Your search keyword '"Good SS"' showing total 29 results

1. Bemnifosbuvir (BEM, AT-527), a novel nucleotide analogue inhibitor of the hepatitis C virus NS5B polymerase.

Author

Zhou XJ, Good SS, Pietropaolo K, Huang Q, Moussa A, Hammond JM, and Sommadossi JP

Subjects

Humans, Hepacivirus, Antiviral Agents adverse effects, Sofosbuvir pharmacology, Sofosbuvir therapeutic use, Genotype, Drug Therapy, Combination, Viral Nonstructural Proteins, Hepatitis C, Chronic drug therapy, Hepatitis C drug therapy, Guanosine Monophosphate analogs & derivatives, Phosphoramides

Abstract

Introduction: Chronic hepatitis C virus (HCV) persists as a public health concern worldwide. Consequently, optimizing HCV therapy remains an important objective. While current therapies are generally highly effective, advanced antiviral agents are needed to maximize cure rates with potentially shorter treatment durations in a broader patient population, particularly those patients with advanced diseases who remain difficult to treat., Areas Covered: This review summarizes the in vitro anti-HCV activity, preclinical pharmacological properties of bemnifosbuvir (BEM, AT-527), a novel prodrug that is metabolically converted to AT-9010, the active guanosine triphosphate analogue that potently and selectively inhibits several viral RNA polymerases, including the HCV NS5B polymerase. Results from clinical proof-of-concept and phase 2 combination studies are also discussed., Expert Opinion: BEM exhibits potent pan-genotype activity against HCV, and has favorable safety, and drug interaction profiles. BEM is approximately 10-fold more potent than sofosbuvir against HCV genotypes (GT) tested in vitro. When combined with a potent NS5A inhibitor, BEM is expected to be a promising once-daily oral antiviral for chronic HCV infection of all genotypes and fibrosis stages with potentially short treatment durations.

Published

2024

2. A dual mechanism of action of AT-527 against SARS-CoV-2 polymerase.

Author

Shannon A, Fattorini V, Sama B, Selisko B, Feracci M, Falcou C, Gauffre P, El Kazzi P, Delpal A, Decroly E, Alvarez K, Eydoux C, Guillemot JC, Moussa A, Good SS, La Colla P, Lin K, Sommadossi JP, Zhu Y, Yan X, Shi H, Ferron F, and Canard B

Subjects

COVID-19 virology, Cryoelectron Microscopy, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Guanosine Monophosphate chemistry, Guanosine Monophosphate pharmacology, Humans, RNA-Dependent RNA Polymerase chemistry, RNA-Dependent RNA Polymerase genetics, RNA-Dependent RNA Polymerase metabolism, SARS-CoV-2 chemistry, SARS-CoV-2 drug effects, SARS-CoV-2 genetics, Viral Proteins genetics, Antiviral Agents chemistry, Antiviral Agents pharmacology, Guanosine Monophosphate analogs & derivatives, Phosphoramides chemistry, Phosphoramides pharmacology, RNA-Dependent RNA Polymerase antagonists & inhibitors, SARS-CoV-2 enzymology, Viral Proteins antagonists & inhibitors, Viral Proteins metabolism

Abstract

The guanosine analog AT-527 represents a promising candidate against Severe Acute Respiratory Syndrome coronavirus type 2 (SARS-CoV-2). AT-527 recently entered phase III clinical trials for the treatment of COVID-19. Once in cells, AT-527 is converted into its triphosphate form, AT-9010, that presumably targets the viral RNA-dependent RNA polymerase (RdRp, nsp12), for incorporation into viral RNA. Here we report a 2.98 Å cryo-EM structure of the SARS-CoV-2 nsp12-nsp7-nsp8 2 -RNA complex, showing AT-9010 bound at three sites of nsp12. In the RdRp active-site, one AT-9010 is incorporated at the 3' end of the RNA product strand. Its modified ribose group (2'-fluoro, 2'-methyl) prevents correct alignment of the incoming NTP, in this case a second AT-9010, causing immediate termination of RNA synthesis. The third AT-9010 is bound to the N-terminal domain of nsp12 - known as the NiRAN. In contrast to native NTPs, AT-9010 is in a flipped orientation in the active-site, with its guanine base unexpectedly occupying a previously unnoticed cavity. AT-9010 outcompetes all native nucleotides for NiRAN binding, inhibiting its nucleotidyltransferase activity. The dual mechanism of action of AT-527 at both RdRp and NiRAN active sites represents a promising research avenue against COVID-19., (© 2022. The Author(s).)

Published

2022

3. AT-752, a double prodrug of a guanosine nucleotide analog, inhibits yellow fever virus in a hamster model.

Author

Lin K, Good SS, Julander JG, Weight AE, Moussa A, and Sommadossi JP

Subjects

Animals, Antiviral Agents chemistry, Antiviral Agents pharmacokinetics, Chlorocebus aethiops, Cricetinae, Female, Male, Mesocricetus, Prodrugs chemistry, Prodrugs pharmacokinetics, Vero Cells, Viremia, Yellow Fever virology, Antiviral Agents pharmacology, Guanosine analogs & derivatives, Prodrugs pharmacology, Yellow Fever drug therapy, Yellow fever virus drug effects

Abstract

Yellow fever virus (YFV) is a zoonotic pathogen re-emerging in parts of the world, causing a viral hemorrhagic fever associated with high mortality rates. While an effective vaccine is available, having an effective antiviral against YFV is critical against unexpected outbreaks, or when vaccination is not recommended. We have previously identified AT-281, the free base of AT-752, an orally available double prodrug of a guanosine nucleotide analog, as a potent inhibitor of YFV in vitro, with a 50% effective concentration (EC50) of 0.31 μM. In hamsters infected with YFV (Jimenez strain), viremia rose about 4 log10-fold and serum alanine aminotransferase (ALT) 2-fold compared to sham-infected animals. Treatment with 1000 mg/kg AT-752 for 7 days, initiated 4 h prior to viral challenge, reduced viremia to below the limit of detection by day 4 post infection (pi) and returned ALT to normal levels by day 6 pi. When treatment with AT-752 was initiated 2 days pi, the virus titer and ALT dropped >2 log10 and 53% by day 4 and 6 pi, respectively. In addition, at 21 days pi, 70-100% of the infected animals in the treatment groups survived compared to 0% of the untreated group (p<0.001). Moreover, in vivo formation of the active triphosphate metabolite AT-9010 was measured in the animal tissues, with the highest concentrations in liver and kidney, organs that are vulnerable to the virus. The demonstrated in vivo activity of AT-752 suggests that it is a promising compound for clinical development in the treatment of YFV infection., Competing Interests: I have read the journal’s policy and the authors of this manuscript have the following competing interests: KL, AM and JS are employees of Atea Pharmaceuticals, Inc. and SG is a consultant for Atea Pharmaceuticals, Inc.

Published

2022

4. Evaluation of AT-752, a Double Prodrug of a Guanosine Nucleotide Analog with In Vitro and In Vivo Activity against Dengue and Other Flaviviruses.

