time at 24 h post-dose (trough) was pre-specified as the primary pharmacodynamic endpoint in both studies. Two separate, double-blind, randomized, placebo-controlled, crossover studies evaluated the effects of multiple-dose LRPT on the pharmacodynamics of multiple-dose clopidogrel or aspirin. Healthy subjects were...

Published
2011

25. The potent calcitonin gene-related peptide receptor antagonist, telcagepant, does not affect nitroglycerin-induced vasodilation in healthy men

Author

Rebecca L. Blanchard, Marleen Depré, Jan de Hoon, M. Gail Murphy, Bart Van der Schueren, John Palcza, Inge De Lepeleire, and Anne Van Hecken

Subjects
Pharmacology, medicine.medical_specialty, Telcagepant, business.industry, Haemodynamic response, medicine.drug_class, Antagonist, Hemodynamics, Vasodilation, Calcitonin gene-related peptide, Receptor antagonist, Endocrinology, Calcitonin gene-related peptide receptor antagonist, Internal medicine, Medicine, Pharmacology (medical), business
Abstract

WHAT IS ALREADY KNOWN ABOUT THIS SUBJECT • Telcagepant (MK-0974, Merck & Co., Inc.), an oral calcitonin gene-related peptide (CGRP) antagonist, is effective in treating acute migraine headache. Although CGRP receptor antagonists seem devoid of direct vasoconstrictor activity, animal research suggests a role for CGRP in nitroglycerin (NTG) induced vasodilation. Pulse wave analysis and high resolution ultrasound are sensitive techniques to investigate cardiovascular responses to drugs in vivo in humans. WHAT THIS STUDY ADDS • This study shows that telcagepant, at a supra-therapeutic dose for the treatment of acute migraine headache, has no clinically relevant effect on NTG-induced haemodynamic changes in healthy male volunteers. There is also no measurable vasoconstrictor effect of telcagepant as such in both the central and peripheral vascular bed. The results of the present study support the favourable cardiovascular safety profile of telcagepant and indicate that CGRP is not involved in NTG-induced vasodilation in humans. AIMS To assess the effect of the calcitonin gene-related peptide (CGRP) receptor antagonist, telcagepant, on the haemodynamic response to sublingual nitroglycerin (NTG). METHODS Twenty-two healthy male volunteers participated in a randomized, placebo-controlled, double-blind, two-period, crossover study. Subjects received 500 mg telcagepant or placebo followed, 1.5 h later, by 0.4 mg NTG. To assess the haemodynamic response the following vascular parameters were measured: blood pressure, aortic augmentation index (AIx) and brachial artery diameter (BAD). Data are presented as mean (95% confidence interval, CI). RESULTS The aortic AIx following NTG decreased by −18.50 (−21.02, −15.98) % after telcagepant vs. −17.28 (−19.80, −14.76) % after placebo. The BAD fold increase following NTG was 1.14 (1.12, 1.17) after telcagepant vs. 1.13 (1.10, 1.15) after placebo. For both AIx and BAD, the hypothesis that telcagepant does not significantly affect the changes induced by NTG is supported (P < 0.0001). In addition, no vasoconstrictor effect of telcagepant could be demonstrated. CONCLUSIONS Telcagepant did not affect NTG-induced haemodynamic changes. These data suggest that NTG-induced vasodilation is not CGRP dependent.

Published
2011

26. Antiviral Activity, Safety, and Tolerability of Multiple Ascending Doses of Elbasvir or Grazoprevir in Participants Infected With Hepatitis C Virus Genotype-1 or -3

Author

Robert B. Nachbar, John A. Wagner, Deborah Panebianco, Valentin S. Moiseev, Zhanna Kobalava, Edward Gane, Christina Reitmann, Sorin Visan, Kristien Van Dyck, Frank J. Dutko, Martine Robberechts, Inge De Lepeleire, Wendy W. Yeh, Andreas Hüser, Zifang Guo, Christian Schwabe, Joan R. Butterton, Edward O'Mara, Markus Uhle, Iain P. Fraser, Xiaobi Huang, Nelea Ghicavii, Patricia Jumes, Serghei Popa, Amelia S. Petry, and Frank Wagner

Subjects
Adult, Cyclopropanes, Male, Elbasvir, Genotype, Dose, Hepatitis C virus, Hepacivirus, Pharmacology, medicine.disease_cause, Antiviral Agents, 03 medical and health sciences, 0302 clinical medicine, Double-Blind Method, Oral administration, Quinoxalines, Humans, Medicine, Pharmacology (medical), 030212 general & internal medicine, Benzofurans, Sulfonamides, business.industry, Imidazoles, Hepatitis C, Chronic, Middle Aged, Amides, Grazoprevir, Tolerability, Pharmacodynamics, RNA, Viral, 030211 gastroenterology & hepatology, Carbamates, business, Viral load
Abstract

Purpose Elbasvir (MK-8742) and grazoprevir (MK-5172; Merck & Co, Inc, Kenilworth, New Jersey) are hepatitis C virus (HCV)-specific inhibitors of the nonstructural protein 5A phosphoprotein and the nonstructural protein 3/4A protease, respectively. The aims of these studies were to evaluate the antiviral activity and safety of different doses of elbasvir or grazoprevir each administered as monotherapy to participants infected with either HCV genotype (GT) 1 or GT3. Methods These 2 double-blind, randomized, placebo-controlled, sequential-panel, multiple ascending dose studies were conducted to assess the safety and pharmacodynamics of 5 days of once-daily elbasvir or 7 days of once-daily grazoprevir in adult male participants chronically infected with either HCV GT1 or GT3. Findings Oral administration of elbasvir or grazoprevir once daily exhibited potent antiviral activity in participants with chronic GT1 or GT3 HCV infections. HCV RNA levels declined rapidly (within 1 day for elbasvir and 2 days for grazoprevir). At 50 mg of elbasvir once daily, the mean maximum reductions in HCV RNA from baseline were 5.21, 4.17, and 3.12 log10 IU/mL for GT1b-, GT1a-, and GT3-infected participants, respectively. At 100 mg of grazoprevir once daily, the mean maximum reductions in HCV RNA from baseline were 4.74 and 2.64 log10 IU/mL for GT1- and GT3-infected participants. Implications The results in the elbasvir monotherapy study showed that 10 to 50 mg of elbasvir was associated with a rapid decline in HCV viral load; the results in the grazoprevir monotherapy study suggest that doses of 50 mg of grazoprevir and higher are on the maximum response plateau of the dose–response curve for GT1-infected participants. The results of these proof-of-concept studies provided preliminary data for the selection of the dosages of elbasvir and grazoprevir to test in Phase II and III clinical studies. ClinicalTrials.gov identifiers: NCT00998985 (Protocol 5172-004) and NCT01532973 (Protocol 8742-002).

