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关于真菌感染如何影响药物透过甲癣患者甲板渗透的研究。

An investigation of how fungal infection influences drug penetration through onychomycosis patient's nail plates.

作者信息

McAuley W J, Jones S A, Traynor M J, Guesné S, Murdan S, Brown M B

机构信息

Department of Pharmacy, School of Life and Medical Sciences, University of Hertfordshire, College Lane, Hatfield, Hertfordshire AL10 9AB, UK.

Pharmaceutical Science Division, King's College London, Franklin-Wilkins Building, 150 Stamford Street, London SE1 9NH, UK.

出版信息

Eur J Pharm Biopharm. 2016 May;102:178-84. doi: 10.1016/j.ejpb.2016.03.008. Epub 2016 Mar 8.

Abstract

The treatment of onychomycosis remains problematic even though there are several potent antifungal agents available for patient use. The aim of this investigation was to understand whether the structural modifications that arise when a patient's nail become infected plates influences the permeation of drugs into the nail following topical application. It was hoped that through improving understanding of the nail barrier in the diseased state, the development of more effective topical treatments for onychomycosis could be facilitated. The permeation of three compounds with differing hydrophobicities, caffeine, terbinafine and amorolfine (clogD at pH 7.4 of -0.55, 3.72 and 4.49 respectively), was assessed across both healthy and onychomycosis infected, full thickness, human nail plate sections. Transonychial water loss (TOWL) measurements performed on the healthy and diseased nails supported previous observations that the nail behaves like a porous barrier given the lack of correlation between TOWL values with the thicker, diseased nails. The flux of the more hydrophilic caffeine was twofold greater across diseased in comparison with the healthy nails, whilst the hydrophobic molecules terbinafine and amorolfine showed no statistically significant change in their nail penetration rates. Caffeine flux across the nail was found to correlate with the TOWL measurements, though no correlation existed for the more hydrophobic drugs. These data supported the notion that the nail pores, opened up by the infection, facilitated the passage of hydrophilic molecules, whilst the keratin binding of hydrophobic molecules meant that their transport through the nail plate was unchanged. Therefore, in order to exploit the structural changes induced by nail fungal infection it would be beneficial to develop a small molecular weight, hydrophilic antifungal agent, which exhibits low levels of keratin binding.

摘要

尽管有几种有效的抗真菌药物可供患者使用,但甲癣的治疗仍然存在问题。本研究的目的是了解患者指甲感染后结构的改变是否会影响局部用药后药物渗透进入指甲。希望通过更好地了解患病状态下的指甲屏障,能够促进开发更有效的甲癣局部治疗方法。评估了三种具有不同疏水性的化合物咖啡因、特比萘芬和阿莫罗芬(在pH 7.4时的clogD分别为-0.55、3.72和4.49)在健康和感染甲癣的全厚度人指甲板切片中的渗透情况。对健康和患病指甲进行的经甲失水(TOWL)测量支持了先前的观察结果,即鉴于TOWL值与较厚的患病指甲之间缺乏相关性,指甲表现得像一个多孔屏障。与健康指甲相比,亲水性更强的咖啡因在患病指甲中的通量增加了两倍,而疏水性分子特比萘芬和阿莫罗芬的指甲渗透率没有统计学上的显著变化。发现咖啡因在指甲中的通量与TOWL测量结果相关,而疏水性更强的药物则不存在这种相关性。这些数据支持了这样一种观点,即感染使指甲孔隙开放,促进了亲水性分子的通过,而疏水性分子与角蛋白的结合意味着它们在甲板中的转运没有变化。因此,为了利用指甲真菌感染引起的结构变化,开发一种分子量小、亲水性强、对角蛋白结合水平低的抗真菌剂将是有益的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/50de/4827374/02261ef4f0f6/fx1.jpg

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