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半乳糖化聚合物载体用于索拉非尼的肝靶向。

Galactosylated polymeric carriers for liver targeting of sorafenib.

机构信息

Dipartimento di Scienze e Tecnologie Biologiche Chimiche e Farmaceutiche (STEBICEF), Sezione di Chimica e Tecnologie Farmaceutiche, Università di Palermo, via Archirafi 32, 90123 Palermo, Italy.

Dipartimento di Scienze e Tecnologie Biologiche Chimiche e Farmaceutiche (STEBICEF), Sezione di Biologia Cellulare, Università di Palermo, viale delle Scienze, edificio 16, 90128 Palermo, Italy.

出版信息

Int J Pharm. 2014 May 15;466(1-2):172-80. doi: 10.1016/j.ijpharm.2014.02.047. Epub 2014 Mar 4.

Abstract

In this paper, we describe the preparation of liver-targeted polymeric micelles potentially able to carry sorafenib to hepatocytes for treatment of hepatocarcinoma (HCC), exploiting the presence of carbohydrate receptors, ASGPR. These micelles were prepared starting from a galactosylated polylactide-polyaminoacid conjugate. This latter was obtained by chemical reaction of α,β-poly(N-2-hydroxyethyl) (2-aminoethylcarbamate)-d,l-aspartamide (PHEA-EDA) with polylactic acid (PLA), and subsequent reaction with lactose, leading to PHEA-EDA-PLA-GAL copolymer. Liver-targeted sorafenib-loaded micelles were obtained in aqueous media at low PHEA-EDA-PLA-GAL copolymer concentration value with nanometer size and slightly positive zeta potential. Biodistribution studies on mice demonstrated, after oral administration of sorafenib loaded PHEA-EDA-PLA-GAL micelles, the preferential sorafenib accumulation into the liver. This finding raises hope in terms of future drug delivery strategy of sorafenib-loaded micelles targeted to the liver for the HCC treatment.

摘要

在本文中,我们描述了肝靶向聚合物胶束的制备,这些胶束有可能携带索拉非尼进入肝细胞,用于治疗肝癌(HCC),利用了碳水化合物受体 ASGPR 的存在。这些胶束是从半乳糖化聚丙交酯-聚氨基酸缀合物开始制备的。该缀合物通过 α,β-聚(N-2-羟乙基)(2-氨基乙基碳酸酯)-d,l-天冬酰胺(PHEA-EDA)与聚乳酸(PLA)的化学反应,以及随后与乳糖的反应而得到,得到 PHEA-EDA-PLA-GAL 共聚物。在低 PHEA-EDA-PLA-GAL 共聚物浓度值的水性介质中,得到了具有纳米尺寸和略带正 ζ 电位的肝靶向索拉非尼载药胶束。在小鼠中的分布研究表明,口服索拉非尼负载的 PHEA-EDA-PLA-GAL 胶束后,索拉非尼优先积聚在肝脏中。这一发现为索拉非尼负载的靶向肝脏的胶束的药物输送策略提供了未来治疗 HCC 的希望。

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