Published
2018

27. Kinetic analysis of the cannabinoid-1 receptor PET tracer [18F]MK-9470 in human brain

Author

Guy Bormans, H. Donald Burns, Koen Van Laere, Inge De Lepeleire, Karolien Goffin, Sandra M. Sanabria-Bohórquez, and Terence G. Hamill

Subjects
Reproducibility, medicine.medical_specialty, Chemistry, medicine.medical_treatment, Kinetics, General Medicine, MK-9470, Blood flow, Human brain, chemistry.chemical_compound, Nuclear magnetic resonance, medicine.anatomical_structure, Endocrinology, TRACER, Internal medicine, medicine, Radiology, Nuclear Medicine and imaging, Cannabinoid, Distribution Volume
Abstract

Quantitative imaging of the type 1 cannabinoid receptor (CB1R) opens perspectives for many neurological and psychiatric disorders. We characterized the kinetics and reproducibility of the CB1R tracer [18F]MK-9470 in human brain. [18F]MK-9470 data were analysed using reversible models and the distribution volume V T and V ND k 3 (V ND k 3 = K 1 k 2) were estimated. Tracer binding was also evaluated using irreversible kinetics and the irreversible uptake constant K i and fractional uptake rate (FUR) were estimated. The effect of blood flow on these parameters was evaluated. Additionally, the possibility of determining the tracer plasma kinetics using a reduced number of blood samples was also examined. A reversible two-tissue compartment model using a global k 4 value was necessary to describe brain kinetics. Both V T and V ND k 3 were estimated satisfactorily and their test–retest variability was between 10% and 30%. Irreversible methods adequately described brain kinetics and FUR values were equivalent to K i. The linear relationship between K i and V ND k 3 demonstrated that K i or FUR and thus the simple measure of tracer brain uptake provide CB1R availability information. The test–retest variability of K i and FUR was

Published
2009

28. Whole-Body Biodistribution and Radiation Dosimetry of the Human Cannabinoid Type-1 Receptor Ligand 18F-MK-9470 in Healthy Subjects

Author

Michel Koole, Ilonka Guenther, Marie J. Belanger, Sandra M. Sanabria Bohorquez, Karolien Goffin, Igor D. Grachev, Josee Cote, Paul Rothenberg, Richard Hargreaves, Koen Van Laere, Inge De Lepeleire, H. Donald Burns, and Guy Bormans

Subjects
Adult, Male, medicine.medical_specialty, Biodistribution, Cannabinoid receptor, Metabolic Clearance Rate, Pyridines, brain, medicine.medical_treatment, Radiation Dosage, cannabinoid type-1 receptor, Whole-Body Counting, stimulation, Effective dose (radiation), Receptor, Cannabinoid, CB1, pet, Reference Values, Internal medicine, human pet, medicine, Radioligand, Humans, Dosimetry, Tissue Distribution, Radiology, Nuclear Medicine and imaging, endocannabinoid system, Radionuclide Imaging, Receptor, biodistribution, dosimetry, business.industry, Brain, nuclear-medicine, Middle Aged, tracer, f-18-mk-9470, Endocrinology, Organ Specificity, Absorbed dose, healthy subjects, Body Burden, Female, Cannabinoid, Radiopharmaceuticals, Nuclear medicine, business, Relative Biological Effectiveness
Abstract

The cannabinoid type-1 (CB1) receptor is one of the most abundant G-coupled protein receptors in the human body and is responsible for signal transduction of both endogenous and exogenous cannabinoids. The endocannabinoid system is strongly implicated in regulation of homeostasis and several neuropsychiatric disorders, obesity, and associated comorbidities, such as dyslipidemia and metabolic syndrome. We have used whole-body PET/CT to characterize the biodistribution and dosimetry of a novel high-affinity, subtype-selective radioligand, F-18-MK-9470, in healthy male and female subjects. Methods: Eight nonobese subjects (5 men, 3 women; age, 22-54 y) underwent serial whole-body PET/CT for 6 h after a bolus injection of 251 +/- 25 MBq F-18-MK-9470 (N-[2-(3-cyano-phenyl)-3-(4-(2-F-18-fluorethoxy)phenyl)-1-methylpropyl]-2-(5-methyl-2-pyridyloxy)-2-methylproponamide). Source organs were delineated 3-dimensionally using the combined morphologic and functional data. Residence times were derived from time-activity profiles using both the trapezoid rule and curve fitting. Individual organ doses and effective doses were determined using the OLINDA software package, with different approaches for gastrointestinal and urinary excretion modeling. Results: F-18-MK-9470 is taken up slowly in the brain, reaching a plateau at approximately 90-120 min after bolus injection and is excreted predominantly through the hepatobiliary system. The gallbladder, upper large intestine, small intestine, and liver are the organs with the highest absorbed dose (average: 159, 98, 87 and 86 mu Gy/MBq, respectively). The mean effective dose (ED) was 22.8 +/- 4.3 mu Sv/MBq, indicating relatively low intersubject variability and a mean value in the range of many commercially available F-18-labeled radiopharmaceuticals. Brain uptake was relatively high compared with that of existing central nervous system ligands for other receptors, between 3.2% and 4.9% of the injected dose. Conclusion: The estimated radiation bur-den of F-18-MK-9470 for PET CB1 receptor imaging shows relatively low variability between subjects and has an acceptable ED, which allows multiple serial cerebral scans of good image quality, while remaining within the risk category class II-b defined by the World Health Organization and the International Commission for Radiation Protection for a standard injected activity (185-370 MBq). ispartof: Journal of Nuclear Medicine vol:49 issue:3 pages:439-445 ispartof: location:United States status: published

Published
2008

29. A randomized, double-blind, placebo-controlled, short-term monotherapy study of doravirine in treatment-naive HIV-infected individuals

Author

Ying Guo, Ka Lai Yee, John A. Wagner, Dirk Schürmann, Joan R. Butterton, Jocelyn Gilmartin, Rachael Liu, Frank Wagner, Martine Robberechts, Christian Sobotha, Matt S. Anderson, and Inge De Lepeleire

Subjects
0301 basic medicine, Adult, Male, medicine.medical_specialty, Adolescent, Drug-Related Side Effects and Adverse Reactions, Anti-HIV Agents, Pyridones, 030106 microbiology, Immunology, Cmax, HIV Infections, Pharmacology, Placebo, Gastroenterology, law.invention, Placebos, 03 medical and health sciences, chemistry.chemical_compound, Plasma, Young Adult, Randomized controlled trial, Pharmacokinetics, Double-Blind Method, law, Internal medicine, Doravirine, medicine, Immunology and Allergy, Humans, Adverse effect, business.industry, Hepatitis C, Middle Aged, Triazoles, medicine.disease, Confidence interval, 030104 developmental biology, Infectious Diseases, Treatment Outcome, chemistry, RNA, Viral, business
Abstract

Objective To assess the antiviral activity, pharmacokinetics, and safety of doravirine in nonnucleoside reverse transcriptase inhibitor-naive, HIV-infected men. Design Double-blind, randomized, two-panel, dose-escalation study. Methods In two sequential panels, 18 individuals received doravirine [25 mg (Panel A) or 200 mg (Panel B)] or matching placebo once daily for 7 days. Plasma samples were collected daily for measurement of HIV-1 RNA levels and doravirine pharmacokinetics. Results For the mean change from baseline in HIV RNA (log10 copies/ml) at 24 h after the day 7 dose, the mean difference (90% confidence interval) between doravirine and placebo was -1.37 (-1.60, -1.14) in the 25-mg group and -1.26 (-1.51, -1.02) in the 200-mg group. None of the participants had viral breakthrough. Increases in mean AUC0-24 h, Cmax, and C24 h were slightly less than dose-proportional, with median Tmax of 1.0-2.0 h. Steady state was achieved after 3-5 days of once-daily dosing. At steady state, accumulation ratios (day 7/day 1) for AUC0-24 h, Cmax, and C24 h were 1.2-1.6. The calculated effective t1/2 (10-16 h) was similar to that in HIV-uninfected individuals. Adverse events were limited in number, transient, and generally mild to moderate in intensity. One participant had a serious adverse event of elevated liver enzymes (judged probably not drug related) in concurrence with a newly acquired hepatitis C infection. Conclusion Doravirine monotherapy demonstrated robust antiviral activity at both dose levels, without evidence of viral resistance, and was generally well tolerated. Doravirine pharmacokinetics in HIV-infected individuals were similar to those in uninfected individuals receiving similar doses in prior studies.

