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使用受激拉曼散射显微镜和多元曲线分辨-交替最小二乘法测量皮肤中的化学渗透。

Measurement of chemical penetration in skin using Stimulated Raman scattering microscopy and multivariate curve resolution - alternating least squares.

作者信息

Goel Anukrati, Tsikritsis Dimitrios, Belsey Natalie A, Pendlington Ruth, Glavin Stephen, Chen Tao

机构信息

Department of Chemical and Process Engineering, University of Surrey, Guildford, GU2 7XH, UK.

Chemical & Biological Sciences Department, National Physical Laboratory, Hampton Road, Teddington, TW11 0LW, UK.

出版信息

Spectrochim Acta A Mol Biomol Spectrosc. 2023 Aug 5;296:122639. doi: 10.1016/j.saa.2023.122639. Epub 2023 Mar 20.

DOI:10.1016/j.saa.2023.122639
PMID:36989692
Abstract

The mechanistic understanding of skin penetration underpins the design, efficacy and risk assessment of many high-value products including functional personal care products, topical and transdermal drugs. Stimulated Raman scattering (SRS) microscopy, a label free chemical imaging tool, combines molecular spectroscopy with submicron spatial information to map the distribution of chemicals as they penetrate the skin. However, the quantification of penetration is hampered by significant interference from Raman signals of skin constituents. This study reports a method for disentangling exogeneous contributions and measuring their permeation profile through human skin combining SRS measurements with chemometrics. We investigated the spectral decomposition capability of multivariate curve resolution - alternating least squares (MCR-ALS) using hyperspectral SRS images of skin dosed with 4-cyanophenol. By performing MCR-ALS on the fingerprint region spectral data, the distribution of 4-cyanophenol in skin was estimated in an attempt to quantify the amount permeated at different depths. The reconstructed distribution was compared with the experimental mapping of CN, a strong vibrational peak in 4-cyanophenol where the skin is spectroscopically silent. The similarity between MCR-ALS resolved and experimental distribution in skin dosed for 4 h was 0.79 which improved to 0.91 for skin dosed for 1 h. The correlation was observed to be lower for deeper layers of skin where SRS signal intensity is low which is an indication of low sensitivity of SRS. This work is the first demonstration, to the best of our knowledge, of combining SRS imaging technique with spectral unmixing methods for direct observation and mapping of the chemical penetration and distribution in biological tissues.

摘要

对皮肤渗透的机制理解是许多高价值产品(包括功能性个人护理产品、局部和透皮药物)设计、功效和风险评估的基础。受激拉曼散射(SRS)显微镜是一种无标记化学成像工具,它将分子光谱与亚微米空间信息相结合,以绘制化学物质渗透皮肤时的分布情况。然而,皮肤成分的拉曼信号产生的显著干扰阻碍了渗透的量化。本研究报告了一种方法,通过将SRS测量与化学计量学相结合,来区分外源性贡献并测量其通过人体皮肤的渗透情况。我们使用4-氰基苯酚处理皮肤的高光谱SRS图像研究了多元曲线分辨-交替最小二乘法(MCR-ALS)的光谱分解能力。通过对指纹区光谱数据进行MCR-ALS,估计了4-氰基苯酚在皮肤中的分布,试图量化不同深度处的渗透量。将重建的分布与CN的实验图谱进行比较,CN是4-氰基苯酚中的一个强振动峰,而皮肤在该峰处光谱无信号。在4小时处理的皮肤中,MCR-ALS分辨的分布与实验分布之间的相似度为0.79,在1小时处理的皮肤中提高到了0.91。在SRS信号强度较低的皮肤深层观察到相关性较低,这表明SRS的灵敏度较低。据我们所知,这项工作首次展示了将SRS成像技术与光谱解混方法相结合,用于直接观察和绘制生物组织中化学物质的渗透和分布情况。

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