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经皮给药后聚合物纳米胶囊的体内毒理学评价。

In vivo toxicological evaluation of polymeric nanocapsules after intradermal administration.

机构信息

Programa de Pós-Graduação em Ciências Farmacêuticas, Universidade Federal do Rio Grande do Sul, Brazil; Laboratório de Toxicologia (LATOX), Universidade Federal do Rio Grande do Sul, Porto Alegre, Brazil.

Departamento de Ciências Básicas da Saúde, Universidade Federal de Ciências da Saúde de Porto Alegre, Porto Alegre, Brazil.

出版信息

Eur J Pharm Biopharm. 2014 Feb;86(2):167-77. doi: 10.1016/j.ejpb.2013.04.001. Epub 2013 May 2.

Abstract

Polymeric nanocarriers have shown great promise as delivery systems. An alternative strategy has been to explore new delivery routes, such as intradermal (i.d.), that can be used for vaccines and patch-based drug delivery. Despite their many advantages, there are few toxicity studies, especially in vivo. We report a safety assessment of biodegradable poly(ɛ-caprolactone) lipid-core nanocapsules (LNC) with a mean size of 245±10nm following single and repeated intradermal injections to Wistar rats. Suspensions were prepared by interfacial deposition of polymer. The animals (n=6/group) received a single-dose of saline solution (1.2ml/kg) or LNC (7.2×10(12)LNC/kg), or repeated-doses of two controls, saline solution or Tween 80 (0.9ml/kg), or three different concentrations of LNC (1.8, 3.6, and 5.4×10(12)LNC/kg) for 28 consecutive days. Clinical and physiological signs and mortality were observed. Samples of urine, blood, and tissue were used to perform toxicological evaluation. There were no clinical signs of toxicity or mortality, but there was a slight decrease in the relative body weights in the Tween 80-treated group (p<0.01) after repeated administration. No histopathological alterations were observed in tissues or significant changes in blood and urinary biomarkers for tissue damage. Mild alterations in white blood cells count with increases in granulocytes in the Tween-80 group (p<0.05) were found. Genotoxicity was evaluated through the comet assay, and no statistical difference was observed among the groups. Therefore, we conclude that, under the conditions of these experiments, biodegradable LNC did not present appreciable toxicity after 28 consecutive days of intradermal administration and is promising for its future application in vaccines and patch-based devices for enhancing the delivery of drugs.

摘要

聚合物纳米载体作为递药系统显示出巨大的应用前景。另一种策略是探索新的给药途径,如皮内(i.d.)途径,可用于疫苗和贴剂给药。尽管它们有许多优点,但很少有关于毒性的研究,尤其是体内研究。我们报告了一种生物可降解聚(ε-己内酯)脂质核纳米胶囊(LNC)的安全性评估,该纳米胶囊的平均粒径为 245±10nm,单次和重复皮内注射 Wistar 大鼠后。通过界面沉积聚合物制备混悬液。动物(每组 6 只)单次给予生理盐水(1.2ml/kg)或 LNC(7.2×10(12)LNC/kg),或重复给予生理盐水或吐温 80(0.9ml/kg)两种对照药物,或三种不同浓度的 LNC(1.8、3.6 和 5.4×10(12)LNC/kg),连续 28 天。观察临床和生理体征及死亡率。采集尿液、血液和组织样本进行毒理学评价。吐温 80 处理组在重复给药后(p<0.01)相对体重略有下降,但未见毒性或死亡的临床体征。组织未见组织病理学改变,血液和尿液组织损伤生物标志物也无显著变化。在吐温 80 组发现白细胞计数略有改变,粒细胞计数增加(p<0.05)。通过彗星试验评估遗传毒性,各组间未见统计学差异。因此,我们得出结论,在这些实验条件下,生物可降解 LNC 连续 28 天皮内给药后未见明显毒性,有望用于疫苗和贴剂给药装置,增强药物传递。

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