Published
2015

30. Kinetics of TH2 biomarkers in sputum of asthmatics following inhaled allergen

Author

Veronica M. Rivas, Nicoletta Morelli, Ingrid M C Kamerling, Michael Tanen, Rob Zuiker, J. Diderik Boot, Robin Mogg, Marcella Ruddy, Kristien Van Dyck, Inge De Lepeleire, and Zuzana Diamant

Subjects
Pulmonary and Respiratory Medicine, allergen bronchial provocation test, asthma, sputum, Th2 inflammation, fluticasone, medicine.disease_cause, Placebo, Allergen, Medicine, Original Research Article, Asthma, Fluticasone, business.industry, Eosinophil, respiratory system, medicine.disease, Crossover study, respiratory tract diseases, TH2 inflammation, medicine.anatomical_structure, Pharmacodynamics, Immunology, Sputum, medicine.symptom, business, medicine.drug
Abstract

Background : Allergen-induced late airway response offers important pharmacodynamic targets, including T helper 2 (TH2) biomarkers. However, detection of inflammatory markers has been limited in dithiothreitol-processed sputum. Objectives : To test whether allergen-induced TH2 inflammatory markers can be reproducibly quantified by sensitive detection techniques in ultracentrifuged sputum and the effect of fluticasone (FP) on these endpoints. Methods : Thirteen allergic asthmatics with dual allergen-induced airway responses, documented during a single-blind placebo run-in period, participated in a double-blind, two-period crossover study. Each period consisted of three consecutive days, separated by ≥3 weeks. Following randomization, subjects inhaled FP (500 µg bid, five doses total) or placebo. On Day 2 in each study period, allergen challenge was performed and airway response measured by forced expiratory volume in 1 sec (FEV1) until 7 h post-challenge. Sputum was induced 24 h pre-allergen and 7 and 24 h post-allergen. Sputum samples were split into two portions: TH2 biomarkers were quantified by Meso Scale multiplex platform following ultracentrifugation, and cell differentials were counted on Giemsa–May-Grunwald-stained cytospins. Allergen-induced changes in inflammatory endpoints were compared between FP and placebo using a mixed model ANCOVA. Results : Inhaled allergen induced dual airway responses in all subjects during both placebo periods with reproducible late asthmatic response (LAR) and increased sputum inflammatory biomarkers (IL-2, IL-4, IL-13, and eotaxin-1) and eosinophil counts. FP effectively blunted both the LAR and the inflammatory biomarkers. Conclusions : Combining novel, sensitive quantification methods with ultracentrifugation allows reproducible quantification of sputum biomarkers following allergen challenge, reversed by FP. This approach allows non-invasive identification of pharmacodynamic targets for anti-asthma therapies. Keywords : allergen bronchial provocation test; asthma; sputum; TH2 inflammation; fluticasone (Published: 26 May 2015) Citation: European Clinical Respiratory Journal 2015, 2: 28319 - http://dx.doi.org/10.3402/ecrj.v2.28319

Published
2015

31. Effect of Single Oral Doses of Sitagliptin, a Dipeptidyl Peptidase-4 Inhibitor, on Incretin and Plasma Glucose Levels after an Oral Glucose Tolerance Test in Patients with Type 2 Diabetes

Author

Mark Kipnes, Amy Qiu Wang, Deborah Hilliard, Kenneth C. Lasseter, John A. Wagner, Karen Snyder, Keith Gottesdiener, Wesley Tanaka, Bruno Dietrich, Jens J. Holst, Peng Zhao, Andreas Schrodter, Bart Keymeulen, Catherine Stevens, Carolyn F. Deacon, Kristien Van Dyck, Inge De Lepeleire, Caroline Cilissen, Arthur J. Bergman, Gary A. Herman, Wei Zeng, Marina De Smet, George Golor, Bingming Yi, Michael J. Davies, Paul Kotey, and Michael Tanen

Subjects
Adult, Blood Glucose, Male, endocrine system, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Administration, Oral, Incretin, Gastric Inhibitory Polypeptide, Type 2 diabetes, Dipeptidyl peptidase-4 inhibitor, Biochemistry, Sitagliptin Phosphate, Placebos, Endocrinology, Double-Blind Method, Glucagon-Like Peptide 1, Internal medicine, medicine, Humans, Hypoglycemic Agents, Enzyme Inhibitors, Dipeptidyl-Peptidase IV Inhibitors, Glucose tolerance test, Cross-Over Studies, medicine.diagnostic_test, business.industry, digestive, oral, and skin physiology, Biochemistry (medical), Glucose Tolerance Test, Middle Aged, Triazoles, medicine.disease, Glucagon-like peptide-1, Diabetes Mellitus, Type 2, Area Under Curve, Pyrazines, Pharmacodynamics, Sitagliptin, Female, business, hormones, hormone substitutes, and hormone antagonists, medicine.drug
Abstract

In response to a meal, glucagon-like peptide-1 (GLP-1) and glucose-dependent insulinotropic peptide (GIP) are released and modulate glycemic control. Normally these incretins are rapidly degraded by dipeptidyl peptidase-4 (DPP-4). DPP-4 inhibitors are a novel class of oral antihyperglycemic agents in development for the treatment of type 2 diabetes. The degree of DPP-4 inhibition and the level of active incretin augmentation required for glucose lowering efficacy after an oral glucose tolerance test (OGTT) were evaluated.The objective of the study was to examine the pharmacodynamics, pharmacokinetics, and tolerability of sitagliptin.This was a randomized, double-blind, placebo-controlled, three-period, single-dose crossover study.The study was conducted at six investigational sites.The study population consisted of 58 patients with type 2 diabetes who were not on antihyperglycemic agents.Interventions included sitagliptin 25 mg, sitagliptin 200 mg, or placebo.Measurements included plasma DPP-4 activity; post-OGTT glucose excursion; active and total incretin GIP levels; insulin, C-peptide, and glucagon concentrations; and sitagliptin pharmacokinetics.Sitagliptin dose-dependently inhibited plasma DPP-4 activity over 24 h, enhanced active GLP-1 and GIP levels, increased insulin/C-peptide, decreased glucagon, and reduced glycemic excursion after OGTTs administered at 2 and 24 h after single oral 25- or 200-mg doses of sitagliptin. Sitagliptin was generally well tolerated, with no hypoglycemic events.In this study in patients with type 2 diabetes, near maximal glucose-lowering efficacy of sitagliptin after single oral doses was associated with inhibition of plasma DPP-4 activity of 80% or greater, corresponding to a plasma sitagliptin concentration of 100 nm or greater, and an augmentation of active GLP-1 and GIP levels of 2-fold or higher after an OGTT.

