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离子电渗法实现阳离子肽非侵入性透皮递送的结构-渗透关系

Structure-permeation relationships for the non-invasive transdermal delivery of cationic peptides by iontophoresis.

作者信息

Schuetz Yannic B, Carrupt Pierre-Alain, Naik Aarti, Guy Richard H, Kalia Yogeshvar N

机构信息

Laboratory of Medicinal Chemistry, School of Pharmaceutical Sciences, University of Geneva, Geneva, Switzerland.

出版信息

Eur J Pharm Sci. 2006 Sep;29(1):53-9. doi: 10.1016/j.ejps.2006.05.012. Epub 2006 Jun 3.

Abstract

Transdermal iontophoresis enables the controlled, non-invasive administration of peptide therapeutics. The aims of this study were (i) to evaluate the effect of amino acid sequence and the spatial distribution of peptide physicochemical properties on electrotransport, and (ii) to develop a quantitative model to predict peptide transport rates. Experimental results showed that the distribution of molecular properties over the peptide surface significantly affected iontophoretic delivery: different arrangements of the same residues resulted in different transport behavior. Computational studies generated three-dimensional quantitative structure-permeation relationships (3D-QSPR) based on 3D descriptors. The model predicted that iontophoresis was favored by peptide hydrophilicity but hindered by voluminous, localized hydrophobicity. Molecular characteristics that favor electrotransport are the converse of those required for passive diffusion across biological membranes. The data represent the first analysis of peptide electrotransport in terms of the spatial distribution of molecular properties and provide insight into the ab initio prediction of transdermal iontophoretic peptide delivery.

摘要

经皮离子电渗疗法能够实现肽类治疗药物的可控、非侵入性给药。本研究的目的是:(i)评估氨基酸序列和肽理化性质的空间分布对电转运的影响,以及(ii)建立一个定量模型来预测肽的转运速率。实验结果表明,肽表面分子性质的分布显著影响离子电渗递送:相同残基的不同排列导致不同的转运行为。计算研究基于三维描述符生成了三维定量结构-渗透关系(3D-QSPR)。该模型预测,离子电渗疗法有利于肽的亲水性,但会受到大量局部疏水性的阻碍。有利于电转运的分子特征与跨生物膜被动扩散所需的特征相反。这些数据首次从分子性质的空间分布角度对肽的电转运进行了分析,并为经皮离子电渗肽递送的从头预测提供了见解。

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