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1. Reproductive and developmental toxicology studies of iminosugar UV-4

Author

Jeffry, Shearer, Gary, Wolfe, Mansoora, Khaliq, Brian, Kaufman, Aruna, Sampath, Kelly L, Warfield, Urban, Ramstedt, and Anthony, Treston

Subjects
Male, Mammals, Dose-Response Relationship, Drug, Reproduction, Body Weight, Toxicology, Rats, Rats, Sprague-Dawley, Fertility, Pregnancy, Sperm Motility, Humans, Animals, Female, Rabbits
Abstract

UV-4 (N-(9-methoxynonyl)-1-deoxynojirimycin) is a host-targeted antiviral agent, which targets mammalian proteins (endoplasmic reticulum glucosidases) rather than virally encoded proteins. This mechanism confers both broad-spectrum activity and low potential for generation of viral drug resistance mutations. Reproductive and developmental studies of UV-4 evaluated effects on fertility and early embryonic development in rats, embryo-fetal development in rats and rabbits, and pre- and postnatal development including maternal function in rats. All reproductive and developmental studies conducted achieved dose levels where parental toxicity (generally decreased body weight, decreased food consumption and adverse clinical signs) were observed. Toxicokinetic evaluations confirmed UV-4 crossed the placenta exposing fetal rats and rabbits in utero. Adverse findings in reproductive and developmental studies included decreases in sperm motility with histopathology correlates, visceral and skeletal malformations, changes in eye opening, air drop reflex, vaginal opening and preputial separation. The combined results of the fertility and early embryonic developmental study and pre- and postnatal study suggested that there may be an increased risk for male fertility. These effects are similar to those reported in pre-clinical studies of the structurally related drug Miglustat (N-butyl-1-deoxynojirimycin), therefore UV-4 may have risk of developmental or reproductive adverse outcomes in humans similar to existing approved agents in this drug class.

Published
2022
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2. Investigational New Drug Enabling Nonclinical Safety Pharmacology Assessment of the Iminosugar UV-4, a Broad-Spectrum Host-Targeted Antiviral Agent

Author

Jeffry Shearer, Gary Wolfe, Aruna Sampath, Kelly L Warfield, Brian Kaufman, Urban Ramstedt, and Anthony Treston

Subjects
Mice, Dogs, Drug-Related Side Effects and Adverse Reactions, Drug Evaluation, Preclinical, Animals, Telemetry, Drugs, Investigational, Toxicology, Antiviral Agents, Cardiovascular System, Article
Abstract

UV-4 (N-(9-methoxynonyl)-1-deoxynojirimycin) is a broad-spectrum antiviral drug candidate with demonstrated activity in vitro and in vivo against multiple, diverse viruses. Nonclinical safety pharmacology studies were conducted to support the filing of an Investigational New Drug (IND) application. Preliminary in vitro pharmacology testing evaluating potential for binding to “off-target” receptors and enzymes indicated no significant liability for advanced development of UV-4. The safety pharmacology of UV-4 was evaluated in the in vitro human ether-à-go-go-related gene (hERG) assay, in a central nervous system (CNS) study in the mouse (modified Irwin test), in a respiratory safety study in conscious mice using whole body plethysmography, and in a cardiovascular safety study in conscious, radiotelemetry-instrumented beagle dogs. There were no observed adverse treatment-related effects following administration of UV-4 as the hydrochloride salt in the hERG potassium channel assay, on respiratory function, in the CNS study, or in the cardiovascular assessment. Treatment-related cardiovascular effect of decreased arterial pulse pressure after 50 or 200 mg of UV-4/kg was the only change outside the normal range, and all hemodynamic parameters returned to control levels by the end of the telemetry recording period. These nonclinical safety pharmacology assessments support the evaluation of this host-targeted broad-spectrum antiviral drug candidate in clinical studies.

Published
2022
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3. Investigational New Drug Enabling Nonclinical Safety Assessment of the Iminosugar UV-4, a Broad-Spectrum Host-Targeted Antiviral Agent

Author

Jeffry Shearer, Gary Wolfe, Aruna Sampath, Kelly L. Warfield, Brian Kaufman, Urban Ramstedt, and Anthony Treston

Subjects
Mice, Dogs, Maximum Tolerated Dose, Administration, Oral, Animals, Drugs, Investigational, Toxicology, Antiviral Agents, Rats
Abstract

The iminosugar UV-4 is a broad-spectrum antiviral drug candidate with activity in vitro and in vivo against multiple, diverse viruses. The toxicological profile of UV-4, dosed as the hydrochloride salt, was evaluated in single-dose and repeat-dose oral toxicity studies in mice, rats, dogs, and non-human primates (NHP). No moribundity or deaths were associated with the drug up to the maximum tolerated dose. No treatment-related adverse effects were observed following single oral doses in dogs, rats, and mice up to 250, 400, 1000 mg/kg, respectively, and in NHP up to 180 mg/kg administered three times daily for 10 days. UV-4-related findings were generally seen at higher doses after 7- or 14-day exposure. The most common clinical pathology findings (increase in aspartate aminotransferase and decreased platelet count) were consistently found across species and each appeared dose related. The kidney, mesenteric lymph nodes, stomach including gastrointestinal tract, and thymus were identified as target organs in mice, rats, and dogs. In 14-day repeat-dose toxicology studies in mice and dogs conducted in compliance with Good Laboratory Practice regulations, the dog was considered to be the most sensitive species to UV-4 exposure based on the treatment-related adverse effects noted in the identified target organs. The results of these studies demonstrate the safety profile of UV-4 hydrochloride and supported the selection of starting and maximal doses for a single ascending dose first-in-human clinical study.

