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首页> 外文期刊>Journal of pharmaceutical sciences. >Influence of drug lipophilicity on drug release from sclera after iontophoretic delivery of mixed micellar carrier system to human sclera
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Influence of drug lipophilicity on drug release from sclera after iontophoretic delivery of mixed micellar carrier system to human sclera

机译:混合胶束载体系统离子导入人体巩膜后,药物亲脂性对药物从巩膜释放的影响

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Mixed micelles prepared using sodium taurocholate (TA) and egg lecithin (LE) were previously found to be an effective carrier for sustained release of a poorly water-soluble drug in transscleral iontophoretic delivery. The objectives of the present study were to investigate the effects of drug lipophilicity upon micellar carrier solubilization potential and drug release profiles from the sclera after iontophoretic delivery of model lipophilic drugs dexamethasone (DEX), triamcinolone acetonide (TRIAM), and β-estradiol (E2β) with a mixed micellar carrier system of TA-LE (1:1 mole ratio). In this study, the micellar carrier system was characterized for drug solubilization. The micelles encapsulating these drugs were evaluated for transscleral passive and 2-mA iontophoretic delivery (both cathodal and anodal) and drug release from excised human sclera in vitro. The results show that drug solubility enhancement of the micellar carrier system increased with increasing drug lipophilicity. The more lipophilic drugs E2β and TRIAM displayed slower drug release from the sclera compared with the less lipophilic drug DEX after iontophoretic drug delivery with the mixed micelles. These results suggest that the combination of transscleral iontophoresis and micellar carriers is more effective in sustaining transscleral delivery of the more lipophilic drugs studied in this investigation.
机译:以前发现使用牛磺胆酸钠(TA)和卵磷脂(LE)制备的混合胶束是在巩膜离子电渗疗法中持续释放水溶性差的药物的有效载体。本研究的目的是研究亲脂性模型药物地塞米松(DEX),曲安奈德(TRIAM)和β-雌二醇(E2β )和TA-LE(1:1摩尔比)的混合胶束载体系统。在这项研究中,胶束载体系统表征了药物的增溶作用。评估封装这些药物的胶束的经巩膜被动和2-mA离子电渗传递(阴极和阳极)以及体外从切除的人巩膜释放的药物。结果表明,随着药物亲脂性的增加,胶束载体系统的药物溶解度增强。与混合胶束一起进行离子电渗疗法药物递送后,与亲脂性药物DEX相比,亲脂性药物E2β和TRIAM越多,从巩膜释放的药物越慢。这些结果表明,跨巩膜离子电渗疗法和胶束载体的组合在维持跨卵泡递送更多亲脂性药物方面更为有效。

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