Author

Good SS, Shannon A, Lin K, Moussa A, Julander JG, La Colla P, Collu G, Canard B, and Sommadossi JP

Subjects

Animals, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Guanosine pharmacology, Guanosine therapeutic use, Leukocytes, Mononuclear, Mice, Nucleotides therapeutic use, Rats, Virus Replication, Dengue drug therapy, Dengue Virus, Flavivirus, Prodrugs pharmacology, Prodrugs therapeutic use

Abstract

Every year, millions of people worldwide are infected with dengue virus (DENV), with a significant number developing severe life-threatening disease. There are currently no broadly indicated vaccines or therapeutics available for treatment of DENV infection. Here, we show that AT-281, the free base of AT-752, an orally available double prodrug of a guanosine nucleotide analog, was a potent inhibitor of DENV serotypes 2 and 3 in vitro , requiring concentrations of 0.48 and 0.77 μM, respectively, to inhibit viral replication by 50% (EC 50 ) in Huh-7 cells. AT-281 was also a potent inhibitor of all other flaviviruses tested, with EC 50 values ranging from 0.19 to 1.41 μM. Little to no cytotoxicity was observed for AT-281 at concentrations up to 170 μM. After oral administration of AT-752, substantial levels of the active triphosphate metabolite AT-9010 were formed in vivo in peripheral blood mononuclear cells of mice, rats, and monkeys. Furthermore, AT-9010 competed with GTP in RNA template-primer elongation assays with DENV2 RNA polymerase, which is essential for viral replication, with incorporation of AT-9010 resulting in termination of RNA synthesis. In AG129 mice infected with DENV D2Y98P, treatment with AT-752 significantly reduced viremia and morbidity and increased survival. The demonstrated in vitro and in vivo activity of AT-752 suggests that it is a promising compound for the treatment of dengue virus infection and is currently under evaluation in clinical studies.

Published

2021

5. AT-527, a Double Prodrug of a Guanosine Nucleotide Analog, Is a Potent Inhibitor of SARS-CoV-2 In Vitro and a Promising Oral Antiviral for Treatment of COVID-19.

Author

Good SS, Westover J, Jung KH, Zhou XJ, Moussa A, La Colla P, Collu G, Canard B, and Sommadossi JP

Subjects

Administration, Oral, Animals, COVID-19 virology, Cell Line, Cell Line, Tumor, Chlorocebus aethiops, Coronavirus 229E, Human metabolism, Coronavirus OC43, Human metabolism, Cricetinae, Epithelial Cells virology, Guanosine Monophosphate pharmacology, Humans, Lung virology, SARS-CoV-2 metabolism, Vero Cells, Virus Replication drug effects, Antiviral Agents pharmacology, Guanosine pharmacology, Guanosine Monophosphate analogs & derivatives, Phosphoramides pharmacology, Prodrugs pharmacology, SARS-CoV-2 drug effects, COVID-19 Drug Treatment

Abstract

The impact of severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2), the causative agent of COVID-19, is global and unprecedented. Although remdesivir has recently been approved by the FDA to treat SARS-CoV-2 infection, no oral antiviral is available for outpatient treatment. AT-527, an orally administered double prodrug of a guanosine nucleotide analog, was previously shown to be highly efficacious and well tolerated in hepatitis C virus (HCV)-infected subjects. Here, we report the potent in vitro activity of AT-511, the free base of AT-527, against several coronaviruses, including SARS-CoV-2. In normal human airway epithelial cells, the concentration of AT-511 required to inhibit replication of SARS-CoV-2 by 90% (EC 90 ) was 0.47 μM, very similar to its EC 90 against human coronavirus (HCoV)-229E, HCoV-OC43, and SARS-CoV in Huh-7 cells. Little to no cytotoxicity was observed for AT-511 at concentrations up to 100 μM. Substantial levels of the active triphosphate metabolite AT-9010 were formed in normal human bronchial and nasal epithelial cells incubated with 10 μM AT-511 (698 ± 15 and 236 ± 14 μM, respectively), with a half-life of at least 38 h. Results from steady-state pharmacokinetic and tissue distribution studies of nonhuman primates administered oral doses of AT-527, as well as pharmacokinetic data from subjects given daily oral doses of AT-527, predict that twice daily oral doses of 550 mg AT-527 will produce AT-9010 trough concentrations in human lung that exceed the EC 90 observed for the prodrug against SARS-CoV-2 replication. This suggests that AT-527 may be an effective treatment option for COVID-19., (Copyright © 2021 Good et al.)

Published

2021

6. Preclinical evaluation of AT-527, a novel guanosine nucleotide prodrug with potent, pan-genotypic activity against hepatitis C virus.

Author

Good SS, Moussa A, Zhou XJ, Pietropaolo K, and Sommadossi JP

Subjects

Animals, Antiviral Agents chemistry, Antiviral Agents metabolism, Antiviral Agents pharmacokinetics, Cell Line, Drug Discovery, Drug Evaluation, Preclinical, Female, Guanosine analogs & derivatives, Guanosine metabolism, Guanosine pharmacokinetics, Haplorhini, Hepacivirus genetics, Hepatocytes drug effects, Hepatocytes metabolism, Hepatocytes virology, Humans, Male, Mice, Prodrugs chemistry, Prodrugs metabolism, Prodrugs pharmacokinetics, Rats, Antiviral Agents pharmacology, Guanosine pharmacology, Hepacivirus drug effects, Hepatitis C drug therapy, Prodrugs pharmacology

Abstract

Despite the availability of highly effective direct-acting antiviral (DAA) regimens for the treatment of hepatitis C virus (HCV) infections, sustained viral response (SVR) rates remain suboptimal for difficult-to-treat patient populations such as those with HCV genotype 3, cirrhosis or prior treatment experience, warranting development of more potent HCV replication antivirals. AT-527 is the hemi-sulfate salt of AT-511, a novel phosphoramidate prodrug of 2'-fluoro-2'-C-methylguanosine-5'-monophosphate that has potent in vitro activity against HCV. The EC50 of AT-511, determined using HCV laboratory strains and clinical isolates with genotypes 1-5, ranged from 5-28 nM. The active 5'-triphosphate metabolite, AT-9010, specifically inhibited the HCV RNA-dependent RNA polymerase. AT-511 did not inhibit the replication of other selected RNA or DNA viruses in vitro. AT-511 was approximately 10-fold more active than sofosbuvir (SOF) against a panel of laboratory strains and clinical isolates of HCV genotypes 1-5 and remained fully active against S282T resistance-associated variants, with up to 58-fold more potency than SOF. In vitro, AT-511 did not inhibit human DNA polymerases or elicit cytotoxicity or mitochondrial toxicity at concentrations up to 100 μM. Unlike the other potent guanosine analogs PSI-938 and PSI-661, no mutagenic O6-alkylguanine bases were formed when incubated with cytochrome P450 (CYP) 3A4, and AT-511 had IC50 values ≥25 μM against a panel of CYP enzymes. In hepatocytes from multiple species, the active triphosphate was the predominant metabolite produced from the prodrug, with a half-life of 10 h in human hepatocytes. When given orally to rats and monkeys, AT-527 preferentially delivered high levels of AT-9010 in the liver in vivo. These favorable preclinical attributes support the ongoing clinical development of AT-527 and suggest that, when used in combination with an HCV DAA from a different class, AT-527 may increase SVR rates, especially for difficult-to-treat patient populations, and could potentially shorten treatment duration for all patients., Competing Interests: AM, XZ, KP and JS are employees of Atea Pharmaceuticals, Inc. and SG is a consultant for Atea Pharmaceuticals, Inc. AM and JS are co-inventors on the patent for AT-527. AT-527 is a product under development by Atea Pharmaceuticals, Inc. This does not alter our adherence to all PLOS ONE policies on sharing data and materials.

