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43 results on '"Wong, Bradley K."'

1. A Naphthyridine Carboxamide Provides Evidence for Discordant Resistance between Mechanistically Identical Inhibitors of HIV-1 Integrase

Author

Hazuda, Daria J., Anthony, Neville J., Gomez, Robert P., Jolly, Samson M., Wai, John S., Zhuang, Linghang, Fisher, Thorsten E., Embrey, Mark, Guare,, James P., Egbertson, Melissa S., Vacca, Joseph P., Huff, Joel R., Felock, Peter J., Witmer, Marc V., Stillmock, Kara A., Danovich, Robert, Grobler, Jay, Miller, Michael D., Espeseth, Amy S., Jin, Lixia, Lin, Jiunn H., Kassahun, Kelem, Ellis, Joan D., Wong, Bradley K., Xu, Wei, Pearson, Paul G., Schleif, William A., Cortese, Riccardo, Emini, Emilio, Summa, Vincenzo, Holloway, M. Katharine, Young, Steven D., and Coffin, John M.

Published
2004

4. Preclinical and clinical evaluation of the LRRK2 inhibitor DNL201 for Parkinson’s disease

Author

Jennings, Danna, primary, Huntwork-Rodriguez, Sarah, additional, Henry, Anastasia G., additional, Sasaki, Jennifer C., additional, Meisner, René, additional, Diaz, Dolores, additional, Solanoy, Hilda, additional, Wang, Xiang, additional, Negrou, Elvira, additional, Bondar, Vitaliy V., additional, Ghosh, Rajarshi, additional, Maloney, Michael T., additional, Propson, Nicholas E., additional, Zhu, Yuda, additional, Maciuca, Romeo D., additional, Harris, Laura, additional, Kay, Angela, additional, LeWitt, Peter, additional, King, T. Alex, additional, Kern, Drew, additional, Ellenbogen, Aaron, additional, Goodman, Ira, additional, Siderowf, Andrew, additional, Aldred, Jason, additional, Omidvar, Omid, additional, Masoud, Shababa T., additional, Davis, Sonnet S., additional, Arguello, Annie, additional, Estrada, Anthony A., additional, de Vicente, Javier, additional, Sweeney, Zachary K., additional, Astarita, Giuseppe, additional, Borin, Marie T., additional, Wong, Bradley K., additional, Wong, Harvey, additional, Nguyen, Hoang, additional, Scearce-Levie, Kimberly, additional, Ho, Carole, additional, and Troyer, Matthew D., additional

Published
2022
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7. Discovery of potent, selective 4-fluoroproline-based thrombin inhibitors with improved metabolic stability

Author

Staas, Donnette D., Savage, Kelly L., Sherman, Vanessa L., Shimp, Heidi L., Lyle, Terry A., Tran, Lekhanh O., Wiscount, Catherine M., McMasters, Daniel R., Sanderson, Philip E.J., Williams, Peter D., Lucas, Bobby J., Jr., Krueger, Julie A., Dale Lewis, S., White, Rebecca B., Yu, Sean, Wong, Bradley K., Kochansky, Christopher J., Reza Anari, M., Yan, Youwei, and Vacca, Joseph P.

Published
2006
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8. A peptide-doxorubicin 'prodrug' activated by prostate-specific antigen selectively kills prostate tumor cells positive for prostate-specific antigen in vivo

Author

DeFeo-Jones, Deborah, Garsky, Victor M., Wong, Bradley K., Feng, Dong-Mei, Bolyar, Trina, Haskell, Kathleen, Kiefer, David M., Leander, Karen, McAvoy, Elizabeth, Lumma, Patricia, Wai, Jenny, Senderak, Edith T., Motzel, Sherri L., Keenan, Kevin, Zwieten, Matthew Van, Lin, Jiunn H., Freidinger, Roger, Huff, Joel, Oliff, Allen, and Jones, Raymond E.

