Pharmacokinetics and Hepatic Targeting of Trionycis Carapax Peptide Sterically Stabilized Liposomes

TANG Han-xiao; ZHAO Tian-wen; HUANG Yu; SHENG Yun-jie; ZHENG Hang-sheng; ZHANG Yong-sheng

doi:10.13422/j.cnki.syfjx.2017090068

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Pharmacokinetics and Hepatic Targeting of Trionycis Carapax Peptide Sterically Stabilized Liposomes

更新时间：2024-01-04

- Pharmacokinetics and Hepatic Targeting of Trionycis Carapax Peptide Sterically Stabilized Liposomes
- Chinese Journal of Experimental Traditional Medical Formulae Vol. 23, Issue 9, Pages: 68-73(2017)
- 作者机构：
- 作者简介：
- 基金信息：
- DOI：10.13422/j.cnki.syfjx.2017090068
  CLC： R285.5
- Published：2017
- 稿件说明：
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TANG Han-xiao, ZHAO Tian-wen, HUANG Yu, et al. Pharmacokinetics and Hepatic Targeting of Trionycis Carapax Peptide Sterically Stabilized Liposomes[J]. Chinese journal of experimental traditional medical formulae, 2017, 23(9): 68-73.
DOI：

TANG Han-xiao, ZHAO Tian-wen, HUANG Yu, et al. Pharmacokinetics and Hepatic Targeting of Trionycis Carapax Peptide Sterically Stabilized Liposomes[J]. Chinese journal of experimental traditional medical formulae, 2017, 23(9): 68-73. DOI： 10.13422/j.cnki.syfjx.2017090068.

摘要

目的：制备含DiR碘化物荧光染料的长循环脂质体（DiR-SSL），采用SD大鼠和BALB/c裸鼠进行荧光成像的体内靶向性研究，利用空白SSL包封含5-羧基荧光素（5-FAM）的鳖甲肽（HGRFG-5-FAM，HF）制备HGRFG-5-FAM-SSL（HFL），研究HF及HFL分别给药于大鼠的药代动力学。方法：采用薄膜分散法制备DiR-SSL及HFL，取2组SD大鼠分别尾静脉注射HF及HFL，其HF质量浓度及剂量一致，于不同时间点采血，利用多功能微孔板检测仪分析HF血药浓度，计算药代动力学参数；将DiR-SSL尾静脉注射于BALB/c裸鼠，分别于1，2，5，7，24 h活体成像，读取荧光强度值；取正常SD大鼠尾静脉注射DiR-SSL，24 h后解剖心、肝、脾、肺、肾于荧光成像系统成像并读取荧光强度值，将肝组织冷冻切片进行激光共聚焦扫描。结果： HF注射到SD大鼠体内，其半衰期（T1/2）仅0.826 h，而HFL在相同剂量下，T1/2和药时曲线下面积（AUC0-∞）分别为HF的16.253，11.899倍；在BALB/c裸鼠活体成像中，荧光主要集中于肝脏位置，随着时间增加荧光强度逐渐减弱；SD大鼠各脏器中的DiR-SSL荧光在肝脏中最强，注射24 h后DiR-SSL仍能在肝脏储留。结论： SSL递药系统能显著延长HF在SD大鼠体内的T1/2。SSL递药系统具有肝靶向作用，提示该系统可作为药物载体进行肝靶向递药。

Abstract

Objective: In this study

sterically stabilized liposomes (SSL) containing DiR-iodide fluorescent dye (DiR-SSL) was prepared

this liposome was performed on SD rats and BALB/c nude mice for in vivo targeting studies.HGRFG-5-FAM-SSL (HFL) was preparing by SSL loading Trionycis Carapax peptide containing 5-carboxylfluorescein(5-FAM) (HGRFG-5-FAM

HF)

and to investigate pharmacokinetics of administration by HF and HFL in rats

respectively. Method: DiR-SSL and HFL were prepared by thin-film dispersion method.HF and HFL were injected into the tail vein of two groups of SD rats

respectively;the concentration and dose of HF were the same.Plasma samples were collected at different time points and analyzed by multi-function microplate detector

and pharmacokinetic parameters were calculated.DiR-SSL was injected intravenously in BALB/c nude mice

the mice were in vivo imaged respectively at 1

24 h

and fluorescence values were read.The normal SD rats were injected DiR-SSL intravenously

after 24 h

the heart

liver

spleen

lung and kidney were imaged in fluorescence imaging system and fluorescence values were read

frozen sections of liver tissue were taken for confocal laser scanning. Result: After HF being injected into rats

its T1/2 was only 0.826 h;at the same dose

T1/2 and AUC0-∞ of HFL were 16.253 times and 11.899 times that of HF

respectively.In vivo fluorescence imaging of BALB/c nude mice showed fluorescence was mainly in the liver position and weakened gradually over time.The fluorescence of DiR-SSL in the liver of SD rats among different organs was strongest

DiR-SSL remained in the liver tissue at 24 h after injection. Conclusion: SSL drug delivery system can significantly extend T1/2 of HF in SD rats

and this system has a liver targeting effect

suggesting that this system can be used as drug carriers to realize liver targeted drug delivery.

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