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Development of novel chitosan derivatives as micellar carriers of taxol.

机译:新型壳聚糖衍生物作为紫杉醇的胶束载体的开发。

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摘要

PURPOSE: To develop an intravenous injectable carrier composed of chitosan derivatives for taxol. METHODS: A chitosan with lauryl groups attached to amino groups to provide the hydrophobic moieties and, carboxymethyl groups attached to hydroxy groups to provide the hydrophilic moieties (N-lauryl-carboxymethyl-chitosan = LCC), was newly synthesized. The solubility of taxol in LCC micelles in aqueous solution was examined. The hemolysis test of LCC and the growth inhibition experiment of taxol-loading micelle using KB cells were also performed as in vitro assay. RESULTS: It was found that LCC solubilized taxol by forming micelles with particle sizes less than 100nm. This particle size was considered effective for passive targeting for tumors. The concentration of taxol in the micellar solution was very high, with a maximum of 2.37mg/mL. This maximum was 1000 times above that in a saturated solution of taxol at pH 7.4. Hemolysis testing as an in vitro assay indicated that LCC was safer than Polysorbate 80 (TO-10M) as intravenous surfactant in terms of induction of membrane damage. As judged by cytostatic activity against KB cells, taxol retained activity even when included in LCC micelles. LCC-entrapped taxol was more effective in cytostatic activity than free taxol in low concentrations. CONCLUSIONS: The results of solubilization capacity examination, hemolysis testing, and cytostatic activity suggest that LCC may be useful as a carrier of taxol.
机译:目的:开发一种由紫杉醇的壳聚糖衍生物组成的静脉注射载体。方法:新合成了一个壳聚糖,其中月桂基与氨基相连,以提供疏水部分,羧甲基与羟基相连,以提供亲水部分(N-月桂基-羧甲基-壳聚糖= LCC)。检查紫杉醇在水溶液中LCC胶束中的溶解度。还进行了LCC的溶血试验和使用KB细胞的紫杉醇负载胶束的生长抑制实验作为体外测定。结果:发现LCC通过形成粒径小于100nm的胶束增溶了紫杉醇。该粒径被认为对肿瘤的被动靶向有效。胶束溶液中紫杉醇的浓度很高,最高为2.37mg / mL。该最大值是在pH 7.4的紫杉醇饱和溶液中的最大值的1000倍。作为体外测定的溶血试验表明,就诱导膜损伤而言,LCC比作为表面活性剂的聚山梨酯80(TO-10M)更安全。通过针对KB细胞的细胞抑制活性判断,紫杉醇即使保留在LCC胶束中也保留了活性。携带LCC的紫杉醇在低浓度下比游离紫杉醇在细胞抑制活性方面更有效。结论:溶解能力检查,溶血测试和细胞抑制活性的结果表明,LCC可能作为紫杉醇的载体。

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