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首页> 外文期刊>Placenta >Effect of lipid composition of cationic SUV liposomes on materno-fetal transfer of warfarin across the perfused human term placenta
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Effect of lipid composition of cationic SUV liposomes on materno-fetal transfer of warfarin across the perfused human term placenta

机译:阳离子SUV脂质体脂质成分对华法林在人胎盘灌注过程中胎-胎转移的影响

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Introduction Use of drugs that cross the placenta freely are currently avoided during pregnancy. We investigated whether cationic small unilamellar (SUV) liposomes of different lipid compositions could prevent the transfer and uptake of warfarin across human term placenta. Methods Cationic liposomes encapsulated warfarin was prepared by using lecithin (F-SUV) or sterylamine (S-SUV) with cholesterol and stearylamine. The size distribution, encapsulation efficiency, and stability were determined in blood-based media. The transfer kinetics of free and liposomally encapsulated warfarin were studied in a dually perfused isolated lobule of human term placenta with creatinine. Concentrations of warfarin were measured by fluorimetry. Data are expressed as % of initial dose added and given as mean ± sd. Results Warfarin crossed the placenta freely (14.9 ± 1.1%). Trans placental transfer of warfarin was significantly reduced by F-SUV (6.4 ± 0.6%; P < 0.001) and S-SUV liposomes (5.0 ± 0.8%; P < 0.001). Placental uptake of F-SUV (6.3 ± 1.7%; P < 0.001) was greater than that of S-SUV liposomes (2.2 ± 0.5%; P < 0.001). Conclusion Our data suggest that cationic liposomes reduce trans placental transfer of warfarin. If confirmed "in vivo", liposomes might provide an alternative non-invasive method of drug delivery to the mother.
机译:引言目前在怀孕期间避免使用可自由穿过胎盘的药物。我们研究了不同脂质组成的阳离子小单层(SUV)脂质体是否可以阻止华法林在人类足月胎盘上的转移和摄取。方法采用卵磷脂(F-SUV)或甾胺(S-SUV)与胆固醇和硬脂胺制备阳离子型华法林脂质体。在基于血液的介质中确定尺寸分布,包封效率和稳定性。游离和脂质体包封的华法令的转移动力学是在人类足月胎盘与肌酐的双重灌注分离小叶中研究的。通过荧光法测量华法林的浓度。数据表示为添加的初始剂量的%,并表示为平均值±sd。结果华法林自由地穿过胎盘(14.9±1.1%)。 F-SUV(6.4±0.6%; P <0.001)和S-SUV脂质体(5.0±0.8%; P <0.001)显着降低了华法林经胎盘的转移。 F-SUV的胎盘摄取(6.3±1.7%; P <0.001)大于S-SUV脂质体的胎盘摄取(2.2±0.5%; P <0.001)。结论我们的数据表明阳离子脂质体可减少华法林的胎盘转运。如果确认为“体内”,脂质体可能会提供另一种非侵入性的方式将药物输送给母亲。

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