Subjects
Doxorubicin -- Dosage and administration, Prostate cancer -- Genetic aspects, Prostate cancer -- Drug therapy, Prostate cancer -- Research, Prostate-specific antigen -- Measurement, Prostate-specific antigen -- Health aspects, Prostate-specific antigen -- Research
Abstract

We covalently linked doxorubicin with a peptide that is hydrolyzable by prostate-specific antigen. In the presence of prostate tumor cells secreting prostate-specific antigen, the peptide moiety of this conjugate, L-377,202, was hydrolyzed, resulting in the release of leucine-doxorubicin and doxorubicin, which are both very cytotoxic to cancer cells. However, L-377,202 was much less cytotoxic than conventional doxorubicin to cells in culture that do not secrete prostate-specific antigen. L-377,202 was approximately 15 times more effective than was conventional doxorubicin at inhibiting the growth of human prostate cancer tumors in nude mice when both drugs were used at their maximally tolerated doses. Nude mice inoculated with human prostate tumor cells secreting prostate-specific antigen showed considerable reductions in tumor burden with minimal total body weight loss when treated with L-377,202. This improvement in therapeutic index correlated with the selective localization of leucine-doxorubicin and free doxorubicin in tissues secreting prostate-specific antigen after exposure to L-377,202., Author(s): Deborah DeFeo-Jones [1]; Victor M. Garsky [2]; Bradley K. Wong [3]; Dong-Mei Feng [2]; Trina Bolyar [1]; Kathleen Haskell [1]; David M. Kiefer [1]; Karen Leander [1]; Elizabeth McAvoy [...]

Published
2000

16. P3 optimization of functional potency, in vivo efficacy and oral bioavailability in 3-aminopyrazinone thrombin inhibitors bearing non-charged groups at the P1 position

Author

Isaacs, Richard C.A., Newton, Christina L., Cutrona, Kellie J., Mercer, Swati P., Dorsey, Bruce D., McDonough, Colleen M., Cook, Jacquelynn J., Krueger, Julie A., Lewis, S. Dale, Lucas, Bobby J., Lyle, Elizabeth A., Lynch, Joseph J., Miller-Stein, Cynthia, Michener, Maria T., Wallace, Audrey A., White, Rebecca B., and Wong, Bradley K.

Published
2011
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17. The identification of potent, orally bioavailable tricyclic CGRP receptor antagonists

Author

Bell, Ian M., Bednar, Rodney A., Corcoran, Halea A., Fay, John F., Gallicchio, Steven N., Johnston, Victor K., Hershey, James C., Miller-Stein, Cynthia M., Moore, Eric L., Mosser, Scott D., Roller, Shane A., Salvatore, Christopher A., Theberge, Cory R., Wong, Bradley K., Blair Zartman, C., Kane, Stefanie A., Williams, Theresa M., Graham, Samuel L., and Vacca, Joseph P.

Published
2009
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19. Sequential Metabolism of AMG 487, a Novel CXCR3 Antagonist, Results in Formation of Quinone Reactive Metabolites That Covalently Modify CYP3A4 Cys239 and Cause Time-Dependent Inhibition of the Enzyme

Author

Henne, Kirk R., primary, Tran, Thuy B., additional, VandenBrink, Brooke M., additional, Rock, Dan A., additional, Aidasani, Divesh K., additional, Subramanian, Raju, additional, Mason, Andrew K., additional, Stresser, David M., additional, Teffera, Yohannes, additional, Wong, Simon G., additional, Johnson, Michael G., additional, Chen, Xiaoqi, additional, Tonn, George R., additional, and Wong, Bradley K., additional

Published
2012
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20. Bioactivation of a Novel 2-Methylindole-Containing Dual Chemoattractant Receptor-Homologous Molecule Expressed on T-Helper Type-2 Cells/d-Prostanoid Receptor Antagonist Leads to Mechanism-Based CYP3A Inactivation: Glutathione Adduct Characterization and Prediction of In Vivo Drug-Drug Interaction

Author

Wong, Simon G., primary, Fan, Peter W., additional, Subramanian, Raju, additional, Tonn, George R., additional, Henne, Kirk R., additional, Johnson, Michael G., additional, Tadano Lohr, Michelle, additional, and Wong, Bradley K., additional

Published
2010
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21. An Inhibitory Metabolite Leads to Dose- and Time-Dependent Pharmacokinetics of (R)-N-{1-[3-(4-Ethoxy-phenyl)-4-oxo-3,4-dihydro-pyrido[2,3-d]pyrimidin-2-yl]-ethyl}-N-pyridin-3-yl-methyl-2-(4-trifluoromethoxy-phenyl)-acetamide (AMG 487) in Human Subjects After Multiple Dosing