Published
2006

32. Pharmacokinetics of Aprepitant After Single and Multiple Oral Doses in Healthy Volunteers

Author

Michael R. Goldberg, Howard E. Greenberg, Scott A. Waldman, Thomas E. Bradstreet, Kevin J. Petty, A. Knops, Arthur J. Bergman, M.L Constanzer, Kathleen Butler, Laura Howard, Deborah Panebianco, Lisa Hickey, Paul Rothenberg, Nicole Michiels, Anup K. Majumdar, Inge De Lepeleire, and Tami M. Crumley

Subjects
Adult, Male, Nausea, Morpholines, Administration, Oral, Biological Availability, Capsules, Pharmacology, Food-Drug Interactions, Neurokinin-1 Receptor Antagonists, Pharmacokinetics, Humans, Medicine, Pharmacology (medical), Infusions, Intravenous, Aprepitant, Cross-Over Studies, Dose-Response Relationship, Drug, business.industry, Middle Aged, Effective dose (pharmacology), Crossover study, Bioavailability, Regimen, Area Under Curve, Antiemetics, Female, NK1 receptor antagonist, Drug Monitoring, medicine.symptom, business, medicine.drug
Abstract

Aprepitant is the first NK1 receptor antagonist approved for use with corticosteroids and 5HT3 receptor antagonists to prevent chemotherapy-induced nausea and vomiting (CINV). The effective dose to prevent CINV is a 125-mg capsule on day 1 followed by an 80-mg capsule on days 2 and 3. Study 1 evaluated the bioavailability of the capsules and estimated the effect of food. The mean (95% confidence interval [CI]) bioavailabilities of 125-mg and 80-mg final market composition (FMC) capsules, as assessed by simultaneous administration of stable isotope-labeled intravenous (i.v.) aprepitant (2 mg) and FMC capsules, were 0.59 (0.53, 0.65) and 0.67 (0.62, 0.73), respectively. The geometric mean (90% CI) area under the plasma concentration time curve (AUC) ratios (fed/fasted) were 1.2 (1.10, 1.30) and 1.09 (1.00, 1.18) for the 125-mg and 80-mg capsule, respectively, demonstrating that aprepitant can be administered independently of food. Study 2 defined the pharmacokinetics of aprepitant administered following the 3-day regimen recommended to prevent CINV (125 mg/80 mg/80 mg). Consistent daily plasma exposures of aprepitant were obtained following this regimen, which was generally well tolerated.

Published
2006

33. Image-Derived Input Function for [11C]Flumazenil Kinetic Analysis in Human Brain

Author

Alex Maes, Wai-Si Eng, Sandra M. Sanabria-Bohórquez, Patrick Dupont, Guy Bormans, H. Donald Burns, Alexandre Coimbra, T Laethem, José M. Vega, Inge De Lepeleire, Tjibbe de Groot, and Jay Gambale

Subjects
Flumazenil, Cancer Research, Materials science, Kinetic analysis, Image (mathematics), Nuclear magnetic resonance, TRACER, Image Processing, Computer-Assisted, medicine, Humans, Tissue Distribution, Radiology, Nuclear Medicine and imaging, Carbon Radioisotopes, medicine.diagnostic_test, business.industry, Brain, Human brain, Exponential function, Kinetics, Carotid Arteries, medicine.anatomical_structure, Distribution (mathematics), Oncology, Positron emission tomography, Serotonin Antagonists, Radiopharmaceuticals, Nuclear medicine, business, Tomography, Emission-Computed, medicine.drug
Abstract

PURPOSE: We describe a method for analysis of [ 11 C]flumazenil data using an input curve directly derived from the positron emission tomography (PET) images. PROCEDURE: The shape of the tracer plasma curve was obtained from the product of the intact flumazenil fraction in plasma in six arterial samples and the internal carotid artery time-activity curve (TAC). The resulting curve was calibrated using the [ 11 C]flumazenil concentration in three of the six samples. The curve peak was recovered by adding an exponential function to the scaled curve whose parameters were estimated from simultaneous fittings of several tissue TACs assuming that all regions share the same input. RESULTS: Good agreement was found between the image-derived and the experimental plasma curves in six subjects. Distribution volumes were highly correlated with linear regression slope and intercept values between [0.94, 1.03] and [−0.10, 0.16], respectively. CONCLUSION: The proposed method is suitable for benzodiazepine receptor quantification requiring only a few blood samples.

Published
2003

34. O6 Single doses as low as 0.5 mg of the novel NRTTI MK-8591 suppress HIV for at least 7 days

Author

DariaJ Hazuda, Andreas Hüser, Vanessa Levine, Aubrey Stoch, Randolph P. Matthews, Inge De Lepeleire, Sabrina Fox-Bosetti, JayA Grobler, Dirk Schürmann, Sandra Zhang, Marian Iwamoto, Deanne Jackson Rudd, and Martine Robberechts

Subjects
Epidemiology, business.industry, Immunology, Public Health, Environmental and Occupational Health, Human immunodeficiency virus (HIV), Pharmacology, medicine.disease_cause, Microbiology, QR1-502, Infectious Diseases, Virology, medicine, Public aspects of medicine, RA1-1270, business
Published
2017

35. Safety, tolerability and pharmacokinetics of doravirine, a novel HIV non-nucleoside reverse transcriptase inhibitor, after single and multiple doses in healthy subjects

Author

Inge De Lepeleire, Luc M. Van Bortel, Rachael Liu, Matt S. Anderson, June K Ancona, Marissa F. Dockendorf, Ying Guo, Ernestina Tetteh, John A. Wagner, Joan R. Butterton, Jocelyn Gilmartin, and Caroline Cilissen

Subjects
Adult, Male, Pyridones, Midazolam, Human immunodeficiency virus (HIV), Pharmacology, medicine.disease_cause, Multiple dosing, Virus, Drug Administration Schedule, Nucleoside Reverse Transcriptase Inhibitor, chemistry.chemical_compound, Pharmacokinetics, Double-Blind Method, Tandem Mass Spectrometry, Doravirine, medicine, Cytochrome P-450 CYP3A, Humans, Pharmacology (medical), business.industry, Healthy subjects, Middle Aged, Triazoles, Reverse transcriptase, Healthy Volunteers, Infectious Diseases, chemistry, Area Under Curve, Reverse Transcriptase Inhibitors, business, Chromatography, Liquid, Half-Life
Abstract

Background Doravirine is a novel non-nucleoside inhibitor of HIV-1 reverse transcriptase with potent activity against wild-type virus (95% inhibitory concentration 19 nM, 50% human serum). Doravirine has low potential to cause drug–drug interactions since it is primarily eliminated by oxidative metabolism and does not inhibit or significantly induce drug-metabolizing enzymes. Methods The pharmacokinetics and safety of doravirine were investigated in two double-blind, dose-escalation studies in healthy males. Thirty-two subjects received single doses of doravirine (6–1,200 mg) or matching placebo tablets; 40 subjects received doravirine (30–750 mg) or matching placebo tablets once daily for 10 days. In addition, the effect of doravirine (120 mg for 14 days) on single-dose pharmacokinetics of the CYP3A substrate midazolam was evaluated (10 subjects). Results The maximum plasma concentration (Cmax) of doravirine was achieved within 1–5 h with an apparent terminal half-life of 12–21 h. Consistent with single-dose pharma-cokinetics, steady state was achieved after approximately 7 days of once daily administration, with accumulation ratios (day 10/day 1) of 1.1–1.5 in the area under the plasma concentration–time curve during the dosing interval (AUC0–24h), Cmax and trough plasma concentration (C24h). All dose levels produced C24h>19 nM. Administration of 50 mg doravirine with a high-fat meal was associated with slight elevations in AUC time zero to infinity (AUC0–∞) and C24h with no change in Cmax. Midazolam AUC0–∞ was slightly reduced by coadministration of doravirine (geometric mean ratio 0.82, 90% CI 0.70, 0.97). There was no apparent relationship between adverse event frequency or intensity and doravirine dose. No rash or significant central nervous system events other than headache were reported. Conclusions Doravirine is generally well tolerated in single doses up to 1,200 mg and multiple doses up to 750 mg once daily for up to 10 days, with a pharmacokinetic profile supportive of once-daily dosing. Doravirine at steady state slightly reduced the exposure of coadministered midazolam, to a clinically unimportant extent.

