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跨越可见光到短波红外波段的生物吸收光谱特征

Characterization of Biological Absorption Spectra Spanning the Visible to the Short-Wave Infrared.

作者信息

Gruensfelder Hannah D R, Shofu Folaoluwashewa, Michie Megan S, Berezin Mikhail Y, Shmuylovich Leonid, O'Brien Christine M

机构信息

Department of Biomedical Engineering, Washington University in St. Louis.

Department of Radiology, Washington University in St. Louis.

出版信息

J Vis Exp. 2025 Jan 10(215). doi: 10.3791/67403.

Abstract

For noninvasive light-based physiological monitoring, optimal wavelengths of individual tissue components can be identified using absorption spectroscopy. However, because of the lack of sensitivity of hardware at longer wavelengths, absorption spectroscopy has typically been applied for wavelengths in the visible (VIS) and near-infrared (NIR) range from 400 to 1,000 nm. Hardware advancements in the short-wave infrared (SWIR) range have enabled investigators to explore wavelengths in the ~1,000 nm to 3,000 nm range in which fall characteristic absorption peaks for lipid, protein, and water. These molecules are difficult to visualize in the VIS-NIR and can provide label-free sources of biological contrast. Furthermore, lower SWIR absorption has been observed for melanin, the primary chromophore responsible for skin pigmentation. In vivo optical devices like clinically standard pulse oximeters have been found to have reduced accuracy in people with darkly pigmented skin, possibly because of the stronger melanin absorption in the VIS range. Thus, error associated with skin pigmentation could be reduced by using devices operating in the SWIR. Optical instrument design is facilitated by the understanding of the absorption properties of core tissue components from the VIS to the SWIR range. This article describes protocols and instrumentation for obtaining VIS-SWIR absorption spectra of common tissue absorbers: oxygenated hemoglobin, deoxygenated hemoglobin, melanin, water, and lipid.

摘要

对于基于光的无创生理监测,可以使用吸收光谱法来识别各个组织成分的最佳波长。然而,由于硬件在较长波长下缺乏灵敏度,吸收光谱法通常应用于400至1000纳米的可见光(VIS)和近红外(NIR)范围内的波长。短波红外(SWIR)范围内的硬件进步使研究人员能够探索1000纳米至3000纳米范围内的波长,其中包含脂质、蛋白质和水的特征吸收峰。这些分子在VIS-NIR范围内难以可视化,并且可以提供无标记的生物对比度来源。此外,已观察到黑色素(导致皮肤色素沉着的主要发色团)在SWIR下的吸收较低。已发现临床标准脉搏血氧仪等体内光学设备在皮肤色素沉着较深的人群中准确性降低,这可能是因为黑色素在VIS范围内的吸收更强。因此,使用在SWIR下工作的设备可以减少与皮肤色素沉着相关的误差。对从VIS到SWIR范围的核心组织成分的吸收特性的了解有助于光学仪器设计。本文介绍了获取常见组织吸收剂(含氧血红蛋白、脱氧血红蛋白、黑色素、水和脂质)的VIS-SWIR吸收光谱的方案和仪器。

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