Author

Tonn, George R., primary, Wong, Simon G., additional, Wong, Sylvia C., additional, Johnson, Michael G., additional, Ma, Ji, additional, Cho, Robert, additional, Floren, Leslie C., additional, Kersey, Kathryn, additional, Berry, Karen, additional, Marcus, Andrew P., additional, Wang, Xuemei, additional, Van Lengerich, Bettina, additional, Medina, Julio C., additional, Pearson, Paul G., additional, and Wong, Bradley K., additional

Published
2008
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22. Potent, Orally Bioavailable Calcitonin Gene-Related Peptide Receptor Antagonists for the Treatment of Migraine: Discovery of N-[(3R,6S)-6-(2,3-Difluorophenyl)-2-oxo-1- (2,2,2-trifluoroethyl)azepan-3-yl]-4- (2-oxo-2,3-dihydro-1H-imidazo[4,5-b]pyridin- 1-yl)piperidine-1-carboxamide (MK-0974)

Author

Paone, Daniel V., primary, Shaw, Anthony W., additional, Nguyen, Diem N., additional, Burgey, Christopher S., additional, Deng, James Z., additional, Kane, Stefanie A., additional, Koblan, Kenneth S., additional, Salvatore, Christopher A., additional, Mosser, Scott D., additional, Johnston, Victor K., additional, Wong, Bradley K., additional, Miller-Stein, Cynthia M., additional, Hershey, James C., additional, Graham, Samuel L., additional, Vacca, Joseph P., additional, and Williams, Theresa M., additional

Published
2007
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23. Pharmacokinetics and metabolism of AMG 232, a novel orally bioavailable inhibitor of the MDM2-p53 interaction, in rats, dogs and monkeys: in vitro-in vivo correlation.

Author

Ye, Qiuping, Jiang, Min, Huang, Wotang T., Ling, Yun, Olson, Steven H., Sun, Daqing, Xu, Guifen, Yan, Xuelei, Wong, Bradley K., and Jin, Lixia

Subjects
PHARMACOKINETICS, ENZYME inhibitors, DRUG metabolism, BIOAVAILABILITY, P53 protein
Abstract

1. AMG 232 is a novel inhibitor of the p53-MDM2 protein-protein interaction currently in Phase I clinical trials for multiple tumor indications. The objectives of the investigations reported in this article were to characterize the pharmacokinetic and drug metabolism properties of AMG 232 in pre-clinical species in vivo and in vitro, and in humans in vitro, and to predict its pharmacokinetics in humans through integrating PKDM data. 2. AMG 232 exhibited low clearance (<0.25 × Qh) and moderate to high oral bioavailability in mice, rats and monkeys (>42%), but high clearance (0.74 × Qh) and low oral exposure in dogs (18%). 3. Biotransformation was the major route of elimination of AMG 232 in rats, with only 7% of intravenously administered 14C-labeled AMG 232 recovered as parent molecule in bile. The major metabolite was an acyl glucuronide as measured by in vivo rat studies and in vitro hepatocyte incubations in multiple species. 4. The in vitro-in vivo correlation of AMG 232 clearance was within 2-fold in pre-clinical species using hepatocytes. AMG 232 was predicted to exhibit low clearance, high volume distribution and long half-life in humans. The predictions are consistent with the preliminary human pharmacokinetic parameters of AMG 232 in clinical trials. [ABSTRACT FROM AUTHOR]

Published
2015
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24. Identification of novel, orally bioavailable spirohydantoin CGRP receptor antagonists

Author

Bell, Ian M., primary, Bednar, Rodney A., additional, Fay, John F., additional, Gallicchio, Steven N., additional, Hochman, Jerome H., additional, McMasters, Daniel R., additional, Miller-Stein, Cynthia, additional, Moore, Eric L., additional, Mosser, Scott D., additional, Pudvah, Nicole T., additional, Quigley, Amy G., additional, Salvatore, Christopher A., additional, Stump, Craig A., additional, Theberge, Cory R., additional, Wong, Bradley K., additional, Zartman, C. Blair, additional, Zhang, Xu-Fang, additional, Kane, Stefanie A., additional, Graham, Samuel L., additional, Vacca, Joseph P., additional, and Williams, Theresa M., additional

Published
2006
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25. Potent 2-[(pyrimidin-4-yl)amine}-1,3-thiazole-5-carbonitrile-based inhibitors of VEGFR-2 (KDR) kinase