Published
2014

36. Effect of Montelukast on the Pharmacokinetics and Pharmacodynamics of Warfarin in Healthy Volunteers

Author

Barry J. Gertz, Marleen Depré, Amanda Freeman, Sherry D. Holland, Kathleen Wynants, Paul J. De Schepper, René Verbesselt, Peggy H. Wong, Inge De Lepeleire, Jef Arnout, and Anne Van Hecken

Subjects
Adult, Cyclopropanes, Male, medicine.drug_class, Acetates, Sulfides, Pharmacology, Double-Blind Method, Pharmacokinetics, Oral administration, Humans, Medicine, Drug Interactions, Pharmacology (medical), Anti-Asthmatic Agents, International Normalized Ratio, Montelukast, Prothrombin time, Cross-Over Studies, medicine.diagnostic_test, business.industry, Anticoagulant, Warfarin, Anticoagulants, Drug interaction, Crossover study, Area Under Curve, Prothrombin Time, Quinolines, Leukotriene Antagonists, business, medicine.drug
Abstract

Montelukast, a cysteinyl leukotriene receptor antagonist, is being developed for the treatment of asthma and related diseases. This study was designed to evaluate whether montelukast at clinically used dosage levels would interfere with the anticoagulant effect of warfarin. In a two-period, double-blind, randomized crossover study, 12 healthy male subjects received a single oral dose of 30 mg warfarin on the 7th day of a 12-day treatment with montelukast, 10 mg daily by mouth, or a placebo. Montelukast had no significant effect on the area under the plasma concentration-time curves and peak plasma concentrations of either R- or S-warfarin. However, slight but statistically significant decreases in time to peak concentration of both warfarin enantiomers and in elimination half-life of the less potent R-warfarin were observed in the presence of montelukast. These changes were not considered as clinically relevant. Montelukast had no significant effect on the anticoagulant effect of warfarin, as assessed by the international normalized ratio (INR) for prothrombin time (AUC0-144 and INR maximum). The results of this study suggest that a clinically important interaction between these drugs is unlikely to occur in patients requiring concomitant administration of both drugs.

Published
1999

37. Evaluation of [¹⁸F]MK-0911, a positron emission tomography (PET) tracer for opioid receptor-like 1 (ORL1), in rhesus monkey and human

Author

Eric D, Hostetler, Sandra, Sanabria-Bohórquez, Waisi, Eng, Aniket D, Joshi, Shailendra, Patel, Raymond E, Gibson, Stacey, O'Malley, Stephen M, Krause, Christine, Ryan, Kerry, Riffel, Sheng, Bi, Osamu, Okamoto, Hiroshi, Kawamoto, Satoshi, Ozaki, Hisashi, Ohta, Tjibbe, de Groot, Guy, Bormans, Marleen, Depré, Jan, de Hoon, Inge, De Lepeleire, Tom, Reynders, Jacquelynn J, Cook, H Donald, Burns, Michael, Egan, William, Cho, Koen, van Laere, and Richard J, Hargreaves

Subjects
Adult, Male, Fluorine Radioisotopes, Brain, Middle Aged, Macaca mulatta, Nociceptin Receptor, Young Adult, Piperidines, Positron-Emission Tomography, Receptors, Opioid, Animals, Humans, Benzimidazoles, Tissue Distribution, Radiopharmaceuticals
Abstract

Antagonism of the central opioid receptor like-1 receptor (ORL1) has been implicated in cognition, and has been a focus of drug discovery efforts to ameliorate the cognitive deficits that remain during the stable treatment of schizophrenia with current antipsychotics. In order to facilitate dose selection for phase II clinical testing an ORL1-specific PET tracer was developed to determine drug plasma concentration versus occupancy relationships in order to ensure that the doses selected and the degree of target engagement were sufficient to ensure adequate proof of concept testing. MK-0911 is a selective, high affinity antagonist for the ORL1 receptor radiolabeled with high specific activity (18)F for positron emission tomography (PET) studies. Evaluation of [(18)F]MK-0911 in rhesus monkey PET studies showed a pattern of brain uptake which was consistent with the known distribution of ORL1. In vitro autoradiography with [(18)F]MK-0911 in rhesus monkey and human brain tissue slices showed a regional distribution that was consistent with in vivo imaging results in monkey. Pre-treatment of rhesus monkeys with high doses of structurally diverse ORL1 antagonists MK-0584, MK-0337, or MK-5757 achieved blockade of [(18)F]MK-0911 in all gray matter regions. Baseline PET studies with [(18)F]MK-0911 in healthy human subjects showed tracer distribution and kinetics similar to that observed in rhesus monkey. Quantification of [(18)F]MK-0911 uptake in repeat human baseline PET studies showed a test-retest variability in volume of distribution (V(T)) averaging 3% across brain regions. Humans dosed orally with MK-5757 showed reduced [(18)F]MK-0911 tracer concentration in brain proportional with MK-5757 dose and plasma level. [(18)F]MK-0911 was useful for determining MK-5757-induced receptor occupancy of ORL1 to guide MK-5757 dose-selection for clinical proof-of-concept studies. Additionally, [(18)F]MK-0911 may be a useful tool for studying the pharmacology of ORL1 in various human populations and disease states.

Published
2012

38. Pharmacokinetics and pharmacodynamics of MK-383, a selective non-peptide platelet glycoprotein-IIb/IIIa receptor antagonist, in healthy men

Author

Hans Deckmyn, Kathelijne Peerlinck, E. L. Hand, Robert J. Gould, Inge De Lepeleire, Jef Arnout, Jos Vermylen, Jeffrey S. Barrett, Gail Murphy, and Deborah Panebianco

Subjects
Blood Platelets, Male, medicine.medical_specialty, Fibrinogen receptor, Platelet Membrane Glycoproteins, Fibrinogen, Double-Blind Method, Pharmacokinetics, Reference Values, Bleeding time, Internal medicine, medicine, Humans, Pharmacology (medical), Platelet, Pharmacology, Volume of distribution, Analysis of Variance, Aspirin, medicine.diagnostic_test, business.industry, Endocrinology, Tirofiban, Pharmacodynamics, Tyrosine, business, medicine.drug
Abstract