Published

2020

7. Safety, pharmacokinetics and antiviral activity of AT-527, a novel purine nucleotide prodrug, in HCV-infected subjects with and without cirrhosis.

Author

Berliba E, Bogus M, Vanhoutte F, Berghmans PJ, Good SS, Moussa A, Pietropaolo K, Murphy RL, Zhou XJ, and Sommadossi JP

Abstract

AT-527 is a novel modified guanosine nucleotide prodrug inhibitor of the hepatitis C virus (HCV) NS5B polymerase, with increased in vitro antiviral activity as compared to sofosbuvir and a highly differentiated favorable preclinical profile compared to other anti-HCV nucleoside/nucleotide analogs. This was a multiple part clinical study where multiple ascending doses of AT-527 up to 600 mg (expressed as AT-527 salt form; equivalent to 553 mg free base) once daily for seven days were evaluated in a randomized, double-blind, placebo-controlled study of treatment-naïve, non-cirrhotic, genotype 1b, HCV-infected subjects. The highest dose of AT-527 for the same duration was then evaluated in two open label cohorts of a) non-cirrhotic, genotype 3, HCV-infected subjects and b) HCV-infected subjects of any genotype with compensated (Child-Pugh A) cirrhosis. AT-527 was well tolerated for seven days in all cohorts. At the highest dose tested, mean HCV RNA reductions of up to 2.4 log 10 IU/mL occurred within the first 24 hours of dosing. Mean maximum reductions observed with seven days of dosing were 4.4, 4.5 and 4.6 log 10 IU/mL in non-cirrhotic subjects with HCV genotype 1b, non-cirrhotic subjects with HCV genotype 3, and subjects with compensated cirrhosis, respectively. The systemic half-life of AT-273, the nucleoside metabolite considered a surrogate of intracellular phosphates including the active triphosphate, exceeded 20 hours, supporting once daily dosing. In summary, AT-527 demonstrated rapid, potent, dose/exposure-related and pan-genotypic antiviral activity with similar responses between subjects with and without cirrhosis. Exposure-antiviral response analysis identified 550 mg (free base equivalent) as the optimal dose of AT-527. Safety and antiviral activity data from this study warrant continued clinical development of AT-527 dosed once daily., (Copyright © 2019 Berliba et al.)

Published

2019

8. Pharmacokinetics of IDX184, a liver-targeted oral prodrug of 2'-methylguanosine-5'-monophosphate, in the monkey and formulation optimization for human exposure.

Author

Pan-Zhou XR, Mayes BA, Rashidzadeh H, Gasparac R, Smith S, Bhadresa S, Gupta K, Cohen ML, Bu C, Good SS, Moussa A, and Rush R

Subjects

Animals, Capsules administration & dosage, Capsules pharmacokinetics, Chemistry, Pharmaceutical methods, Guanosine administration & dosage, Guanosine pharmacokinetics, Guanosine Monophosphate administration & dosage, Guanosine Monophosphate pharmacokinetics, Haplorhini, Humans, Male, Tablets administration & dosage, Tablets pharmacokinetics, Guanosine analogs & derivatives, Guanosine Monophosphate analogs & derivatives, Liver drug effects, Prodrugs administration & dosage, Prodrugs pharmacokinetics

Abstract

IDX184 is a phosphoramidate prodrug of 2'-methylguanosine-5'-monophosphate, developed to treat patients infected with hepatitis C virus. A mass balance study of radiolabeled IDX184 and pharmacokinetic studies of IDX184 in portal vein-cannulated monkeys revealed relatively low IDX184 absorption but higher exposure of IDX184 in the portal vein than in the systemic circulation, indicating >90 % of the absorbed dose was subject to hepatic extraction. Systemic exposures to the main metabolite, 2'-methylguanosine (2'-MeG), were used as a surrogate for liver levels of the pharmacologically active entity 2'-MeG triphosphate, and accordingly, systemic levels of 2'-MeG in the monkey were used to optimize formulations for further clinical development of IDX184. Capsule formulations of IDX184 delivered acceptable levels of 2'-MeG in humans; however, the encapsulation process introduced low levels of the genotoxic impurity ethylene sulfide (ES), which necessitated formulation optimization. Animal pharmacokinetic data guided the development of a tablet with trace levels of ES and pharmacokinetic performance equal to that of the clinical capsule in the monkey. Under fed conditions in humans, the new tablet formulation showed similar exposure to the capsule used in prior clinical trials.

Published

2016

9. Overcoming stability challenges in the quantification of tissue nucleotides: determination of 2'-C-methylguanosine triphosphate concentration in mouse liver.

Author

Rashidzadeh H, Bhadresa S, Good SS, Larsson Cohen M, Gupta KS, and Rush WR

Subjects

Animals, Antiviral Agents metabolism, Antiviral Agents pharmacokinetics, Chromatography, Ion Exchange methods, Chromatography, Liquid methods, Freezing, Guanosine metabolism, Guanosine pharmacokinetics, Guanosine Monophosphate metabolism, Guanosine Monophosphate pharmacokinetics, Guanosine Triphosphate analogs & derivatives, Hepatitis C drug therapy, Male, Mice, Prodrugs pharmacokinetics, Solid Phase Extraction methods, Tandem Mass Spectrometry methods, Trichloroacetic Acid chemistry, Guanosine analogs & derivatives, Guanosine Monophosphate analogs & derivatives, Guanosine Triphosphate metabolism, Liver metabolism, Nucleotides metabolism, Prodrugs metabolism

Abstract

A conventional, rapid and high throughput method for tissue extraction and accurate and selective LC-MS/MS quantification of 2'-C-methylguanosine triphosphate (2'-MeGTP) in mouse liver was developed and qualified. Trichloroacetic acid (TCA) was used as the tissue homogenization reagent that overcomes instability challenges of liver tissue nucleotide triphosphates due to instant ischemic degradation to mono- and diphosphate nucleotides. Degradation of 2'-MeGTP was also minimized by harvesting livers using in situ clamp-freezing or snap-freezing techniques. The assay also included a sample clean-up procedure using weak anion exchange solid phase extraction followed by ion exchange chromatography and tandem mass spectrometry detection. The linear assay range was from 50 to 10000 pmol/mL concentration in liver homogenate (250-50000 pmol/g in liver tissue). The method was qualified over three intraday batches for accuracy, precision, selectivity and specificity. The assay was successfully applied to pharmacokinetic studies of 2'-MeGTP in liver tissue samples after single oral doses of IDX184, a nucleotide prodrug inhibitor of the viral polymerase for the treatment of hepatitis C, to mice. The study results suggested that the clamp-freezing liver collection method was marginally more effective in preventing 2'-MeGTP degradation during liver tissue collection compared to the snap-freezing method.

Published

2015

10. Estimation of human drug clearance using multiexponential techniques.

Author

Goteti K, Brassil PJ, Good SS, and Garner CE

Subjects

Animals, Body Weight, Data Interpretation, Statistical, Drug Evaluation, Preclinical methods, Haplorhini, Humans, Liver Circulation physiology, Species Specificity, Models, Biological, Pharmaceutical Preparations metabolism, Pharmacokinetics

Abstract

A multiexponential allometry (MA) method was developed to predict human drug clearance from preclinical data. Separate data sets containing clearances from human and preclinical species were chosen for the study. Human clearance was estimated using the MA technique according to the equation: CL = aBWb + cBWd, where CL is clearance in milliliters/minute, and a, b, c, and d are constants derived from preclinical pharmacokinetic data. Simple allometry (SA) gave the poorest prediction using any data set, and the percentage outliers remained larger than MA or monkey liver blood flow within 1.5-, 2-, and 3-fold error. Analysis of compounds common to both data sets suggested that MA could accurately predict human clearances within approximately 10% of 3-fold error. The analysis also showed that monkey is an important species for scaling, and MA is a better predictor of human clearance when the slope of SA is >0.7.