Author

Sisko, John T., primary, Tucker, Thomas J., additional, Bilodeau, Mark T., additional, Buser, Carolyn A., additional, Ciecko, Patrice A., additional, Coll, Kathleen E., additional, Fernandes, Christine, additional, Gibbs, Jackson B., additional, Koester, Timothy J., additional, Kohl, Nancy, additional, Lynch, Joseph J., additional, Mao, Xianzhi, additional, McLoughlin, Debra, additional, Miller-Stein, Cynthia M., additional, Rodman, Leonard D., additional, Rickert, Keith W., additional, Sepp-Lorenzino, Laura, additional, Shipman, Jennifer M., additional, Thomas, Kenneth A., additional, Wong, Bradley K., additional, and Hartman, George D., additional

Published
2006
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26. A series of 5-(5,6)-dihydrouracil substituted 8-hydroxy-[1,6]naphthyridine-7-carboxylic acid 4-fluorobenzylamide inhibitors of HIV-1 integrase and viral replication in cells

Author

Embrey, Mark W., primary, Wai, John S., additional, Funk, Timothy W., additional, Homnick, Carl F., additional, Perlow, Debbie S., additional, Young, Steven D., additional, Vacca, Joseph P., additional, Hazuda, Daria J., additional, Felock, Peter J., additional, Stillmock, Kara A., additional, Witmer, Marc V., additional, Moyer, Gregory, additional, Schleif, William A., additional, Gabryelski, Lori J., additional, Jin, Lixia, additional, Chen, I-Wu, additional, Ellis, Joan D., additional, Wong, Bradley K., additional, Lin, Jiunn H., additional, Leonard, Yvonne M., additional, Tsou, Nancy N., additional, and Zhuang, Linghang, additional

Published
2005
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27. Potent N-(1,3-Thiazol-2-yl)pyridin-2-amine Vascular Endothelial Growth Factor Receptor Tyrosine Kinase Inhibitors with Excellent Pharmacokinetics and Low Affinity for the hERG Ion Channel

Author

Bilodeau, Mark T., primary, Balitza, Adrienne E., additional, Koester, Timothy J., additional, Manley, Peter J., additional, Rodman, Leonard D., additional, Buser-Doepner, Carolyn, additional, Coll, Kathleen E., additional, Fernandes, Christine, additional, Gibbs, Jackson B., additional, Heimbrook, David C., additional, Huckle, William R., additional, Kohl, Nancy, additional, Lynch, Joseph J., additional, Mao, Xianzhi, additional, McFall, Rosemary C., additional, McLoughlin, Debra, additional, Miller-Stein, Cynthia M., additional, Rickert, Keith W., additional, Sepp-Lorenzino, Laura, additional, Shipman, Jennifer M., additional, Subramanian, Raju, additional, Thomas, Kenneth A., additional, Wong, Bradley K., additional, Yu, Sean, additional, and Hartman, George D., additional

Published
2004
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28. Low molecular weight thrombin inhibitors with excellent potency, metabolic stability, and oral bioavailability

Author

Morrissette, Matthew M, primary, Stauffer, Kenneth J, additional, Williams, Peter D, additional, Lyle, Terry A, additional, Vacca, Joseph P, additional, Krueger, Julie A, additional, Lewis, S.Dale, additional, Lucas, Bobby J, additional, Wong, Bradley K, additional, White, Rebecca B, additional, Miller-Stein, Cynthia, additional, Lyle, Elizabeth A, additional, Wallace, Audrey A, additional, Leonard, Yvonne M, additional, Welsh, Denise C, additional, Lynch, Joseph J, additional, and McMasters, Daniel R, additional

Published
2004
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29. Optimization of the indolyl quinolinone class of KDR (VEGFR-2) kinase inhibitors

Author

Fraley, Mark E., primary, Arrington, Kenneth L., additional, Buser, Carolyn A., additional, Ciecko, Patrice A., additional, Coll, Kathleen E., additional, Fernandes, Christine, additional, Hartman, George D., additional, Hoffman, William F., additional, Lynch, Joseph J., additional, McFall, Rosemary C., additional, Rickert, Keith, additional, Singh, Romi, additional, Smith, Sheri, additional, Thomas, Kenneth A., additional, and Wong, Bradley K., additional

Published
2004
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30. Metabolic Activation of a Pyrazinone-Containing Thrombin Inhibitor. Evidence for Novel Biotransformation Involving Pyrazinone Ring Oxidation, Rearrangement, and Covalent Binding to Proteins

