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首页> 外文期刊>International Journal of Pharmaceutics >Inhibition of liver metastasis by all-trans retinoic acid incorporated into O/W emulsions in mice.
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Inhibition of liver metastasis by all-trans retinoic acid incorporated into O/W emulsions in mice.

机译:掺入小鼠O / W乳剂的全反式视黄酸对肝转移的抑制作用。

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All-trans retinoic acid (ATRA) was incorporated into lipid emulsions in an attempt to alter its distribution characteristics and improve its inhibition of liver cancer metastasis. Lipid emulsions composed of egg phosphatidylcholine, cholesterol, and soybean oil were the optimized carriers for ATRA delivery, as shown by the submicron particle size and high incorporation efficiency. The particle size and zeta potential of ATRA incorporated into emulsions were about 133nm and -11mV, respectively. In vitro drug release study demonstrated that the release of ATRA from emulsions was sustained in the absence and present of bovine serum albumin, suggesting that ATRA was stable when incorporated in emulsions. After intravenous administration in mice, [(3)H]cholesteryl hexadecyl ether incorporated into emulsion, which is the inherent distribution of emulsions, accumulated gradually mainly in the liver. The blood concentration and hepatic accumulation of [(3)H]ATRA incorporated into emulsion was significantly higher than that of serum dissolving [(3)H]ATRA, which represent the original distribution characteristic of free ATRA. In a murine liver metastasis model by colon adenocarcinoma, the liver metastasis number and liver weight were significantly reduced and the survival time of mice was prolonged following intravenous injection of ATRA incorporated into emulsions.
机译:将全反式视黄酸(ATRA)掺入脂质乳剂中,以试图改变其分布特征并改善其对肝癌转移的抑制作用。如亚微米粒径和高掺入效率所示,由蛋磷脂酰胆碱,胆固醇和大豆油组成的脂质乳液是用于ATRA输送的最佳载体。掺入乳液中的ATRA的粒径和Zeta电位分别约为133nm和-11mV。体外药物释放研究表明,在不存在和存在牛血清白蛋白的情况下,乳状液中ATRA的释放得以持续,这表明掺入乳状液中时ATRA是稳定的。在小鼠中静脉内给药后,[(3)H]胆固醇基十六烷基醚掺入乳液中,这是乳液的固有分布,主要在肝脏中逐渐积累。掺入乳剂中的[(3)H] ATRA的血药浓度和肝蓄积显着高于血清溶解的[(3)H] ATRA,这代表游离ATRA的原始分布特征。在由结肠腺癌引起的鼠肝转移模型中,将ATRA静脉注射到乳状液中后,肝转移数目和肝脏重量显着减少,小鼠的存活时间延长。

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