MK-383 (L-tyrosine, N-n-butylsulfonyl)-O-[4-butyl(4-piperidinyl)], monohydrochloride monohydrate) is a potent and specific platelet fibrinogen receptor antagonist that may be useful in preventing processes that lead to occlusive thrombus formation in the lumen of the blood vessel. Two placebo-controlled phase I trials were completed in 56 healthy volunteers to investigate the safety, tolerability, pharmacokinetics, and pharmacodynamics of MK-383 administered as 1- and 4-hour infusions in the presence and absence of aspirin. When administered to healthy male subjects by constant infusions up to 0.4 µg/kg/min over 1 hour or up to 0.2 µg/min over 4 hours, it provided a well-tolerated reversible means of inhibiting platelet function. At infusion rates of 0.25 and 0.15 µg/kg/min for 1 and 4 hours, respectively, MK-383 extended baseline bleeding time by 2.0- to 2.5-fold and inhibited adenosine diphosphate (ADP)-induced platelet aggregation by at least 80%. The pharmacokinetics of MK-383 include a mean plasma clearance of 329 ml/min, steady-state volume of distribution of 76 L, and half-life of 1.6 hours. The percentage of dose excreted in the urine was 37%. Correlations between MK-383 plasma concentration (C) and inhibition of platelet aggregation were examined by fitting with a sigmoid maximum-effect model. The plasma concentration yielding 50% inhibition (C50) for MK-383 in healthy volunteers is approximately 13 ng/ml, with a Hill coefficient >5. Based on a naive pooled analysis, an exponential empirical model best describes the MK-383 C–extension of template bleeding time (BTE) relationship. The model indicates that the MK-383 plasma concentration necessary to double BTE is approximately 30 ng/ml (i.e., 2.5-fold greater than the C50 for ADP-induced inhibition of platelet aggregation). The pharmacokinetics of MK-383 was unaffected by pretreatment with 325 mg aspirin 1 day before and 1 hour before infusion. Conversely, aspirin pretreatment reduced C50 and increased bleeding time extension, suggesting that aspirin may have an additive effect with respect to inhibition of platelet function. Based on the putative role of the fibrinogen receptor in thrombotic processes and an acceptable human pharmacokinetic-pharmacodynamic profile, MK-383 should be evaluated in patients with unstable angina. Clinical Pharmacology and Therapeutics (1994) 56, 377–388; doi:10.1038/clpt.1994.152

Published
1994

39. Pharmacokinetics and pharmacodynamics of multiple oral doses of MK-0591, a 5-lipoxygenase—activating protein inhibitor

Author

Beth Friedman, Aimee Dallob, Sumiko Shingo, Charles Lin, Anne Van Hecken, Inge De Lepeleire, Wesley Tanaka, Paul J. De Schepper, Arturo Porras, and Marken Depré

Subjects
Adult, Male, Indoles, Leukotriene B4, 5-Lipoxygenase-Activating Proteins, Administration, Oral, Pharmacology, chemistry.chemical_compound, Double-Blind Method, Pharmacokinetics, Reference Values, Oral administration, Blood plasma, Humans, Testosterone, Pharmacology (medical), Lipoxygenase Inhibitors, Whole blood, Analysis of Variance, Leukotriene E4, Membrane Proteins, Respiratory Function Tests, chemistry, Pharmacodynamics, Quinolines, Leukotriene Antagonists, Carrier Proteins, Ex vivo
Abstract

The pharmacodynamics, kinetics, and tolerability of a new orally active 5-lipoxygenase inhibitor were evaluated in healthy male volunteers. MK-0591, 50, 125, and 250 mg every morning and 250 mg every 12 hours, was administered for 10 days. Leukotriene B4 biosynthesis ex vivo in ionophore (A23187)-stimulated whole blood and leukotriene E4 levels in urine were determined. Leukotriene B4 production was inhibited up to 90% of baseline for 12 hours after administration at the highest dose. The degree of leukotriene B4 inhibition ex vivo in whole blood significantly correlated with plasma MK-0591 concentrations (0 to 1500 ng/ml; r = 0.73). Urinary leukotriene E4 was inhibited by >80% at 24 hours after administration for all dose levels. Pharmacokinetics of MK-0591 were linear, with a half-life of approximately 6 hours. Very little accumulation was seen after multiple dosing. MK-0591 had no effect on testosterone levels, and good tolerability was shown at all dose levels of MK-0591 administered for up to 10 days. Clinical Pharmacology and Therapeutics (1994) 56, 22–30; doi:10.1038/clpt.1994.96

Published
1994

40. A randomized clinical trial comparing point-of-care platelet function assays and bleeding time in healthy subjects treated with aspirin or clopidogrel

Author

Fabian Chen, Jan de Hoon, Victor Maridakis, Kristien Van Dyck, Marleen Depré, Chan R. Beals, Inge De Lepeleire, James Bolognese, Marc Jacquemin, Waldemar Radziszewski, and Edward A. O'Neill

Subjects
Adult, Male, Bleeding Time, Ticlopidine, Genotype, Platelet Aggregation, Platelet Function Tests, Point-of-Care Systems, Placebo, law.invention, Young Adult, Randomized controlled trial, Bleeding time, law, medicine, Humans, Platelet, Aspirin, Cross-Over Studies, medicine.diagnostic_test, business.industry, Hematology, General Medicine, Middle Aged, Clopidogrel, Crossover study, Clinical trial, Cytochrome P-450 CYP2C19, Anesthesia, Female, Aryl Hydrocarbon Hydroxylases, business, Platelet Aggregation Inhibitors, medicine.drug
Abstract

Traditional assays of the coagulation status of patients, bleeding time assessment (BT) and light transmission aggregometry (LTA), are useful in clinical drug development. However, these assays are both labor intensive and expensive. BT results can be operator dependent and by its nature can inhibit subject enrollment in a clinical trial. The preparation of platelet-rich plasma necessary for LTA requires specialized training and laboratory support. Alternatives to these methods are desirable. The goal of this study was identification of a quantitative, easy-to-use, point-of-care device with minimal technical variables that could facilitate assessment of platelet aggregation in clinical drug development. This was a double-blind, placebo-controlled, randomized, three-period cross-over study in healthy volunteers designed to compare the abilities of BT, LTA, and three point-of-care devices, Multiplate®, Platelet Function Analyzer-100®, and VerifyNow® to quantitate the effects on platelet function of 3 days of treatment with aspirin, clopidogrel, or placebo. The effect size (difference in treatment means divided by the pooled standard deviations [SD]) of the three point-of-care devices was greater than or similar to BT and LTA for all treatment comparisons examined. VerifyNow® had the highest effect size comparing ASA to placebo. Multiplate® had the highest effect size comparing clopidogrel to placebo. From this study, we conclude that any one of the three simple-to-use point-of-care devices can reliably assess the treatment effect of ASA and CLP on platelet function in comparison with BT or LTA at the study population level

Published
2011

41. P2‐035: Preliminary evaluation of the amyloid PET Radioligand [18F]MK‐3328 in Alzheimer's Disease patients

Author

Kim Serdons, John Seibyl, Olivier Barret, Cyrille Sur, Laura B. Rosen, Guy Bormans, Sandra M. Sanabria-Bohórquez, Michel Koole, Kenneth Marek, Jeffrey L. Evelhoch, Gilles Tamagnan, Eric D. Hostetler, Inge De Lepeleire, Richard Hargreaves, Jan Versijpt, Danna Jennings, Tom Reynders, Koen Van Laere, Mark S. Forman, Andrei O. Koren, Rik Vandenberghe, and Jan de Hoon

Subjects
Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, media_common.quotation_subject, Amyloid pet, Neurology (clinical), Art, Geriatrics and Gerontology, University hospital, Humanities, media_common
Abstract

P2-035 PRELIMINARY EVALUATION OF THE AMYLOID PET RADIOLIGAND [18F]MK-3328 IN ALZHEIMER’S DISEASE PATIENTS Sandra Sanabria-Bohorquez, Eric Hostetler, Koen Van Laere, Michel Koole, Guy Bormans, Kim Serdons, Jan de Hoon, Rik Vandenberghe, Jan Versijpt, Inge De Lepeleire, Tom Reynders, Gilles Tamagnan, Kenneth Marek, John Seibyl, Danna Jennings, Olivier Barret, Andrei Koren, Laura Rosen, Richard Hargreaves, Jeffrey Evelhoch, Cyrille Sur, Mark Forman, Merck, West Point, Pennsylvania, United States; University Hospital Leuven, Leuven, Belgium; UZ Leuven, Leuven, Belgium; KU Leuven, Leuven, Belgium; University Hospitals Leuven, Leuven, Belgium; UZ Brussels, Brussels, Belgium; Merck, Brussels, Belgium; MNI, New Haven, Connecticut, United States; Merck, Upper Gwynedd, Pennsylvania, United States; Merck, West point, Pennsylvania, United States.

