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1064nm 分散拉曼微光谱学与药物气溶胶的光阱。

1064 nm Dispersive Raman Microspectroscopy and Optical Trapping of Pharmaceutical Aerosols.

机构信息

Department of Chemistry , University of Cambridge , Cambridge , CB2 1EW , United Kingdom.

School of Geography, Earth and Environmental Sciences , University of Birmingham , Birmingham , B15 2TT , United Kingdom.

出版信息

Anal Chem. 2018 Aug 7;90(15):8838-8844. doi: 10.1021/acs.analchem.8b00817. Epub 2018 Jul 13.

Abstract

Raman spectroscopy is a powerful tool for investigating chemical composition. Coupling Raman spectroscopy with optical microscopy (Raman microspectroscopy) and optical trapping (Raman tweezers) allows microscopic length scales and, hence, femtolitre volumes to be probed. Raman microspectroscopy typically uses UV/visible excitation lasers, but many samples, including organic molecules and complex tissue samples, fluoresce strongly at these wavelengths. Here we report the development and application of dispersive Raman microspectroscopy designed around a near-infrared continuous wave 1064 nm excitation light source. We analyze microparticles (1-5 μm diameter) composed of polystyrene latex and from three real-world pressurized metered dose inhalers (pMDIs) used in the treatment of asthma: salmeterol xinafoate (Serevent), salbutamol sulfate (Salamol), and ciclesonide (Alvesco). For the first time, single particles are captured, optically levitated, and analyzed using the same 1064 nm laser, which permits a convenient nondestructive chemical analysis of the true aerosol phase. We show that particles exhibiting overwhelming fluorescence using a visible laser (514.5 nm) can be successfully analyzed with 1064 nm excitation, irrespective of sample composition and irradiation time. Spectra are acquired rapidly (1-5 min) with a wavelength resolution of 2 nm over a wide wavenumber range (500-3100 cm). This is despite the microscopic sample size and low Raman scattering efficiency at 1064 nm. Spectra of individual pMDI particles compare well to bulk samples, and the Serevent pMDI delivers the thermodynamically preferred crystal form of salmeterol xinafoate. 1064 nm dispersive Raman microspectroscopy is a promising technique that could see diverse applications for samples where fluorescence-free characterization is required with high spatial resolution.

摘要

拉曼光谱是研究化学成分的有力工具。将拉曼光谱与光学显微镜(拉曼显微镜)和光镊(拉曼镊子)相结合,可以探测微观长度尺度,从而探测到飞升体积。拉曼显微镜通常使用紫外/可见激发激光,但许多样品,包括有机分子和复杂的组织样本,在这些波长下强烈荧光。在这里,我们报告了一种围绕近红外连续波 1064nm 激发光源设计的分散拉曼显微镜的开发和应用。我们分析了由聚苯乙烯乳胶组成的微粒子(直径为 1-5μm)和三种用于治疗哮喘的实际压力计量吸入器(pMDI)中的微粒:沙美特罗昔萘酸酯(Serevent)、硫酸沙丁胺醇(Salamol)和环索奈德(Alvesco)。我们首次使用相同的 1064nm 激光捕获、光学悬浮和分析单个颗粒,这允许对真实气溶胶相进行方便的无损化学分析。我们表明,对于使用可见激光(514.5nm)表现出压倒性荧光的颗粒,可以使用 1064nm 激发成功地进行分析,而与样品组成和辐照时间无关。在很宽的波数范围内(500-3100cm),可以快速(1-5 分钟)获得具有 2nm 波长分辨率的光谱,尽管在 1064nm 处样品尺寸较小且拉曼散射效率较低。单个 pMDI 颗粒的光谱与体相样品相比,Serevent pMDI 释放了沙美特罗昔萘酸酯的热力学上优先的晶体形式。1064nm 分散拉曼显微镜是一种很有前途的技术,它可以为需要高空间分辨率进行无荧光特性分析的各种样品提供应用。

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