Published

2008

11. Preclinical and toxicology studies of 1263W94, a potent and selective inhibitor of human cytomegalovirus replication.

Author

Koszalka GW, Johnson NW, Good SS, Boyd L, Chamberlain SC, Townsend LB, Drach JC, and Biron KK

Subjects

Administration, Oral, Animals, Area Under Curve, Biotransformation, Blood Proteins metabolism, Dogs, Female, Half-Life, Humans, Injections, Intravenous, Macaca fascicularis, Male, Mice, Mutagenicity Tests, Protein Binding, Rats, Rats, Sprague-Dawley, Rats, Wistar, Tissue Distribution, Antiviral Agents pharmacokinetics, Antiviral Agents toxicity, Benzimidazoles pharmacokinetics, Benzimidazoles toxicity, Cytomegalovirus drug effects, Ribonucleosides pharmacokinetics, Ribonucleosides toxicity

Abstract

1263W94 is a novel benzimidazole compound being developed for treatment of human cytomegalovirus infection. No adverse pharmacological effects were demonstrated in safety pharmacology studies with 1263W94. The minimal-effect dose in a 1-month rat study was 100 mg/kg/day, and the no-effect dose in a 1-month monkey study was 180 mg/kg/day. Toxic effects were limited to increases in liver weights, neutrophils, and monocytes at higher doses in female rats. 1263W94 was not genotoxic in the Ames or micronucleus assays. In the mouse lymphoma assay, 1263W94 was mutagenic in the absence of the rat liver S-9 metabolic activation system, with equivocal results in the presence of the S-9 mix. Mean oral bioavailability of 1263W94 was >90% in rats and approximately 50% in monkeys. Clearance in rats and monkeys was primarily by biliary secretion, with evidence of enterohepatic recirculation. In 1-month studies in rats and monkeys, mean peak concentrations and exposures to 1263W94 increased in near proportion to dose. Metabolism of 1263W94 to its primary metabolite, an N-dealkylated analog, appeared to be mediated via the isozyme CYP3A4 in humans. 1263W94 was primarily distributed in the gastrointestinal tract of rats but did not cross the blood-brain barrier. In monkeys, 1263W94 levels in the brain, cerebrospinal fluid, and vitreous humor ranged from 4 to 20%, 1 to 2%, and <1%, of corresponding concentrations in plasma, respectively. The high level of binding by 1263W94 to human plasma proteins (primarily albumin) was readily reversible, with less protein binding seen in the monkey, rat, and mouse. Results of these studies demonstrate a favorable safety profile for 1263W94.

Published

2002

12. Potent and selective inhibition of human cytomegalovirus replication by 1263W94, a benzimidazole L-riboside with a unique mode of action.

Author

Biron KK, Harvey RJ, Chamberlain SC, Good SS, Smith AA 3rd, Davis MG, Talarico CL, Miller WH, Ferris R, Dornsife RE, Stanat SC, Drach JC, Townsend LB, and Koszalka GW

Subjects

Antiviral Agents toxicity, Biomarkers, Cell Survival drug effects, Cells, Cultured, Cytomegalovirus enzymology, Cytomegalovirus genetics, DNA, Viral drug effects, DNA-Directed DNA Polymerase biosynthesis, DNA-Directed DNA Polymerase genetics, Drug Resistance, Drug Resistance, Microbial, Erythroid Precursor Cells drug effects, Fibroblasts, Humans, Nucleic Acid Synthesis Inhibitors, Phosphorylation, Protein Kinases metabolism, Sequence Analysis, DNA, Structure-Activity Relationship, Antiviral Agents pharmacology, Benzimidazoles pharmacology, Cytomegalovirus drug effects, Ribonucleosides pharmacology, Virus Replication drug effects

Abstract

Benzimidazole nucleosides have been shown to be potent inhibitors of human cytomegalovirus (HCMV) replication in vitro. As part of the exploration of structure-activity relationships within this series, we synthesized the 2-isopropylamino derivative (3322W93) of 1H-beta-D-ribofuranoside-2-bromo-5,6-dichlorobenzimidazole (BDCRB) and the biologically unnatural L-sugars corresponding to both compounds. One of the L derivatives, 1H-beta-L-ribofuranoside-2-isopropylamino-5,6-dichlorobenzimidazole (1263W94), showed significant antiviral potency in vitro against both laboratory HCMV strains and clinical HCMV isolates, including those resistant to ganciclovir (GCV), foscarnet, and BDCRB. 1263W94 inhibited viral replication in a dose-dependent manner, with a mean 50% inhibitory concentration (IC(50)) of 0.12 +/- 0.01 microM compared to a mean IC(50) for GCV of 0.53 +/- 0.04 microM, as measured by a multicycle DNA hybridization assay. In a single replication cycle, 1263W94 treatment reduced viral DNA synthesis, as well as overall virus yield. HCMV mutants resistant to 1263W94 were isolated, establishing that the target of 1263W94 was a viral gene product. The resistance mutation was mapped to the UL97 open reading frame. The pUL97 protein kinase was strongly inhibited by 1263W94, with 50% inhibition occurring at 3 nM. Although HCMV DNA synthesis was inhibited by 1263W94, the inhibition was not mediated by the inhibition of viral DNA polymerase. The parent benzimidazole D-riboside BDCRB inhibits viral DNA maturation and processing, whereas 1263W94 does not. The mechanism of the antiviral effect of L-riboside 1263W94 is thus distinct from those of GCV and of BDCRB. In summary, 1263W94 inhibits viral replication by a novel mechanism that is not yet completely understood.

Published

2002

13. 1592U89, a novel carbocyclic nucleoside analog with potent, selective anti-human immunodeficiency virus activity.

Author

Daluge SM, Good SS, Faletto MB, Miller WH, St Clair MH, Boone LR, Tisdale M, Parry NR, Reardon JE, Dornsife RE, Averett DR, and Krenitsky TA

Subjects

Acquired Immunodeficiency Syndrome metabolism, Adenosine Deaminase metabolism, Administration, Oral, Animals, Anti-HIV Agents blood, Anti-HIV Agents chemistry, Anti-HIV Agents urine, Antiviral Agents blood, Antiviral Agents pharmacokinetics, Area Under Curve, Biotransformation, Cells, Cultured, Dideoxynucleosides blood, Dideoxynucleosides chemistry, Dideoxynucleosides urine, Drug Resistance, Microbial, Female, HIV-1 drug effects, Half-Life, Humans, Injections, Intravenous, Macaca fascicularis, Male, Rats, Structure-Activity Relationship, Acquired Immunodeficiency Syndrome drug therapy, Anti-HIV Agents pharmacokinetics, Dideoxynucleosides pharmacokinetics