Published
2011

42. The effects of laropiprant, a selective prostaglandin D₂ receptor 1 antagonist, on the antiplatelet activity of clopidogrel or aspirin

Author

Aimee, Dallob, Wen-Lin, Luo, Julie Mabalot, Luk, Lisa, Ratcliffe, Amy O, Johnson-Levonas, Jules I, Schwartz, Victor, Dishy, Walter K, Kraft, Jan N, De Hoon, Anne, Van Hecken, Inge, De Lepeleire, Waldemar, Radziszewski, John A, Wagner, and Eseng, Lai

Subjects
Adult, Blood Platelets, Male, Bleeding Time, Indoles, Ticlopidine, Adolescent, Aspirin, Platelet Aggregation, Receptors, Prostaglandin, Middle Aged, Clopidogrel, Young Adult, Humans, Female, Receptors, Immunologic, Platelet Aggregation Inhibitors
Abstract

Laropiprant (LRPT) is being developed in combination with Merck's extended-release niacin (ERN) formulation for the treatment of dyslipidemia. LRPT, an antagonist of the prostaglandin PGD₂ receptor DP1, reduces flushing symptoms associated with ERN. LRPT also has affinity for the thromboxane A₂ receptor TP (approximately 190-fold less potent at TP compared with DP1). Aspirin and clopidogrel are two frequently used anti-clotting agents with different mechanisms of action. Since LRPT may potentially be co-administered with either one of these agents, these studies were conducted to assess the effects of steady-state LRPT on the antiplatelet activity of steady-state clopidogrel or aspirin. Bleeding time at 24 h post-dose (trough) was pre-specified as the primary pharmacodynamic endpoint in both studies. Two separate, double-blind, randomized, placebo-controlled, crossover studies evaluated the effects of multiple-dose LRPT on the pharmacodynamics of multiple-dose clopidogrel or aspirin. Healthy subjects were randomized to once-daily oral doses of LRPT 40 mg or placebo to LRTP co-administered with clopidogrel 75 mg or aspirin 81 mg for 7 days with at least a 21-day washout between treatments. In both studies, bleeding time and platelet aggregation were assessed 4 and 24 hours post-dose on Day 7. Comparability was declared if the 90% confidence interval for the estimated geometric mean ratio ([LRPT+clopidogrel]/clopidogrel alone or [LRPT+aspirin]/aspirin alone) for bleeding time at 24 hours post-dose on Day 7 was contained within (0.66, 1.50). Concomitant daily administration of LRPT 40 mg with clopidogrel 75 mg or aspirin 81 mg resulted in an approximate 4-5% increase in bleeding time at 24 hours after the last dose vs. bleeding time after treatment with clopidogrel or aspirin alone, demonstrating that the treatments had comparable effects on bleeding time. Percent inhibition of platelet aggregation was not significantly different between LRPT co-administered with clopidogrel or aspirin vs. clopidogrel or aspirin alone at 24 hours post-dose at steady state. At 4 hours after the last dose, co-administration of LRPT 40 mg resulted in 3% and 41% increase in bleeding time vs. bleeding time after treatment with aspirin or clopidogrel alone, respectively. Co-administration of LPRT with clopidogrel or aspirin was generally well tolerated in healthy subjects. Co-administration of multiple doses of LRPT 40 mg and clopidogrel 75 mg or aspirin 81 mg had no clinically important effects on bleeding time or platelet aggregation.

Published
2011

43. The potent calcitonin gene-related peptide receptor antagonist, telcagepant, does not affect nitroglycerin-induced vasodilation in healthy men

Author

Bart J, Van der Schueren, Rebecca, Blanchard, M Gail, Murphy, John, Palcza, Inge, De Lepeleire, Anne, Van Hecken, Marleen, Depré, and Jan N, de Hoon

Subjects
Adult, Male, Cross-Over Studies, Brachial Artery, Vasodilator Agents, Imidazoles, Blood Pressure, Azepines, Middle Aged, Vasodilation, Nitroglycerin, Young Adult, Double-Blind Method, Pharmacodynamics, Calcitonin Gene-Related Peptide Receptor Antagonists, Heart Rate, Humans, Drug Interactions, Aorta
Abstract

To assess the effect of the calcitonin gene-related peptide (CGRP) receptor antagonist, telcagepant, on the haemodynamic response to sublingual nitroglycerin (NTG).Twenty-two healthy male volunteers participated in a randomized, placebo-controlled, double-blind, two-period, crossover study. Subjects received 500 mg telcagepant or placebo followed, 1.5 h later, by 0.4 mg NTG. To assess the haemodynamic response the following vascular parameters were measured: blood pressure, aortic augmentation index (AIx) and brachial artery diameter (BAD). Data are presented as mean (95% confidence interval, CI).The aortic AIx following NTG decreased by -18.50 (-21.02, -15.98) % after telcagepant vs. -17.28 (-19.80, -14.76) % after placebo. The BAD fold increase following NTG was 1.14 (1.12, 1.17) after telcagepant vs. 1.13 (1.10, 1.15) after placebo. For both AIx and BAD, the hypothesis that telcagepant does not significantly affect the changes induced by NTG is supported (P0.0001). In addition, no vasoconstrictor effect of telcagepant could be demonstrated.Telcagepant did not affect NTG-induced haemodynamic changes. These data suggest that NTG-induced vasodilation is not CGRP dependent.

Published
2011

44. P3‐179: Development of the amyloid PET radioligand [ 18 F]MK‐3328

Author

Cyrille Sur, Tom Reynders, Koen Van Laere, Jan de Hoon, Laura Rosen, Zhizhen Zeng, Richard Hargreaves, Inge De Lepeleire, Mark Forman, Sandra M. Sanabria-Bohórquez, David L. Williams, Rik Vandenberghe, Michel Koole, Guy Bormans, Eric D. Hostetler, and Kim Serdons

Subjects
Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Chemistry, Health Policy, Radioligand, Amyloid pet, Neurology (clinical), Geriatrics and Gerontology, Pharmacology
Published
2010

45. Allergen-induced RNA Signature Identified In Induced Sputum And In Whole Blood From Allergic Asthmatics Is Modulated By A Short Course Of Inhaled Fluticasone

Author

Kristien Van Dyck, Inge De Lepeleire, George Y. Tokiwa, Rob Zuiker, Peter H. Hu, Marcella Ruddy, Zuzana Diamant, Catherine Tribouley, D Boot, Veronica M. Rivas, and Vladislav A. Malkov

Subjects
Allergen, business.industry, Immunology, medicine, RNA, Induced sputum, medicine.disease_cause, business, Fluticasone, medicine.drug, Whole blood
Published
2010

47. Effect of diltiazem, a moderate CYP3A inhibitor, on the pharmacokinetics of anacetrapib, a potent cholesteryl ester transfer protein inhibitor, in healthy subjects

Author

Christy Corr, Tarun Wadhwa, Jinesh Shah, Andrea Maes, Amit Garg, Nikhil Handa, Rajesh Krishna, Kristien Van Dyck, Inge De Lepeleire, Bo Jin, and John A. Wagner