Author

Singh, Rominder, primary, Silva Elipe, Maria V., additional, Pearson, Paul G., additional, Arison, Byron H., additional, Wong, Bradley K., additional, White, Rebecca, additional, Yu, Xiao, additional, Burgey, Christopher S., additional, Lin, Jiunn H., additional, and Baillie, Thomas A., additional

Published
2003
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31. Design and Synthesis of a Pro-Drug of Vinblastine Targeted at Treatment of Prostate Cancer with Enhanced Efficacy and Reduced Systemic Toxicity

Author

Brady, Stephen F., primary, Pawluczyk, Joseph M., additional, Lumma, Patricia K., additional, Feng, Dong-Mei, additional, Wai, Jenny M., additional, Jones, Raymond, additional, DeFeo-Jones, Deborah, additional, Wong, Bradley K., additional, Miller-Stein, Cynthia, additional, Lin, Jiunn H., additional, Oliff, Allen, additional, Freidinger, Roger M., additional, and Garsky, Victor M., additional

Published
2002
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35. A peptide?doxorubicin 'prodrug' activated by prostate-specific antigen selectively kills prostate tumor cells positive for prostate-specific antigen in vivo.

Author

DeFeo-Jones, Deborah, Garsky, Victor M., Wong, Bradley K., Feng, Dong-Mei, Bolyar, Trina, Haskell, Kathleen, Kiefer, David M., Leander, Karen, McAvoy, Elizabeth, Lumma, Patricia, Wai, Jenny, Senderak, Edith T., Motzel, Sherri L., Keenan, Kevin, Zwieten, Matthew Van, Lin, Jiunn H., Freidinger, Roger, Huff, Joel, and Oliff, Allen

Subjects
DOXORUBICIN, PROSTATE-specific antigen
Abstract

We covalently linked doxorubicin with a peptide that is hydrolyzable by prostate-specific antigen. In the presence of prostate tumor cells secreting prostate-specific antigen, the peptide moiety of this conjugate, L-377,202, was hydrolyzed, resulting in the release of leucine-doxorubicin and doxorubicin, which are both very cytotoxic to cancer cells. However, L-377,202 was much less cytotoxic than conventional doxorubicin to cells in culture that do not secrete prostate-specific antigen. L-377,202 was approximately 15 times more effective than was conventional doxorubicin at inhibiting the growth of human prostate cancer tumors in nude mice when both drugs were used at their maximally tolerated doses. Nude mice inoculated with human prostate tumor cells secreting prostate-specific antigen showed considerable reductions in tumor burden with minimal total body weight loss when treated with L-377,202. This improvement in therapeutic index correlated with the selective localization of leucine-doxorubicin and free doxorubicin in tissues secreting prostate-specific antigen after exposure to L-377,202. [ABSTRACT FROM AUTHOR]

Published
2000
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36. Deletion of Abcg2Has Differential Effects on Excretion and Pharmacokinetics of Probe Substrates in Rats

Author

Huang, Liyue, Be, Xuhai, Tchaparian, Eskouhie H., Colletti, Adria E., Roberts, Jonathan, Langley, Meghan, Ling, Yun, Wong, Bradley K., and Jin, Lixia

Abstract

This study was designed to characterize breast cancer resistance protein (Bcrp) knockout Abcg2(−/−) rats and assess the effect of ATP-binding cassette subfamily G member 2 (Abcg2) deletion on the excretion and pharmacokinetic properties of probe substrates. Deletion of the target gene in the Abcg2(−/−) rats was confirmed, whereas gene expression was unaffected for most of the other transporters and metabolizing enzymes. Biliary excretion of nitrofurantoin, sulfasalazine, and compound A [2-(5-methoxy-2-((2-methyl-1,3-benzothiazol-6-yl)amino)-4-pyridinyl)-1,5,6,7-tetrahydro-4H-pyrrolo[3,2-c]pyridin-4-one] accounted for 1.5, 48, and 48% of the dose in the Abcg2(+/+) rats, respectively, whereas it was decreased by 70 to 90% in the Abcg2(−/−) rats. Urinary excretion of nitrofurantoin, a significant elimination pathway, was unaffected in the Abcg2(−/−) rats, whereas renal clearance of sulfasalazine, a minor elimination pathway, was reduced by >90%. Urinary excretion of compound A was minimal. Systemic clearance in the Abcg2(−/−) rats decreased 22, 43 (p< 0.05), and 57%, respectively, for nitrofurantoin, sulfasalazine, and compound A administered at 1 mg/kg and 27% for compound A administered at 5 mg/kg. Oral absorption of nitrofurantoin, a compound with high aqueous solubility and good permeability, was not limited by Bcrp. In contrast, the absence of Bcrp led to a 33- and 11-fold increase in oral exposure of sulfasalazine and compound A, respectively. These data show that Bcrp plays a crucial role in biliary excretion of these probe substrates and has differential effects on systemic clearance and oral absorption in rats depending on clearance mechanisms and compound properties. The Abcg2(−/−) rat is a useful model for understanding the role of Bcrp in elimination and oral absorption.

