Your search keyword '"Terry Podoll"' showing total 3 results

1. Bioavailability, Biotransformation, and Excretion of the Covalent Bruton Tyrosine Kinase Inhibitor Acalabrutinib in Rats, Dogs, and Humans

Author

Mark Gohdes, J. Greg Slatter, Tim Ingallinera, Hao Sun, Paul G. Pearson, Jerry Evarts, Terry Podoll, Mitesh Sanghvi, Elena Bibikova, and Kristen Cardinal

Subjects

Adult, Male, Administration, Oral, Biological Availability, Pharmaceutical Science, Antineoplastic Agents, Lymphoma, Mantle-Cell, Urine, Pharmacology, 030226 pharmacology & pharmacy, Intestinal absorption, Rats, Sprague-Dawley, Excretion, Feces, Young Adult, 03 medical and health sciences, chemistry.chemical_compound, Dogs, 0302 clinical medicine, Biotransformation, Agammaglobulinaemia Tyrosine Kinase, Animals, Cytochrome P-450 CYP3A, Humans, Bruton's tyrosine kinase, Protein Kinase Inhibitors, biology, Chemistry, Hydrolysis, Middle Aged, Healthy Volunteers, Rats, Bioavailability, Intestinal Absorption, Covalent bond, Pyrazines, 030220 oncology & carcinogenesis, Acrylamide, Benzamides, biology.protein, Acalabrutinib, Female, Oxidation-Reduction, Half-Life

Abstract

Acalabrutinib is a targeted, covalent inhibitor of Bruton tyrosine kinase (BTK) with a unique 2-butynamide warhead that has relatively lower reactivity than other marketed acrylamide covalent inhibitors. A human [14C] microtracer bioavailability study in healthy subjects revealed moderate intravenous clearance (39.4 l/h) and an absolute bioavailability of 25.3% ± 14.3% (n = 8). Absorption and elimination of acalabrutinib after a 100 mg [14C] microtracer acalabrutinib oral dose was rapid, with the maximum concentration reached in

Published

2018

2. IN VITRO METABOLISM OF CLINDAMYCIN IN HUMAN LIVER AND INTESTINAL MICROSOMES

Author

Larry C. Wienkers, Michael A. Wynalda, Terry Podoll, J. Matthew Hutzler, and Michael D. Koets

Subjects

CYP3A, Metabolite, Statistics as Topic, Pharmaceutical Science, Pharmacology, Mixed Function Oxygenases, chemistry.chemical_compound, Cytochrome P-450 Enzyme System, Microsomes, medicine, Cytochrome P-450 CYP3A, Cytochrome P-450 Enzyme Inhibitors, Humans, Enzyme Inhibitors, Antibacterial agent, biology, CYP3A4, Clindamycin, Cytochrome P450, Monooxygenase, Recombinant Proteins, Intestines, chemistry, Sulfoxides, Microsomes, Liver, Oxygenases, biology.protein, Microsome, medicine.drug

Abstract

Incubations with human liver and gut microsomes revealed that the antibiotic, clindamycin, is primarily oxidized to form clindamycin sulfoxide. In this report, evidence is presented that the S-oxidation of clindamycin is primarily mediated by CYP3A. This conclusion is based upon several lines of in vitro evidence, including the following. 1) Incubations with clindamycin in hepatic microsomes from a panel of human donors showed that clindamycin sulfoxide formation correlated with CYP3A-catalyzed testosterone 6beta-hydroxylase activity; 2) coincubation with ketaconazole, a CYP3A4-specific inhibitor, markedly inhibited clindamycin S-oxidase activity; and 3) when clindamycin was incubated across a battery of recombinant heterologously expressed human cytochrome P450 (P450) enzymes, CYP3A4 possessed the highest clindamycin S-oxidase activity. A potential role for flavin-containing monooxygenases (FMOs) in clindamycin S-oxidation in human liver was also evaluated. Formation of clindamycin sulfoxide in human liver microsomes was unaffected either by heat pretreatment or by chemical inhibition (e.g., methimazole). Furthermore, incubations with recombinant FMO isoforms revealed no detectable activity toward the formation of clindamycin sulfoxide. Beyond identifying the drug-metabolizing enzyme responsible for clindamycin S-oxidation, the ability of clindamycin to inhibit six human P450 enzymes was also evaluated. Of the P450 enzymes examined, only the activity of CYP3A4 was inhibited (approximately 26%) by coincubation with clindamycin (100 microM). Thus, it is concluded that CYP3A4 appears to account for the largest proportion of the observed P450 catalytic clindamycin S-oxidase activity in vitro, and this activity may be extrapolated to the in vivo condition.

Published

2003

3. In vitro metabolism of clindamycin in human liver and intestinal microsomes.

Author

A, Wynalda Michael, Matthew, Hutzler J, D, Koets Michael, Terry, Podoll, and C, Wienkers Larry

Abstract

Incubations with human liver and gut microsomes revealed that the antibiotic, clindamycin, is primarily oxidized to form clindamycin sulfoxide. In this report, evidence is presented that the S-oxidation of clindamycin is primarily mediated by CYP3A. This conclusion is based upon several lines of in vitro evidence, including the following. 1) Incubations with clindamycin in hepatic microsomes from a panel of human donors showed that clindamycin sulfoxide formation correlated with CYP3A-catalyzed testosterone 6beta-hydroxylase activity; 2) coincubation with ketaconazole, a CYP3A4-specific inhibitor, markedly inhibited clindamycin S-oxidase activity; and 3) when clindamycin was incubated across a battery of recombinant heterologously expressed human cytochrome P450 (P450) enzymes, CYP3A4 possessed the highest clindamycin S-oxidase activity. A potential role for flavin-containing monooxygenases (FMOs) in clindamycin S-oxidation in human liver was also evaluated. Formation of clindamycin sulfoxide in human liver microsomes was unaffected either by heat pretreatment or by chemical inhibition (e.g., methimazole). Furthermore, incubations with recombinant FMO isoforms revealed no detectable activity toward the formation of clindamycin sulfoxide. Beyond identifying the drug-metabolizing enzyme responsible for clindamycin S-oxidation, the ability of clindamycin to inhibit six human P450 enzymes was also evaluated. Of the P450 enzymes examined, only the activity of CYP3A4 was inhibited (approximately 26%) by coincubation with clindamycin (100 microM). Thus, it is concluded that CYP3A4 appears to account for the largest proportion of the observed P450 catalytic clindamycin S-oxidase activity in vitro, and this activity may be extrapolated to the in vivo condition.

Published

2003