Abstract

1592U89, (-)-(1S,4R)-4-[2-amino-6-(cyclopropylamino)-9H-purin-9-yl]-2-cyclo pentene-1-methanol, is a carbocyclic nucleoside with a unique biological profile giving potent, selective anti-human immunodeficiency virus (HIV) activity. 1592U89 was selected after evaluation of a wide variety of analogs containing a cyclopentene substitution for the 2'-deoxyriboside of natural deoxynucleosides, optimizing in vitro anti-HIV potency, oral bioavailability, and central nervous system (CNS) penetration. 1592U89 was equivalent in potency to 3'-azido-3'-deoxythymidine (AZT) in human peripheral blood lymphocyte (PBL) cultures against clinical isolates of HIV type 1 (HIV-1) from antiretroviral drug-naive patients (average 50% inhibitory concentration [IC50], 0.26 microM for 1592U89 and 0.23 microM for AZT). 1592U89 showed minimal cross-resistance (approximately twofold) with AZT and other approved HIV reverse transcriptase (RT) inhibitors. 1592U89 was synergistic in combination with AZT, the nonnucleoside RT inhibitor nevirapine, and the protease inhibitor 141W94 in MT4 cells against HIV-1 (IIIB). 1592U89 was anabolized intracellularly to its 5'-monophosphate in CD4+ CEM cells and in PBLs, but the di- and triphosphates of 1592U89 were not detected. The only triphosphate found in cells incubated with 1592U89 was that of the guanine analog (-)-carbovir (CBV). However, the in vivo pharmacokinetic, distribution, and toxicological profiles of 1592U89 were distinct from and improved over those of CBV, probably because CBV itself was not appreciably formed from 1592U89 in cells or animals (<2%). The 5'-triphosphate of CBV was a potent, selective inhibitor of HIV-1 RT, with Ki values for DNA polymerases (alpha, beta, gamma, and epsilon which were 90-, 2,900-, 1,200-, and 1,900-fold greater, respectively, than for RT (Ki, 21 nM). 1592U89 was relatively nontoxic to human bone marrow progenitors erythroid burst-forming unit and granulocyte-macrophage CFU (IC50s, 110 microM) and human leukemic and liver tumor cell lines. 1592U89 had excellent oral bioavailability (105% in the rat) and penetrated the CNS (rat brain and monkey cerebrospinal fluid) as well as AZT. Having demonstrated an excellent preclinical profile, 1592U89 has progressed to clinical evaluation in HIV-infected patients.

Published

1997

14. Unique intracellular activation of the potent anti-human immunodeficiency virus agent 1592U89.

Author

Faletto MB, Miller WH, Garvey EP, St Clair MH, Daluge SM, and Good SS

Subjects

Animals, CD4 Antigens drug effects, CD4 Antigens metabolism, Cells, Cultured, Chromatography, High Pressure Liquid, Deamination, Humans, Liver drug effects, Liver metabolism, Phosphorylation, Rats, Structure-Activity Relationship, Anti-HIV Agents metabolism, Antiviral Agents metabolism, Dideoxynucleosides metabolism

Abstract

The anabolism of 1592U89, (-)-(1S,4R)-4-[2-amino-6-(cyclopropylamino)-9H-purin-9-yl]-2-cyclo pentene-1-methanol, a selective inhibitor of human immunodeficiency virus (HIV), was characterized in human T-lymphoblastoid CD4+ CEM cells. 1592U89 was ultimately anabolized to the triphosphate (TP) of the guanine analog (-)-carbovir (CBV), a potent inhibitor of HIV reverse transcriptase. However, less than 2% of intracellular 1592U89 was converted to CBV, an amount insufficient to account for the CBV-TP levels observed. 1592U89 was anabolized to its 5'-monophosphate (MP) by the recently characterized enzyme adenosine phosphotransferase, but neither its diphosphate (DP) nor its TP was detected. The MP, DP, and TP of CBV were found in cells incubated with either 1592U89 or CBV, with CBV-TP being the major phosphorylated species. We confirmed that CBV is phosphorylated by 5'-nucleotidase and that mycophenolic acid increased the formation of CBV-TP from CBV 75-fold. However, mycophenolic acid did not stimulate 1592U89 anabolism to CBV-TP. The adenosine deaminase inhibitor erythro-9-(2-hydroxy-3-nonyl)adenine (EHNA) did not inhibit CBV-TP formation from CBV or 1592U89, whereas the adenylate deaminase inhibitor 2'-deoxycoformycin selectively inhibited 1592U89 anabolism to CBV-TP and reversed the antiviral activity of 1592U89. 1592U89-MP was not a substrate for adenylate deaminase but was a substrate for a distinct cytosolic deaminase that was inhibited by 2'-deoxycoformycin-5'-MP. Thus, 1592U89 is phosphorylated by adenosine phosphotransferase to 1592U89-MP, which is converted by a novel cytosolic enzyme to CBV-MP. CBV-MP is then further phosphorylated to CBV-TP by cellular kinases. This unique activation pathway enables 1592U89 to overcome the pharmacokinetic and toxicological deficiencies of CBV while maintaining potent and selective anti-HIV activity.

Published

1997

15. Metabolism of 5-fluorocytosine to 5-fluorouracil in human colorectal tumor cells transduced with the cytosine deaminase gene: significant antitumor effects when only a small percentage of tumor cells express cytosine deaminase.

Author

Huber BE, Austin EA, Richards CA, Davis ST, and Good SS

Subjects

Animals, Biotransformation, Cell Division, Cell Survival, Chromatography, High Pressure Liquid, Colorectal Neoplasms enzymology, Colorectal Neoplasms pathology, Colorectal Neoplasms therapy, Cytosine Deaminase, DNA, Neoplasm biosynthesis, Humans, Kinetics, Mice, Mice, Nude, Nucleoside Deaminases biosynthesis, RNA, Neoplasm biosynthesis, Thymidylate Synthase antagonists & inhibitors, Time Factors, Transplantation, Heterologous, Tritium, Tumor Cells, Cultured, Colorectal Neoplasms metabolism, Flucytosine metabolism, Fluorouracil metabolism, Gene Expression, Nucleoside Deaminases metabolism

Abstract

The gene encoding cytosine deaminase (CD) has been expressed in the human colorectal carcinoma cell line WiDr. Metabolism studies confirm that tumor cells expressing CD convert the very nontoxic prodrug 5-fluorocytosine (5FCyt) to 5-fluorouracil (5FUra) and 5FUra metabolites. Tumor xenografts composed of CD-expressing cells can selectively generate tumor levels of > 400 microM 5FUra when the host mouse is dosed with nontoxic levels of 5FCyt. The selective metabolic conversion of 5FCyt to 5FUra in CD-expressing tumor cells results in the inhibition of thymidylate synthase and incorporation of 5FUra into RNA. 5FUra is also liberated into the surrounding environment when CD-expressing tumor cells are treated with 5FCyt. The liberated 5FUra is able to kill neighboring, non-CD-expressing tumor cells in vitro and in vivo. Most importantly, when only 2% of the tumor mass contains CD-expressing cells (98% non-CD-expressing cells), significant regressions in all tumors are observed when the host mouse is dosed with nontoxic levels of 5FCyt.

Published

1994

16. In vivo antitumor activity of 5-fluorocytosine on human colorectal carcinoma cells genetically modified to express cytosine deaminase.