Subjects
Adult, Male, Adolescent, CYP3A, Hyperlipidemias, Pharmacology, chemistry.chemical_compound, Diltiazem, Young Adult, Pharmacokinetics, Anacetrapib, Cholesterylester transfer protein, medicine, Humans, Pharmacology (medical), Drug Interactions, Enzyme Inhibitors, Oxazolidinones, biology, Healthy subjects, Middle Aged, Cholesterol Ester Transfer Proteins, chemistry, Delayed-Action Preparations, biology.protein, Linear Models, Cytochrome P-450 CYP3A Inhibitors, Female, medicine.drug, Half-Life
Published
2010

48. Inhibition of capsaicin-induced increase in dermal blood flow by the oral CGRP receptor antagonist, telcagepant (MK-0974)

Author

Alan Xiao, Jay N. De Hoon, Lisa Hickey, Tony W. Ho, M. Gail Murphy, Janet Boyle, S.R. Sinclair, Chi-Chung Li, Yang Xu, Floris H.M. Vanmolkot, Kenneth J. Willson, William S. Denney, Stefanie A. Kane, Anne Van Hecken, Marleen Depré, Bart Van der Schueren, Inge De Lepeleire, and John Palcza

Subjects
Adult, Male, medicine.medical_specialty, Adolescent, medicine.drug_class, Administration, Topical, Vasodilator Agents, Administration, Oral, Vasodilation, Calcitonin gene-related peptide, Models, Biological, chemistry.chemical_compound, Young Adult, Oral administration, Calcitonin Gene-Related Peptide Receptor Antagonists, Internal medicine, medicine, Laser-Doppler Flowmetry, Humans, Pharmacology (medical), Drug Interactions, Skin, Pharmacology, Telcagepant, Cross-Over Studies, Dose-Response Relationship, Drug, business.industry, Antagonist, Imidazoles, Azepines, Middle Aged, Receptor antagonist, medicine.disease, Forearm, Endocrinology, chemistry, Migraine, Pharmacodynamics, Capsaicin, Regional Blood Flow, business
Abstract

WHAT IS ALREADY KNOWN ABOUT THIS SUBJECT • Calcitonin gene-related peptide (CGRP) was first described as a potent vasodilator. • CGRP is also increasingly recognized as a key player in the pathophysiology of migraine, and CGRP receptor antagonists potentially offer a new approach for treating migraine. • A novel pharmacodynamic assay to measure CGRP receptor antagonist activity non-invasively in humans has been developed, which involves measuring the increase in dermal blood flow induced by topical application of capsaicin on the forearm. WHAT THIS STUDY ADDS • This study shows that the novel oral CGRP receptor antagonist, telcagepant, inhibits the increases in dermal blood flow induced by the topical application of capsaicin on the human forearm. • This experimental medicine model may have utility to assist in dose selection for the development of CGRP receptor antagonists. AIMS To evaluate inhibition of capsaicin-induced increase in dermal blood flow (DBF) following telcagepant (MK-0974), a potent and selective orally bioavailable calcitonin gene-related peptide (CGRP) receptor antagonist being developed for the acute treatment of migraine. METHODS A three-period crossover study in 12 healthy adult men. Each subject received a single oral dose of telcagepant 300 mg, telcagepant 800 mg or placebo at 0 h, followed 0.5 and 3.5 h later by two topical doses of 300 and 1000 µg capsaicin per 20 µl water–ethanol mixture. Capsaicin was applied at two sites on the volar surface of the subjects' left and right forearms. DBF was assessed by laser Doppler perfusion imaging immediately before (‘baseline’), and 0.5 h after each capsaicin application at 1 and 4 h. Plasma samples to determine telcagepant concentrations were collected immediately after laser Doppler perfusion imaging. A pharmacodynamic model was developed to explore the relationship between plasma concentration and inhibition of capsaicin-induced increase in DBF. RESULTS Geometric mean plasma concentrations after dosing with 300 mg and 800 mg telcagepant were 720 and 1146 nm, respectively, at 1 h, vs. 582 and 2548 nm, respectively, at 4 h. The pharmacodynamic model suggested that the EC90 for telcagepant inhibition of capsaicin-induced increases in DBF was 909 nm. CONCLUSIONS Telcagepant inhibits the increases in DBF induced by the topical application of capsaicin on the human forearm. This experimental medicine model may have utility to assist in dose selection for the development of CGRP receptor antagonists.

Published
2010

49. Lack of erectogenic activity of a novel selective melanocortin-4 receptor agonist in a clinical experimental model

Author

Catherine Stevens, Peggy H. Wong, Kristien Van Dyck, Inge De Lepeleire, Gary A. Herman, Mathieu Peeters, I.N. Gendrano, John A. Wagner, Raymond C. Rosen, and Rajesh Krishna

Subjects
Agonist, Drug, Adult, Male, medicine.drug_class, media_common.quotation_subject, Vasodilator Agents, Pharmacology, Piperazines, Sildenafil Citrate, law.invention, Randomized controlled trial, Double-Blind Method, Erectile Dysfunction, law, Medicine, Humans, Pharmacology (medical), Sulfones, Receptor, media_common, Cross-Over Studies, Dose-Response Relationship, Drug, business.industry, Middle Aged, medicine.disease, Crossover study, Melanocortin 4 receptor, Erectile dysfunction, Purines, Receptor, Melanocortin, Type 4, Melanocortin, business
Published
2008

50. Multiple-dose pharmacokinetics, pharmacodynamics, and safety of taranabant, a novel selective cannabinoid-1 receptor inverse agonist, in healthy male volunteers

Author

Jinyu Yuan, Susie Li, John A. Wagner, Carol Addy, Annemie Knops, Aubrey Stoch, Nancy G. B. Agrawal, Andrea Maes, Jan de Hoon, Kim Rosko, Hankun Li, Kristien Van Dyck, Stephanie Dunbar, Keith Gottesdiener, Anne Van Hecken, Anup K. Majumdar, Inge De Lepeleire, Ling Zhong, Marleen Depré, Paul Rothenberg, and Josee Cote

Subjects
Adult, Male, medicine.medical_specialty, Drug Inverse Agonism, Pyridines, medicine.medical_treatment, Pharmacology, Drug Administration Schedule, Taranabant, Pharmacokinetics, Double-Blind Method, Receptor, Cannabinoid, CB1, Internal medicine, medicine, Inverse agonist, Humans, Pharmacology (medical), Dosing, Obesity, Dose-Response Relationship, Drug, Chemistry, Half-life, Middle Aged, Amides, Dose–response relationship, Endocrinology, Pharmacodynamics, Area Under Curve, Cannabinoid, Anti-Obesity Agents, medicine.drug, Half-Life
Abstract

Taranabant is a cannabinoid-1 receptor inverse agonist for the treatment of obesity. This study evaluated the safety, pharmacokinetics, and pharmacodynamics of taranabant (5, 7.5, 10, or 25 mg once daily for 14 days) in 60 healthy male subjects. Taranabant was rapidly absorbed, with a median t(max) of 1.0 to 2.0 hours and a t(1/2) of approximately 74 to 104 hours. Moderate accumulation was observed in C(max) (1.18- to 1.40-fold) and AUC(0-24 h) (1.5- to 1.8-fold) over 14 days for the 5-, 7.5-, and 10-mg doses, with an accumulation half-life ranging from 15 to 21 hours. Steady state was reached after 13 days. After multiple-dose administration, plasma AUC(0-24 h) and C(max) of taranabant increased dose proportionally (5-10 mg) and increased somewhat less than dose proportionally for 25 mg. Taranabant was generally well tolerated up to doses of 10 mg and exhibited multiple-dose pharmacokinetics consistent with once-daily dosing.

Published
2008

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