Abstract

Introduction One of the perspective approaches to the development of anticancer chemotherapy drugs is the use of submicron vectorized delivery systems that increase the selectivity of action and reduce the toxic side effects of chemotherapy. A delivery system of docetaxel (DOC) loaded poly(lactide-co-glycolide) (PLGA) particles modified with folic acid dodecylamide (FAD) was developed (PLGA-DOC-FAD). The aim of the research was a comparative toxicological study of DOC-loaded particles and standard docetaxel solution form in acute and subchronic experiments in mice after intravenous administration. Materials and methods The research was conducted in female C57BL/6 mice. During the study of acute toxicity, drugs were administered in the following dose range: 20, 60, 90, 120, 160 mg/kg. Over 30 days, mortality and body weight were evaluated, pathomorphological studies were performed. The study of toxicity in conditions of subchronic administration of medicine was conducted using three times daily administration in single doses of 11 and 22 mg/kg. Subchronic toxicity of the drugs was studied with three times daily administration in single doses of 11 and 22 mg/kg. The necessary studies were performed within 30 days. Results With a single injection of PLGA-DOC-FAD in doses of 20, 60, 90 mg/kg, the death of animals wasn’t observed; at doses of 120 and 160 mg/kg, the death of animals was detected in 1–4 days. In the case of administration of the DOC substance, the death of animals occurred within a day after the administration of doses of 60, 90, 120, 160 mg/kg. The pattern of intoxication was similar in case of compared drugs and manifested in hypodynamia, impaired movement coordination, hind limbs paresis, though the manifestation degree thereof was more expressed in the groups with the introduction of DOC than in the case of the introduction of PLGA-DOC-FAD. It was detected that the LD 50 for PLGA-DOC-FAD is 140 mg/kg, and for the DOC substance – 112 mg/kg. In case of subchronic administration, the detected toxic properties of drug depend on the size of the dose applied. The administration of a single dose of 22 mg/kg of PLGA - DOC-FAD caused lethal effects (2/10), reversible delay in weight gain and leucopenia in surviving animals, and an increase in the relative mass of the spleen. The use of PLGA-DOC-FAD in a single dose of 11 mg/kg didn’t cause death, was well tolerated and characterized by similar toxicity with the docetaxel substance. Conclusion Based on experimental data, the toxic dose levels of PLGA-DOC-FAD were determined under acute and subchronic administration. The results obtained allowed us to recommend PLGA-DOC-FAD for further examination.

Highlights

  • One of the perspective approaches to the development of anticancer chemotherapy drugs is the use of submicron vectorized delivery systems that increase the selectivity of action and reduce the toxic side effects of chemotherapy

  • A delivery system of docetaxel (DOC) loaded poly(lactide-co-glycolide) (PLGA) particles modified with folic acid dodecylamide (FAD) was developed (PLGA-DOC-FAD)

  • The pattern of intoxication was similar in case of compared drugs and manifested in hypodynamia, impaired movement coordination, hind limbs paresis, though the manifestation degree thereof was more expressed in the groups with the introduction of DOC than in the case of the introduction of PLGA-DOC-FAD

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Summary

ПОЛИМЕРНЫХ ЧАСТИЦ В ЭКСПЕРИМЕНТЕ IN VIVO

Разработана система доставки доцетаксела (ДОЦ) в составе полилактидгликолидных частиц (poly(lactic-co-glycolic acid), PLGA), модифицированных додециламидом фолиевой кислоты (ДФК) (частицы PLGAДОЦ-ДФК). Цель исследования – сравнительное токсикологическое исследование ДОЦ в форме частиц и в стандартной форме в остром и субхроническом экспериментах на мышах при внутривенном введении. При 1‐кратном введении PLGA-ДОЦ-ДФК в дозах 20, 60, 90 мг / кг гибели животных не наблюдалось; в дозах 120 и 160 мг / кг выявлена гибель животных на 1–4‐е сутки. Введение PLGA-ДОЦ-ДФК в разовой дозе 22 мг / кг вызывало летальные эффекты (2 / 10), обратимую задержку прироста массы и лейкопению у выживших животных, увеличение относительной массы селезенки. На основании экспериментальных данных определены уровни токсических доз PLGA-ДОЦ-ДФК при остром и субхроническом введении. Для цитирования: Крашенинникова А.А., Заварзина В.В., Панова Д.С.

Introduction
Контроль Control
Контрольная группа Control group
Substance DOC
Печень Liver Почки Kidneys Селезенка Spleen Легкие Lungs Сердце Heart
Findings
Изучена токсичность ДОЦ в составе частиц

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