Author

Huber BE, Austin EA, Good SS, Knick VC, Tibbels S, and Richards CA

Subjects

Animals, Cell Division drug effects, Colorectal Neoplasms genetics, Colorectal Neoplasms pathology, Cytosine Deaminase, Female, Flucytosine pharmacokinetics, Flucytosine toxicity, Fluorouracil pharmacokinetics, Fluorouracil toxicity, Humans, Kinetics, Mice, Mice, Nude, Neoplasm Transplantation, Nucleoside Deaminases genetics, Transfection, Transplantation, Heterologous, Tumor Cells, Cultured, Colorectal Neoplasms drug therapy, Colorectal Neoplasms enzymology, Flucytosine therapeutic use, Fluorouracil therapeutic use, Nucleoside Deaminases biosynthesis

Abstract

A human colorectal carcinoma cell line, WiDr, was genetically engineered to express the nonmammalian enzyme, cytosine deaminase (CD). Expression of CD in WiDr cells (WiDr/CD) did not alter the growth rate of these cells when grown in vitro or as solid tumor xenografts in nude mice. However, expression of CD did increase the sensitivity of these cells to the nontoxic prodrug, 5-fluorocytosine (FCyt), decreasing the 50% inhibitory concentration for FCyt from 26,000 microM in parental WiDr cells to 27 microM in WiDr/CD cells. The increase in sensitivity to FCyt in WiDr/CD cells was the result of the CD-mediated conversion of FCyt to 5-fluorouracil (FUra) and subsequent FUra anabolites. The half-life of the prodrug, FCyt, was determined to be approximately 40 min in nude mice. A single i.p. injection of 500 mg FCyt/kg body weight resulted in a transient FCyt plasma level of approximately 4000 microM while osmotic minipumps or constant tail vein infusions of FCyt achieved continual FCyt plasma levels of 5 microM and 50 microM, respectively, with no overt signs of toxicity. Significant antitumor effects were observed in nude mice bearing tumors derived from WiDr/CD cells when these animals were given 500 mg FCyt/kg i.p. for 10 consecutive days. These antitumor effects were demonstrated by decreases in tumor growth rate, tumor size, tumor weight, and thymidine incorporation into tumor DNA. This antitumor effect was significant but less profound if FCyt was administered by constant tail vein infusion. WiDr and WiDr/CD cells were very sensitive to FUra in vitro (50% inhibitory concentration approximately 5 microM). However, no significant antitumor effects were observed in nude mice bearing tumors derived from either WiDr or WiDr/CD cells when these animals were treated with various doses of FUra. Taken collectively, these data indicate that nontoxic plasma levels of FCyt can be attained which can produce profound antitumor effects on tumors engineered to express CD and that these antitumor effects are significantly better than those that can be achieved using FUra. These positive data support the continued development of a gene therapy approach to colorectal carcinoma involving the selective expression of CD in colorectal tumors with subsequent administration of FCyt.

Published

1993

17. Synthesis and biological evaluation of dinucleoside methylphosphonates of 3'-azido-3'-deoxythymidine and 2', 3'-dideoxycytidine.

Author

Puech F, Gosselin G, Balzarini J, Good SS, Rideout JL, De Clercq E, and Imbach JL

Subjects

Animals, Antineoplastic Agents pharmacology, Deoxycytosine Nucleotides pharmacology, Drug Evaluation, Preclinical, HIV growth & development, Hydrolysis, Mice, Mice, Inbred C3H, Moloney murine sarcoma virus drug effects, Moloney murine sarcoma virus growth & development, Thymine Nucleotides pharmacology, Tumor Cells, Cultured, Virus Replication drug effects, Zalcitabine pharmacology, Zidovudine pharmacology, Deoxycytosine Nucleotides chemical synthesis, HIV drug effects, Thymine Nucleotides chemical synthesis, Zalcitabine chemical synthesis, Zidovudine chemical synthesis

Abstract

The 5'----5' dinucleoside methylphosphonates of 3'-azido-3'-deoxythymidine (AZT) and 2',3'-dideoxycytidine (DDC) were prepared and evaluated for their inhibitory properties against different viruses, including human immunodeficiency virus (HIV). The synthesis of the compounds was achieved by reaction of AZT or N4-(4-monomethoxytrityl)-2',3'-dideoxycytidine with in situ prepared methylphosphonic bis (triazolide), followed in the latter case by an acidic treatment. The two title compounds showed in vitro anti-HIV activity, that was 200- to 450-fold less pronounced that that shown by the corresponding monomeric nucleosides AZT and DDC. The decreased antiviral activity may be ascribed to nuclease resistance of the methylphosphonate linkage.

Published

1990

18. Tissue distribution and metabolic disposition of zidovudine in rats.

Author

de Miranda P, Burnette TC, and Good SS

Subjects

Animals, Bile metabolism, Chromatography, High Pressure Liquid, Dideoxynucleosides metabolism, Dideoxynucleosides urine, Feces analysis, In Vitro Techniques, Intestinal Absorption, Male, Rats, Tissue Distribution, Zidovudine analogs & derivatives, Zidovudine metabolism, Zidovudine urine, Zidovudine pharmacokinetics

Abstract

The tissue distribution and metabolic fate of [5'-3H]zidovudine was studied in rats after a single dose of 10 mg/kg by gavage. The drug was absorbed rapidly and distributed into all tissues. Peak blood and tissue levels were observed 0.25 hr post-dose. The level of peak radioactivity in the stomach, intestine, liver, spleen, adrenals, and kidney was higher than in plasma, while in the heart, lung, thymus, lymph nodes, muscle, bone, and skin it was similar to that in plasma. Only in the testes and the brain the radioactivity was lower than in plasma. Blood and plasma radioactivity levels were nearly equivalent. A biphasic disappearance of radioactive material was observed in blood and plasma, as well as in most tissues, with a rapid decline in the early phase (0.25-4 hr) and a slower decline thereafter. The 0-24-hr urinary and fecal recoveries (mean +/- SD) of radioactive material were 78 +/- 14% and 20 +/- 9% of dose, respectively, indicating virtually complete recovery of the radioactive dose. Reversed-phase HPLC analysis indicated that approximately 88% of urinary radioactivity corresponded to unchanged zidovudine, with the remaining radioactivity accounted for by five metabolites. One of these urinary metabolites was identified as 3'-azido-3'-deoxy-5'-O-beta-D-glucopyranuronosylthymidine and another as 3'-amino-3'-deoxythymidine (AMT). The majority of fecal radioactivity (greater than 70%) corresponded to AMT. There is a component of biliary excretion in the disposition of zidovudine. At least 7% of a parenteral dose of zidovudine was secreted in the bile, primarily as 3'-azido-3'-deoxy-5'-beta-D-glucuronylazidothymidine, which may be a source of fecal AMT.

Published

1990

19. Isolation and characterization of an ether glucuronide of zidovudine, a major metabolite in monkeys and humans.

Author

Good SS, Koble CS, Crouch R, Johnson RL, Rideout JL, and de Miranda P

Subjects

Animals, Biotransformation, Chemical Phenomena, Chemistry, Physical, Chromatography, High Pressure Liquid, Glucuronidase metabolism, Humans, In Vitro Techniques, Macaca fascicularis, Magnetic Resonance Spectroscopy, Mass Spectrometry, Microsomes, Liver enzymology, Species Specificity, Spectrophotometry, Infrared, Spectrophotometry, Ultraviolet, Zidovudine analysis, Zidovudine blood, Zidovudine urine, Zidovudine analogs & derivatives, Zidovudine metabolism

Abstract

A major metabolite of zidovudine (3'-azido-3'-deoxythymidine, AZT), which previously had not been observed in a variety of experimental animals, was identified in samples of plasma and urine from cynomolgus monkeys and a patient treated with AZT. The urinary recoveries of metabolite from the monkeys and the patient were, respectively, 1.5- and 6.9-fold higher than the recoveries of unchanged drug. The metabolite was purified in gram quantities from the urines of the monkeys and the patient and was identified enzymatically, using beta-glucuronidase and a specific inhibitor of the enzyme, as a glucuronide conjugate of AZT. The metabolite was formed in vitro by incubating AZT with preparations of human liver in the presence of UDP-glucuronic acid. In addition, the metabolite was prepared synthetically and physical characterizations--including microanalysis and UV, IR, NMR and mass spectra--of compound from all three sources were identical and confirmed the metabolite to be the 5'-O-beta-D-glucuronide of AZT.

