Abstract
Introduction. The antiviral properties of imidazolyl ethanamide pentandioic acid (IPA), the active compound of the drug product, has been proven in various experimental models. However, the literature data on the toxicological properties of IPA are limited.Purpose. To evaluate mutagenic and genotoxic properties in in vitro and in vivo models, as well as to study the toxicity of IPA following chronic oral administration to rats and dogs.Materials and methods. Mutagenic and genotoxic properties of IPA were assessed using the Ames test, the test of chromosomal aberrations in human lymphocytes, and the micronucleus test in rats. The chronic toxicity of IPA was studied in Sprague Dawley rats and beagle dogs of both sexes, to which IPA was administered orally at doses of 30-300 mg/kg/day for 26 and 39 weeks, respectively.Results and discussion. In the Ames test, the addition of IPA up to the maximum dose (5000 mcg/plate) did not result in the increase in the number of revertant colonies. At a concentration of up to 5000 mcg/ml, IPA did not cause chromosomal aberrations in human leukocytes. At doses doses ≤ 2000 mg/kg, IPA did not increase the amount of micronuclei in the bone marrow of rats. In chronic experiments, animals tolerated the administration of IPA well: the dose without an observed effect (NOEL) for rats and dogs was 300 mg/kg/day.Conclusion. IPA did not show mutagenic and genotoxic properties in standard in vitro and in vivo tests. With chronic oral administration to rats and dogs, NOEL IPA equal to 300 mg/kg/day provided a systemic exposure that was 8-10 and 41-65 times higher than that in humans, respectively. The results obtained allow us to consider the safety profile of the prolonged use in humans as favorable.
Highlights
The antiviral properties of imidazolyl ethanamide pentandioic acid (IPA), the active compound of the drug product, has been proven in various experimental models
The chronic toxicity of IPA was studied in Sprague Dawley rats and beagle dogs of both sexes, to which IPA was administered orally at doses of 30–300 mg/kg/day for 26 and 39 weeks, respectively
At doses ≤ 2000 mg/kg, IPA did not increase the amount of micronuclei in the bone marrow of rats
Summary
Генотоксичности и хронической токсичности имидазолилэтанамида пентандиовой кислоты в тест-системах in vitro и in vivo. Оценить мутагенные и генотоксические свойства на моделях in vitro и in vivo, а также токсичность ИПК при хроническом пероральном введении крысам и собакам. Мутагенные и генотоксические свойства ИПК оценивали в тесте Эймса, в тесте хромосомных аберраций на лимфоцитах человека, в микроядерном тесте у крыс. В хронических экспериментах животные хорошо переносили введение ИПК: доза без наблюдаемого эффекта (NOEL) для крыс и собак составляла 300 мг/кг/сут. При хроническом пероральном введении крысам и собакам NOEL ИПК, равная 300 мг/кг/сут, обеспечивала системную экспозицию, превышающую таковую у человека в 8–10 и в 41–65 раз соответственно. Сотрудники АО «Валента Фарм» (Россия) участвовали в анализе данных и подготовке публикации. Работа финансировалась фармацевтической компанией АО «Валента Фарм» (Россия) и «Myelo Therapeutics GmbH» (Германия). Evaluation of mutagenicity, genotoxicity and chronic toxicity of antiviral drug imidazolyl ethanamide pentandioic acid in in vitro and in vivo test systems
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