转运体介导的肾靶向雷公藤内酯醇前体药物TPS-L-Carnitine的合成及体外细胞摄取研究  被引量:2

Cellular Uptake of TPS-L-Carnitine Synthesised as Transporter-based Renal Targeting Prodrug

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作  者:李里[1] 朱迪[2] 孙逊[2] 

机构地区:[1]四川大学华西医院药剂科,成都610041 [2]四川大学华西药学院,成都610041

出  处:《四川大学学报(医学版)》2012年第6期936-940,共5页Journal of Sichuan University(Medical Sciences)

摘  要:目的研究有机阳离子转运体(OCTN2)介导的肾靶向雷公藤内酯醇(TP)前体药物TP丁二酸酯(TPS)-L-肉毒碱(TPS-L-Carnitine)的合成方法和体外靶向细胞摄取。方法将TP与丁二酸酐在碱性条件下生成TPS,再与L-肉毒碱成酯得前体药物TPS-L-Carnitine,利用OCTN2对L-肉毒碱的特异性识别和结合,使前药主动靶向到肾近端小管上皮细胞。初步研究不同温度、浓度以及竞争抑制剂存在时人近端小管上皮细胞株HK-2细胞对前药和母体药物的摄取。结果 HK-2细胞对前药的吸收可饱和,具有温度和浓度依赖性,可被竞争抑制剂抑制,37℃相同给药浓度时,细胞对TPS-L-Carnitine的摄取明显多于TP,证实细胞对TPS-L-Carnitine的摄取机制是通过转运体介导的内吞作用。结论 TPS-L-Carnitine具有良好的肾靶向性,为进一步体内肾靶向研究奠定了基础。Objective To synthesize transporter-based renal targeting prodrug TPS-L-Carnitine and to determine its cellular uptake in vitro. Methods Triptolide (TP) was conjugated with L-carnitine using succinate as the linker to form TPS-L-Carnitine, which could be specifically recognized by OCTN2, a cationic transporter with high affinity to L-Carnitine and is highly expressed on the apical membrane of renal proximal tubule cells. Cellular uptake assays of the prodrug and its parent drug were performed on HK-2 cells, a human proximal tubule cell line, in different temperature, concentration and in the presence of competitive inhibitors. Results TPS-L-Carnitine was taken up into HK-2 cells in a saturable and temperature- and concentration-dependent manner. The uptake process could be inhibited by the competitive inhibitors. The uptake of TPS-L-Carnitine was significantly higher than that of TP at 37℃ in the same drug concentration. TPS-L-Carnitine was taken through endocytosis mediated by transporter. Conclusion TPS-L-Carnitine provides a good renal targeting property and lays the foundation for further studies in vivo.

关 键 词:肾靶向 肾靶向前体药物 雷公藤内酯醇 雷公藤内酯醇丁二酸酯-L-肉毒碱 

分 类 号:R914[医药卫生—药物化学]

 

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