Published
2012
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37. Deletion of Abcg2 has differential effects on excretion and pharmacokinetics of probe substrates in rats.

Author

Huang, Liyue, Be, Xuhai, Tchaparian, Eskouhie H, Colletti, Adria E, Roberts, Jonathan, Langley, Meghan, Ling, Yun, Wong, Bradley K, and Jin, Lixia

Abstract

This study was designed to characterize breast cancer resistance protein (Bcrp) knockout Abcg2(-/-) rats and assess the effect of ATP-binding cassette subfamily G member 2 (Abcg2) deletion on the excretion and pharmacokinetic properties of probe substrates. Deletion of the target gene in the Abcg2(-/-) rats was confirmed, whereas gene expression was unaffected for most of the other transporters and metabolizing enzymes. Biliary excretion of nitrofurantoin, sulfasalazine, and compound A [2-(5-methoxy-2-((2-methyl-1,3-benzothiazol-6-yl)amino)-4-pyridinyl)-1,5,6,7-tetrahydro-4H-pyrrolo[3,2-c]pyridin-4-one] accounted for 1.5, 48, and 48% of the dose in the Abcg2(+/+) rats, respectively, whereas it was decreased by 70 to 90% in the Abcg2(-/-) rats. Urinary excretion of nitrofurantoin, a significant elimination pathway, was unaffected in the Abcg2(-/-) rats, whereas renal clearance of sulfasalazine, a minor elimination pathway, was reduced by >90%. Urinary excretion of compound A was minimal. Systemic clearance in the Abcg2(-/-) rats decreased 22, 43 (p<0.05), and 57%, respectively, for nitrofurantoin, sulfasalazine, and compound A administered at 1 mg/kg and 27% for compound A administered at 5 mg/kg. Oral absorption of nitrofurantoin, a compound with high aqueous solubility and good permeability, was not limited by Bcrp. In contrast, the absence of Bcrp led to a 33- and 11-fold increase in oral exposure of sulfasalazine and compound A, respectively. These data show that Bcrp plays a crucial role in biliary excretion of these probe substrates and has differential effects on systemic clearance and oral absorption in rats depending on clearance mechanisms and compound properties. The Abcg2(-/-) rat is a useful model for understanding the role of Bcrp in elimination and oral absorption.

Published
2012
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38. An Inhibitory Metabolite Leads to Dose- and Time-Dependent Pharmacokinetics of (R)-N-{1-[3-(4-Ethoxy-phenyl)-4-oxo-3,4-dihydro-pyrido[2,3-d]pyrimidin-2-yl]-ethyl}-N-pyridin-3-yl-methyl-2-(4-trifluoromethoxy-phenyl)-acetamide (AMG 487) in Human Subjects After Multiple Dosing

Author

Tonn, George R., Wong, Simon G., Wong, Sylvia C., Johnson, Michael G., Ma, Ji, Cho, Robert, Floren, Leslie C., Kersey, Kathryn, Berry, Karen, Marcus, Andrew P., Wang, Xuemei, Van Lengerich, Bettina, Medina, Julio C., Pearson, Paul G., and Wong, Bradley K.

