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采用衰减全反射红外光谱法在体内测量经皮渗透增强情况。

Percutaneous penetration enhancement in vivo measured by attenuated total reflectance infrared spectroscopy.

作者信息

Mak V H, Potts R O, Guy R H

机构信息

Department of Pharmacy, University of California, San Francisco 94143.

出版信息

Pharm Res. 1990 Aug;7(8):835-41. doi: 10.1023/a:1015960815578.

Abstract

A novel application of attenuated total reflectance IR spectroscopy (ATR-IR) was used to monitor the outer several microns of the stratum corneum (SC) and, thereby, demonstrate enhanced percutaneous absorption in vivo in man. 4-Cyanophenol (CP) as a model permeant yielded a unique IR signal, distinct from those of the stratum corneum and the vehicle components. CP was administered for 1, 2, or 3 hr as a 10% (w/v) solution either in propylene glycol or in propylene glycol containing 5% (v/v) oleic acid. The absorbance at 2230 cm-1, which corresponded to C identical to N bond stretching, diminished significantly faster when CP was codelivered with oleic acid. An IR absorbance due primarily to propylene glycol at 1040 cm-1 (C-O stretching) also disappeared more quickly following application of the enhancer-containing solution. In addition, only the formulations with oleic acid induced a higher wavenumber shift in the frequency of the asymmetric C-H bond stretching absorbance. This change indicates increased lipid-chain disorder, the mechanism by which oleic acid is believed to cause enhanced drug transport across the stratum corneum. Therefore, ATR-IR permits one to examine noninvasively the kinetics, extent, and mechanism of percutaneous penetration enhancement in vivo in human subjects.

摘要

衰减全反射红外光谱(ATR - IR)的一种新应用被用于监测角质层(SC)外层的几微米,并由此证明人体体内经皮吸收增强。4 - 氰基苯酚(CP)作为模型渗透剂产生了独特的红外信号,与角质层和载体成分的信号不同。CP以10%(w/v)的溶液形式在丙二醇或含有5%(v/v)油酸的丙二醇中给药1、2或3小时。对应于碳氮三键拉伸的2230 cm-1处的吸光度,当CP与油酸共同给药时,其下降速度明显更快。在应用含增强剂的溶液后,主要归因于丙二醇的1040 cm-1(碳氧键拉伸)处的红外吸光度也更快消失。此外,只有含油酸的制剂在不对称碳氢键拉伸吸光度的频率上引起了更高的波数偏移。这种变化表明脂质链无序性增加,这被认为是油酸导致药物跨角质层转运增强的机制。因此,ATR - IR允许人们在人体受试者体内非侵入性地研究经皮渗透增强的动力学、程度和机制。

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