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超表面增强的组织中红外光谱化学成像

Metasurface-enhanced mid-infrared spectrochemical imaging of tissues.

作者信息

Rosas S, Schoeller K A, Chang E, Mei H, Kats M A, Eliceiri K W, Zhao X, Yesilkoy F

出版信息

ArXiv. 2023 Apr 27:arXiv:2301.05884v3.

PMID:36713257
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9882561/
Abstract

Label-free and nondestructive mid-infrared vibrational hyperspectral imaging is emerging as an important ex-vivo tissue analysis tool, providing spatially resolved biochemical information critical to understanding physiological and pathological processes. However, the chemically complex and spatially heterogeneous composition of tissue specimens and the inherently weak interaction of infrared light with biomolecules limit the analytical performance of infrared absorption spectroscopy. Here, we introduce an advanced mid-infrared spectrochemical tissue imaging modality using metasurfaces that support strong surface-localized electromagnetic fields to capture quantitative molecular maps of large-area murine brain-tissue sections. Our approach leverages polarization-multiplexed multi-resonance plasmonic metasurfaces to simultaneously detect many different functional biomolecules. The resulting surface-enhanced mid-infrared spectral imaging (SE-MIRSI) method eliminates the non-specific effects of bulk tissue morphology on the quantitative analysis of fingerprint spectra and improves the chemical selectivity. We show that the metasurface enhancement increases the retrieval of amide I and II absorption bands associated with secondary structures of proteins. Moreover, we demonstrate that plasmonic metasurfaces enhance the chemical contrast in infrared images and enable the detection of ultrathin tissue regions that are not otherwise visible to conventional mid-infrared spectral imaging. While we tested our approach on murine brain tissue sections, this chemical imaging method is well-suited for any tissue type, which significantly broadens the potential impacts of our method for both translational research and clinical histopathology.

摘要

无标记且无损的中红外振动高光谱成像正在成为一种重要的离体组织分析工具,它能提供对于理解生理和病理过程至关重要的空间分辨生化信息。然而,组织样本化学组成复杂且空间上具有异质性,以及红外光与生物分子固有的弱相互作用,限制了红外吸收光谱的分析性能。在此,我们介绍一种先进的中红外光谱化学组织成像模式,该模式使用支持强表面局域电磁场的超表面来获取大面积小鼠脑组织切片的定量分子图谱。我们的方法利用偏振复用多共振等离子体超表面同时检测多种不同的功能性生物分子。由此产生的表面增强中红外光谱成像(SE-MIRSI)方法消除了大块组织形态对指纹光谱定量分析的非特异性影响,并提高了化学选择性。我们表明,超表面增强提高了与蛋白质二级结构相关的酰胺I和II吸收带的提取。此外,我们证明等离子体超表面增强了红外图像中的化学对比度,并能够检测到传统中红外光谱成像无法看到的超薄组织区域。虽然我们在小鼠脑组织切片上测试了我们的方法,但这种化学成像方法适用于任何组织类型,这显著拓宽了我们的方法在转化研究和临床组织病理学方面的潜在影响。