Published

1990

20. Pharmacokinetics and bioavailability of zidovudine in humans.

Author

Blum MR, Liao SH, Good SS, and de Miranda P

Subjects

Adult, Antiviral Agents therapeutic use, Biological Availability, Drug Evaluation, Humans, Thymidine pharmacokinetics, Thymidine therapeutic use, Zidovudine, AIDS-Related Complex drug therapy, Acquired Immunodeficiency Syndrome drug therapy, Antiviral Agents pharmacokinetics, Thymidine analogs & derivatives

Abstract

The basic pharmacokinetic and bioavailability information on zidovudine was obtained during the initial phase I study. Following intravenous doses of 1.0 mg/kg every eight hours to 7.5 mg/kg every four hours, zidovudine plasma levels decay in a biexponential manner, indicating two-compartment pharmacokinetics. The mean half-life was 1.1 hours over this dose range and the total body clearance was approximately 1,900 ml/minute/70 kg, up to doses of 5 mg/kg. At 7.5 mg/kg, total body clearance decreased by 35 percent. The 5'-O-glucuronide was identified as a major metabolite of zidovudine in plasma and urine. This inactive metabolite is rapidly formed and cleared from plasma, with a half-life of one hour. No other metabolites have been found in humans. Renal clearance of zidovudine was estimated at 350 ml/minute/70 kg. Zidovudine penetrated the blood brain barrier as indicated by a cerebrospinal fluid:plasma ratio averaging 0.5, determined two to four hours after dosing. Following oral administration of zidovudine at doses from 2.0 mg/kg every eight hours to 10 mg/kg every four hours, peak plasma levels increased proportionately with dose; the average bioavailability was 65 percent. Since 90 percent of the drug was recovered in the urine as zidovudine or the 5'-O-glucuronide, the incomplete bioavailability is assumed to be the result of first-pass metabolism rather than incomplete absorption. Pharmacokinetic questions related to optimal use of the drug are currently being addressed.

Published

1988

21. Metabolic fate of radioactive acyclovir in humans.

Author

de Miranda P, Good SS, Krasny HC, Connor JD, Laskin OL, and Lietman PS

Subjects

Acyclovir, Adult, Aged, Antiviral Agents blood, Blood Proteins metabolism, Carbon Radioisotopes, Feces analysis, Female, Guanine blood, Guanine metabolism, Humans, Kidney metabolism, Kinetics, Male, Middle Aged, Antiviral Agents metabolism, Guanine analogs & derivatives

Abstract

The metabolic fate and the kinetics of elimination of [8-14C]acyclovir in plasma and blood was investigated in five cancer patients. Doses of 0.5 and 2.5 mg/kg were administered by one-hour intravenous infusion. Radioactivity was distributed nearly equally in blood and plasma. The plasma and blood concentration-time data were defined by a two-compartment open pharmacokinetic model. The overall mean acyclovir plasma half-life and total body clearance +/- SD were 2.1 +/- 0.5 hours and 297 +/- 53 ml/min/1.73 m2. Binding of acyclovir to plasma proteins was 15.4 +/- 4.4 percent. The radioactive dose was excreted predominantly in the urine (71 to 99 percent) with less than 2 percent excretion in the feces and only trace amounts of radioactivity in the expired air. Reverse-phase high-performance liquid chromatography indicated that 9-carboxymethoxymethylguanine was the only significant urinary metabolite of acyclovir accounting for 8.5 to 14.1 percent of the dose. A minor metabolite (less than 0.2 percent of dose) had the retention time of 8-hydroxy-9-(2-hydroxyethoxymethyl)guanine. Unchanged urinary acyclovir ranged from 62 to 91 percent of the dose. There was no indication of acyclovir cleavage to guanine. The renal clearances of acyclovir were three times higher than the corresponding creatinine clearances.

Published

1982

22. Metabolic disposition of acyclovir in the guinea pig, rabbit, and monkey.

Author

Good SS and de Miranda P

Subjects

Acyclovir, Animals, Chlorocebus aethiops, Erythrocebus patas, Feces analysis, Guanine blood, Guanine metabolism, Guanine urine, Guinea Pigs, Half-Life, Kinetics, Macaca mulatta, Rabbits, Antiviral Agents metabolism, Guanine analogs & derivatives

Abstract

Two guinea pigs and two rabbits were each inoculated subcutaneously with 14C-labeled acyclovir (25 mg/kg). Both species excreted the entire amount within 72 hours. The rabbits excreted all of the radioactivity in the urine while the guinea pigs excreted an average of 14.2 percent in the feces. The rabbits excreted an average of 71.0 percent of the dose as unchanged drug; 25.1 percent was excreted as 9-carboxymethoxymethylguanine (CMMG) and 3.5 percent as 8-hydroxy-9-(2-hydroxyethoxymethyl)guanine (8-hydroxyacyclovir). An average of 60.7 percent of the dose was recovered from the guinea pigs as acyclovir; 32.3 percent was excreted as CMMG and 3.1 percent as 8-hydroxyacyclovir. The two rabbits showed elimination-phase half-lives (t 1/2 beta) for plasma acyclovir of 0.8 and 2.2 hours. Mean t 1/2 beta for acyclovir in two rhesus, four patas, and four african green monkeys, each receiving acyclovir (10 mg/kg) as a bolus intravenous injection, were 1.2, 1.7, and 1.8 hours respectively. The average 48 hour urinary excretion of acyclovir, 8-hydroxyacyclovir, and CMMG in the rhesus monkey was estimated to be 21.3 percent, 15.3 percent, and 7.1 percent, respectively, of the total administered amount. The patas and african green species excreted the dose mostly as acyclovir and CMMG.

Published

1982

23. Alteration of zidovudine pharmacokinetics by probenecid in patients with AIDS or AIDS-related complex.

Author

de Miranda P, Good SS, Yarchoan R, Thomas RV, Blum MR, Myers CE, and Broder S

Subjects

Adult, Drug Interactions, Drug Therapy, Combination, Half-Life, Humans, Male, Middle Aged, Probenecid pharmacokinetics, Regression Analysis, Zidovudine analogs & derivatives, Zidovudine blood, Zidovudine urine, AIDS-Related Complex metabolism, Acquired Immunodeficiency Syndrome metabolism, Probenecid pharmacology, Zidovudine pharmacokinetics

Abstract

The anti-human immunodeficiency virus drug zidovudine is metabolized extensively in human beings to the 5'-glucuronide (GAZT) and is cleared rapidly, resulting in a short half-life and the need for frequent dosing. This study explores whether probenecid, which is also metabolized by glucuronidation, reduces zidovudine clearance when zidovudine is administered orally to patients with acquired immunodeficiency syndrome (AIDS) or AIDS-related complex (ARC). The mean zidovudine plasma levels were significantly higher after concurrent administration of probenecid than in its absence, resulting in a twofold increase in the mean AUC, a corresponding decline in the apparent total clearance, and a prolongation in the mean half-life. Similar alterations were observed in GAZT disposition. There was a marked reduction in the urinary excretion ratio of GAZT to zidovudine and a decline in the renal clearance of GAZT after probenecid coadministration. Probenecid inhibits zidovudine glucuronidation and renal excretion of GAZT.

