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Preparation, characterization and in vivo distribution of solid lipid nanoparticles loaded with syringopicroside.

机译:载有丁香甙的固体脂质纳米颗粒的制备,表征和体内分布。

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A solvent emulsification evaporation method was employed to prepare solid lipid nanoparticles (SLN) loaded with syringopicroside. The conventional broad-spectrum antibacterial and antiviral drug syringopicroside was incorporated into SLN to improve drug targeting. The SYR-SLNs were spherical and uniform in transmission electron microscopy (TEM). The mean particle size and potential were 180.31 +/- 10 nm, and -41.9 +/- 10.3 mV, respectively. Also, a sephadex column chromatography was adopted to investigate the encapsulation efficiency (EE %) of the SLN. This method is based on the principle of molecular sieve effect, and the EE% of the optimal formulation was 42.35 %. Drug-loading capacity was 5.33 %. The in vitro release profile revealed that syringopicroside was released from SLN efficiently and completely in normal saline (NS) compared with other release media. A HPLC method was established for in vivo assay of syringopicroside. A tissue distribution study was conducted in rats after iv administration of 15 mg/kg SYR-SLN and syringopicroside NS, and it was found that SYR-SLN has improved delivery to the liver compared with any other organizations. These results indicated that solvent emulsification evaporation is a simple, easy, available and effective method for preparing SYR-SLN.
机译:采用溶剂乳化蒸发法制备了载有丁香甙的固体脂质纳米粒(SLN)。将常规的广谱抗菌和抗病毒药丁香甙加入SLN中以改善药物靶向性。 SYR-SLNs是球形的,在透射电子显微镜(TEM)中是均匀的。平均粒径和电势分别为180.31 +/- 10 nm和-41.9 +/- 10.3 mV。另外,采用葡聚糖凝胶柱色谱法研究SLN的包封率(EE%)。该方法基于分子筛效应原理,最佳配方的EE%为42.35%。载药量为5.33%。体外释放曲线表明,与其他释放介质相比,丁香三倍苷在生理盐水(NS)中有效而完全地从SLN中释放出来。建立了一种高效液相色谱法,用于丁香甙的体内测定。静脉内注射15 mg / kg SYR-SLN和丁香甙NS后,在大鼠中进行了组织分布研究,发现SYR-SLN与任何其他组织相比均改善了向肝脏的递送。这些结果表明,溶剂乳化蒸发是一种制备SYR-SLN的简单,简便,有效的方法。

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