Abstract

(R)-N-{1-[3-(4-Ethoxy-phenyl)-4-oxo-3,4-dihydro-pyrido[2,3-d]-pyrimidin-2-yl]-ethyl}-N-pyridin-3-yl-methyl-2-(4-trifluoromethoxyphenyl)-acetamide (AMG 487) is a potent and selective orally bioavailable chemokine (C-X-C motif) receptor 3 (CXCR3) antagonist that displays dose- and time-dependent pharmacokinetics in human subjects after multiple oral dosing. Although AMG 487 exhibited linear pharmacokinetics on both days 1 and 7 at the 25-mg dose, dose- and time-dependent kinetics were evident at the two higher doses. Nonlinear kinetics were more pronounced after multiple dosing. Area under the plasma concentration-time curve from 0 to 24 h [AUC(0–24 h)] increased 96-fold with a 10-fold increase in dose on day 7 compared with a 28-fold increase in AUC(0–24 h)on day 1. These changes were correlated with time- and dose-dependent decreases in the metabolite to parent plasma concentrations, suggesting that these changes result from a decrease in the oral clearance (CL) of AMG 487 (e.g., intestinal/hepatic first-pass metabolism and systemic CL). The biotransformation of AMG 487 is dependent on CYP3A and results in the formation of two primary metabolites, a pyridyl N-oxide AMG 487 (M1) and an O-deethylated AMG 487 (M2). One of these metabolites, M2, undergoes further metabolism by CYP3A. M2 has also been demonstrated to inhibit CYP3A in a competitive (Ki= 0.75 µM) manner as well as via mechanism-based inhibition (unbound KI= 1.4 µM, kinact= 0.041 min–1). Data from this study implicate M2-mediated CYP3A mechanism-based inhibition as the proximal cause for the time-dependent pharmacokinetics of AMG 487. However, the sequential metabolism of M2, nonlinear AMG 487 pharmacokinetics, and the inability to accurately determine the role of intestinal AMG 487 metabolism complicates the correlation between M2 plasma concentrations and the time-dependent AMG 487 pharmacokinetic changes.

Published
2009

39. Complexities of Glucuronidation Affecting In Vitro-In Vivo Extrapolation

Author

Lin, Jiunn H. and Wong, Bradley K.

Abstract

Glucuronidation is responsible for the clearance of a diverse range of drug and chemicals whose topology confers properties that complicate in vitro-in vivo clearance correlations as compared to those possible for oxidative metabolism. The active site of the UGTs faces the inside of the luminal space of the endoplasmic reticulum, thus presenting diffusional barriers for substrates, the cosubstrate, UDPGA, and resultant glucuronide products. Transport processes for the cosubstrate UDPGA and glucuronidated products likely contribute to the well-known latency phenomena in which exogenous detergents or alamethicin are required for maximal UGT activity in microsomes. This complicates the extrapolation of results of in vitro clearance studies to the in vivo situation. Even with activation, the microsomal-based clearance values still underestimate the actual in vivo UGT-mediated clearance; therefore latency is not the only explanation for the poor correlation. Recent data indicate that hepatocytes are a promising in vitro system that can be used for the early evaluation of human clearance behavior of drug candidates. Both induction and inhibition of UGT-mediated clearance are a source of clinical drug-drug interactions. Emerging evidence indicates that the same mechanisms identified in the regulation of CYP enzymes also are involved in regulation of the UGTs, i.e., CAR, AH and probably PXR mediate regulation of UGT1A1, 1A6 and UGT2B7, respectively. In contrast to CYP-mediated interactions, with a few exceptions, the magnitude of UGT-mediated interactions are less than 2-fold because of the relatively high UGT Km values and substrate overlap among the multiple isozymes.

Published
2002

40. Pharmacokinetics and Metabolism of a RasFarnesyl Transferase Inhibitor in Rats and Dogs: In Vitro-In Vivo Correlation

Author

Singh, Rominder, Chen, I-Wu, Jin, Lixia, Silva, Maria V., Arison, Byron H., Lin, Jiunn H., and Wong, Bradley K.

Abstract

Compound I (1-(3-chlorophenyl)-4-[(1-(4-cyanobenzyl)-1H-imidazol-5-yl)methyl]piperazin-2-one) is a potent and selective inhibitor of farnesyl-protein transferase (FPTase). The pharmacokinetics and metabolism of compound I displayed species differences in rats and dogs. After oral administration, the drug was well absorbed in dogs but less so in rats. Following i.v. administration, compound I was cleared rapidly in rats in a polyphasic manner with a terminal t1/2of 41 min. The plasma clearance (CLp) and volume of distribution (Vdss) were 41.2 ml/min/kg and 1.2 l/kg, respectively. About 1% of the dose was excreted in rat bile and urine as unchanged drug over a period of 24 h, suggesting that biotransformation is the major route of elimination of compound I . Using liquid chromatography (LC)-tandem mass spectometry, nineteen metabolites of compound I were identified in urine and bile from dogs and rats. Structures of two major metabolites were confirmed by LC-NMR. N-Dealkylation and phase II metabolism were the major metabolic pathways. Animal and human liver microsomal intrinsic clearance values were scaled to predict hepatic clearance and half-life in humans, and the predicted values were in good agreement to the in vivo data.