Published

1989

24. Disposition in the dog and the rat of 2, 6-diamino-9-(2-hydroxyethoxymethyl)purine (A134U), a potential prodrug of acyclovir.

Author

Good SS, Krasny HC, Elion GB, and de Miranda P

Subjects

Acyclovir administration & dosage, Acyclovir metabolism, Administration, Oral, Animals, Biotransformation, Chromatography, High Pressure Liquid, Dogs, Kinetics, Male, Radioimmunoassay, Rats, Time Factors, Acyclovir analogs & derivatives

Abstract

2,6-Diamino-9-(2-hydroxyethoxymethyl)purine (A134U), the 6-deoxy-6-amino analog of the antiviral agent acyclovir (ACV), was administered orally to dogs and rats. Plasma concentration-time profiles and urinary excretion of A134U and its deamination product, ACV, were determined. Mean peak plasma ACV concentrations achieved in the dog were 57, 156 and 285 microM after A134U doses of 20, 50 and 120 mg/kg, respectively, and increased in near proportion to the dose. The urinary recovery of ACV accounted for 60-92% of the two lower doses, but only 40-58% of the highest dose. In the rat, peak plasma ACV concentrations were 3.1 and 10.7 microM, respectively, after 20- and 50-mg/kg doses of A134U. After 5- and 20-mg/kg oral doses of [2-14C]A134U, the urinary recovery of ACV (20-27%) accounted for 59 to 76% of the absorbed dose. The remainder was excreted largely as unchanged A134U, with negligible (0.4-1.3%) biotransformation to inactive metabolites. Except for small decreases in absorption and increases in deamination, no change in the metabolism of A134U was observed after its repeated oral administration to rats. Oral dosing of dogs and rats with A134U resulted in peak plasma concentrations and total urinary recoveries of ACV greater than those observed after equivalent oral doses of ACV, suggesting that A134U might be an effective prodrug of ACV for use in the oral therapy of herpes simplex virus infections.

Published

1983

25. Disposition of intravenous radioactive acyclovir.

Author

de Miranda P, Good SS, Laskin OL, Krasny HC, Connor JD, and Lietman PS

Subjects

Acyclovir, Blood Proteins metabolism, Carbon Radioisotopes, Chromatography, High Pressure Liquid, Guanine metabolism, Humans, Infusions, Parenteral, Kinetics, Metabolic Clearance Rate, Protein Binding, Radioimmunoassay, Antiviral Agents metabolism, Guanine analogs & derivatives

Abstract

The kinetic and metabolic disposition of (8-14C)acyclovir (ACV) was investigated in five subjects with advanced malignancy. The drug was administered by 1-hr intravenous infusion at doses of 0.5 and 2.5 mg/kg. Plasma and blood radioactivity-time, and plasma concentration-time data were defined by a two-compartment open kinetic model. There was nearly equivalent distribution of radioactivity in blood and plasma. The overall mean plasma half-life and total body clearance +/- SD of ACV were 2.1 +/- 0.5 hr and 297 +/- 53 ml/min/1.73 m2. Binding of ACV to plasma proteins was 15.4 +/- 4.4%. Most of the radioactive dose excreted was recovered in the urine (71% to 99%) with less than 2% excretion in the feces and only trace amounts in the expired Co2. Analyses by reverse-phase high-performance liquid chromatography indicated that 9-(carboxymethoxymethyl)guanine was the only significant urinary metabolite of ACV, accounting for 8.5% to 14.1% of the dose. A minor metabolite (less than 0.2% of dose) had the retention time of 8-hydroxy-9-[(2-hydroxyethoxy)methyl]guanine. Unchanged urinary ACV ranged from 62% to 91% of the dose. There was no indication of ACV cleavage to guanine. Renal clearance of ACV was approximately three times the corresponding creatinine clearances.

Published

1981

26. Simultaneous quantification of zidovudine and its glucuronide in serum by high-performance liquid chromatography.

Author

Good SS, Reynolds DJ, and de Miranda P

Subjects

AIDS-Related Complex blood, AIDS-Related Complex drug therapy, Acquired Immunodeficiency Syndrome blood, Acquired Immunodeficiency Syndrome drug therapy, Chromatography, High Pressure Liquid, Glucuronates blood, Humans, Hydrogen-Ion Concentration, Indicators and Reagents, Zidovudine therapeutic use, Zidovudine blood

Abstract

A sensitive high-performance liquid chromatography (HPLC) assay has been developed to simultaneously determine levels of the anti human immunodeficiency virus agent, zidovudine (AZT), and its major metabolite (the 5'-O-glucuronide) in serum. Samples were first mixed with an internal standard (a stereoisomer of AZT), then prepared for analysis using solid-phase extraction columns and chromatographed using a reversed-phase analytical column. Isocratic elution with a mobile phase of 15% acetonitrile, buffered to pH 2.70 with ammonium phosphate, gave good resolution of the three analytes and endogenous serum components. The HPLC analysis time required per sample was 34 min and analyte recoveries were reproducibly high (greater than 93%). Replicate analyses of prepared standards gave satisfactory precision and accuracy, with coefficients of variation less than 15% and deviations from expected concentrations less than 10%.

Published

1988

27. A single-tube radioimmunoassay for the antiviral agent 2,6-diamino-9-(2-hydroxyethoxymethyl)purine (A134U).

Author

Quinn RP, Good SS, Gerald L, and Sabatka JJ

Subjects

Acyclovir blood, Animals, Cross Reactions, Dogs, Drug Stability, Humans, Rabbits, Radioimmunoassay methods, Rats, Acyclovir analogs & derivatives, Antiviral Agents blood

Abstract

A direct radioimmunoassay for the detection of A134U in biological fluids and extracts has been developed. The entire assay, including scintillation counting, is performed using 12 X 55-mm centrifuge tubes and results in a sensitive, reliable, and relatively inexpensive procedure. The log-logit transformation is linear over a range of 1 to 30 pmol per sample. Intra-assay precision was found to be excellent with a coefficient of variation ranging from 4.1 to 14.5% for the standard curve with plasma and a coefficient of variation ranging from 4.0 to 17.8% for the standard curve with urine. Interassay precision and accuracy were also found to be good. With the antisera chosen for use, no cross-reactivity was found with acyclovir or its two known metabolites, while some cross-reactivity was seen with the corresponding two derivatives of A134U. Only very minor cross-reactivities were seen with a small number of other compounds out of a large number tested.

Published

1983

28. A sensitive radioimmunoassay for the antiviral agent BW248U [9-(2-hydroxyethoxymethyl)guanine].

Author

Quinn RP, de Miranda P, Gerald L, and Good SS

Subjects

Animals, Antigen-Antibody Reactions, Cross Reactions, Guanine analysis, Humans, Immune Sera, Immunoassay, Kinetics, Rabbits immunology, Radioimmunoassay methods, Species Specificity, Antiviral Agents analysis, Guanine analogs & derivatives

Published

1979

29. Transport of threonine and tryptophan by rat brain slices: relation to other amino acids at concentrations found in plasma.

Author

Tews JK, Good SS, and Harper AE

Subjects

Amino Acids blood, Animals, Biological Transport, In Vitro Techniques, Kinetics, Male, Rats, Amino Acids metabolism, Brain metabolism, Threonine metabolism, Tryptophan metabolism

Published

1978