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首页> 外文期刊>European journal of pharmaceutical sciences >Effect of amino acid sequence on transdermal iontophoretic peptide delivery.
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Effect of amino acid sequence on transdermal iontophoretic peptide delivery.

机译:氨基酸序列对透皮离子电渗肽递送的影响。

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摘要

The objective of this study was to investigate the effect of amino acid sequence on the transdermal delivery of peptides by iontophoresis. Structurally related, cationic tripeptides based on the residues at positions (i) 6-8 in LHRH (Ac-X-Leu-Arg-NH(2)) and (ii) 3-5 in octreotide (Ac-X-dTrp-Lys-NH(2)) were studied. Iontophoretic transport experiments were conducted using porcine skin in vitro to investigate the dependence of flux on peptide concentration. Co-iontophoresis of acetaminophen enabled deconvolution of the contributions of electromigration (EM) and electroosmosis (EO) and the calculation of an electroosmotic inhibition factor (IF). A two-fold increase in donor peptide concentration increased iontophoretic flux for most peptides, and electroosmotic inhibition for dNal-containing tripeptides. The improvement in transport and the impact on the EM and EO components were peptide-specific. A reduction in the number of competing ions in the formulation significantly increased transport and, specifically, the EM contribution; it also increased IF of compounds with a propensity to interact with the membrane. No monotonic dependence of flux on either molecular weight or lipophilicity was observed. Iontophoretic peptide transport could not be rationalized in terms of either peptide molecular weight or computational 2D estimates of lipophilicity. Data suggest that a more complex three-dimensional approach is required to develop structure permeation relationships governing iontophoretic peptide delivery.
机译:这项研究的目的是研究氨基酸序列对离子电渗疗法对肽透皮递送的影响。基于LHRH(Ac-X-Leu-Arg-NH(2))(i)6-8和(ii)奥曲肽(Ac-X-dTrp-Lys)3-5中位置上的残基的结构相关的阳离子三肽-NH(2))。体外使用猪皮进行离子电渗转运实验,以研究流量对肽浓度的依赖性。对乙酰氨基酚的离子电渗疗法能够解卷积电迁移(EM)和电渗(EO)的作用以及计算电渗抑制因子(IF)。供体肽浓度增加两倍,对大多数肽增加了离子电渗通量,对含dNal的三肽增加了电渗抑制作用。运输的改善以及对EM和EO成分的影响是肽特异性的。配方中竞争离子的数量减少显着增加了迁移,特别是对EM的贡献;它也增加了与膜相互作用的化合物的IF。没有观察到通量对分子量或亲脂性的单调依赖性。不能通过肽分子量或亲脂性的二维计算估计来合理地进行离子电渗疗法的肽运输。数据表明,需要更复杂的三维方法来发展控制离子电渗疗法肽传递的结构渗透关系。

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