Published
2001
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41. PSA-Specific and Non-PSA-Specific Conversion of a PSA-Targeted Peptide Conjugate of Doxorubicin to Its Active Metabolites

Author

Wong, Bradley K., DeFeo-Jones, Deborah, Jones, Raymond E., Garsky, Victor M., Feng, Dong-Mei, Oliff, Allen, Chiba, Masato, Ellis, Joan D., and Lin, Jiunn H.

Abstract

Tumor-selective delivery of doxorubicin by a prostate-specific antigen (PSA)-targeted peptide conjugate prodrug of doxorubicin was demonstrated in a nude mouse xenograft model of human prostate cancer. The prodrug (referred to as doxorubicin conjugate) contains doxorubicin linked to a seven-amino acid peptide conjugate that was designed to increase delivery of doxorubicin to tumor sites through the hydrolytic properties of PSA, which prostate tumors express in high amounts. Following i.p. administration of the doxorubicin conjugate to mice, tumor exposure to doxorubicin was increased 2.5-fold as compared with that achieved after an equimolar dose of doxorubicin itself. However, in heart tissue, the site of clinical dose-limiting toxicity, doxorubicin concentrations observed after administration of doxorubicin conjugate were substantially lower than those in mice that received doxorubicin itself. While the prodrug provided selective delivery of doxorubicin to tumor tissue, there was substantial non-PSA-specific formation of doxorubicin in laboratory animals, a factor that would limit the extent of therapeutic gain of the prodrug. Following i.v. administration to mice, rats, dogs, and monkeys, about one-third of the dose was metabolized to doxorubicin. In tumor-bearing mice, the fraction of the dose metabolized to doxorubicin appeared even higher. This is likely the result of conjugate conversion to doxorubicin by both PSA-specific (in tumor) and non-PSA-specific proteolytic activities. In vitro studies provided further support for the PSA specificity of metabolism; LNCaP cells mediated rapid metabolism of the conjugate, while DuPRO-1 cells, which are deficient in PSA, were incapable of metabolism.

Published
2001
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42. Enzyme Kinetics of Cytochrome P450-Mediated Reactions

Author

Shou, Magang, Lin, Yuh, Lu, Ping, Tang, Cuyue, Mei, Qin, Cui, Dan, Tang, Wei, Ngui, Jason S., Lin, C. Charles, Singh, Rominder, Wong, Bradley K., Yergey, James A., Lin, Jiunn H., Pearson, Paul G., Baillie, Thomas A., Rodrigues, A. David, and Rushmore, Thomas H.

Abstract

The most common drug-drug interactions may be understood in terms of alterations of metabolism, associated primarily with changes in the activity of cytochrome P450 (CYP) enzymes. Kinetic parameters such as K m , V max , K i and K a , which describe metabolism-based drug interactions, are usually determined by appropriate kinetic models and may be used to predict the pharmacokinetic consequences of exposure to one or multiple drugs. According to classic Michaelis-Menten (M-M) kinetics, one binding site models can be employed to simply interpret inhibition (pure competitive, non-competitive and uncompetitive) or activation of the enzyme. However, some cytochromes P450, in particular CYP3A4, exhibit unusual kinetic characteristics. In this instance, the changes in apparent kinetic constants in the presence of inhibitor or activator or second substrate do not obey the rules of M-M kinetics, and the resulting kinetics are not straightforward and hamper mechanistic interpretation of the interaction in question. These unusual kinetics include substrate activation (autoactivation), substrate inhibition, partial inhibition, activation, differential kinetics and others. To address this problem, several kinetic models can be proposed, based upon the assumption that multiple substrate binding sites exist at the active site of a particular P450, and the resulting kinetic constants are, therefore, solved to adequately describe the observed interaction between multiple drugs. The following is an overview of some cytochrome P450-mediated classic and atypical enzyme kinetics, and the associated kinetic models. Applications of these kinetic models can provide some new insights into the mechanism of P450-mediated drug-drug interactions.

Published
2001

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