Published
2022

5. Phase I safety, pharmacokinetic and pharmacodynamic studies of 2-methoxyestradiol alone or in combination with docetaxel in patients with locally recurrent or metastatic breast cancer.

Author

Jehana James, Daryl Murry, Anthony Treston, Anna Storniolo, George Sledge, Carolyn Sidor, and Kathy Miller

Subjects
CANCER patients, ALKALOIDS, ANTINEOPLASTIC agents, BREAST cancer
Abstract

Summary Purpose: We report the first phase I trials of 2-methoxyestradiol (2ME2, Panzem® Capsules, EntreMed, Rockville, MD), alone and in combination with docetaxel, in patients with metastatic breast cancer (MBC).Patients and methods: In Trial 001, 2ME2 monotherapy was administered orally once (200–1000 mg/d, cohorts 1–5) or twice daily (200–800 mg/q12h, cohorts 6–9) for 28 days followed by a 14-day observation period, continuously thereafter. In Trial 002, docetaxel 35 mg/m2 was administered weekly for four of six weeks for a maximum six cycles; 2ME2 (200–1000 mg/d) was given orally once daily for 28 days followed by a 13-day observation period in cycle one, continuously thereafter. In both trials, responding or stable patients continued 2ME2 until progression.Results: Trial 001 enrolled 31 patients; there were no objective responses. Trial 002 enrolled 15 patients; ORR was 20% including one CR. There were no Grade IV toxicities; MTD was not reached in either study. When combined with docetaxel, three patients had significant transaminase elevations that returned to normal with continued treatment (in two of three patients). There was significant inter-patient variability and extensive metabolism to 2-methoxyestrone (2ME1). Steady-state AUC and trough concentrations of 2ME2 increased linearly up to 400–600 mg/d; doses above 400–600 mg/d did not increase 2ME2 levels. The target trough concentration (3–25 ng/mL) was not attained. Combined administration did not alter docetaxel or 2ME2 pharmacokinetics.Conclusion: 2ME2, alone or in combination with docetaxel, was well tolerated in patients with MBC but systemic exposure remained below the expected therapeutic range. [ABSTRACT FROM AUTHOR]

Published
2007
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8. Identification and synthesis of O-methylcatechol metabolites of phenobarbital and some N-alkyl derivatives

Author

Mervyn J. Eadie, Athena Philippides, Wayne D. Hooper, NW Jacobsen, and Anthony Treston

Subjects
Male, Barbituric acid, Chemistry, Stereochemistry, medicine.medical_treatment, Metabolite, Mephobarbital, Catechols, Pharmaceutical Science, Stereoisomerism, Chemical synthesis, Gas Chromatography-Mass Spectrometry, chemistry.chemical_compound, Anticonvulsant, Phenobarbital, medicine, Humans, Gas chromatography–mass spectrometry, medicine.drug
Abstract

5-Ethyl-5-(4-hydroxy-3-methoxyphenyl) barbituric acid was identified as a new, minor metabolite of phenobarbital in man. The identity of this O-methylcatechol metabolite was confirmed by an unequivocal chemical synthesis, and by GC-MS studies. Mephobarbital and the 1,3-dimethyl, 1-ethyl, and 1,3-diethyl analogues of phenobarbital yielded the corresponding N-alkylated O-methylcatechol metabolites, all of which were confirmed by synthesis. The N-alkyl barbiturates each gave additionally at least one O-methylcatechol metabolite in which N-dealkylation had occurred. These metabolites accounted for approximately 1-5% of the orally administered dose in man.

Published
1987

9. Mechanism of the conversion of a nitrobenzene into a 4-nitrosophenol in 15·8<scp>M</scp>potassium hydroxide

Author

Anthony Treston, Burt Zerner, and Robert L. Blakeley

Subjects
Nitrobenzene, Potassium hydroxide, chemistry.chemical_compound, Proton, chemistry, Inorganic chemistry, 4-nitrosophenol, Molecular Medicine, Hydroxide, Adduct, Ion
Abstract

Quantitative conversion of 2-nitrobenzoate ion into 2-nitroso-5-hydroxybenzoate ion occurs in 15·8 M potassium hydroxide; kinetic and spectral studies are consistent with a mechanism which involves rate-limiting formation of a Meisenheimer adduct with hydroxide ion followed by proton abstraction.

Published
1980
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