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扩展拉曼成像的多重分析能力以揭示高度特异性的分子表达并实现空间分析。

Expanding the Multiplexing Capabilities of Raman Imaging to Reveal Highly Specific Molecular Expression and Enable Spatial Profiling.

作者信息

Eremina Olga E, Czaja Alexander T, Fernando Augusta, Aron Arjun, Eremin Dmitry B, Zavaleta Cristina

机构信息

Department of Biomedical Engineering, University of Southern California, 1042 Downey Way, Los Angeles, California 90089, United States.

Michelson Center for Convergent Bioscience, University of Southern California, 1002 Childs Way, Los Angeles, California 90089, United States.

出版信息

ACS Nano. 2022 Jul 26;16(7):10341-10353. doi: 10.1021/acsnano.2c00353. Epub 2022 Jun 8.

Abstract

Profiling the heterogeneous landscape of cell types and biomolecules is rapidly being adopted to address current imperative research questions. Precision medicine seeks advancements in molecular spatial profiling techniques with highly multiplexed imaging capabilities and subcellular resolution, which remains an extremely complex task. Surface-enhanced Raman spectroscopy (SERS) imaging offers promise through the utilization of nanoparticle-based contrast agents that exhibit narrow spectral features and molecular specificity. The current renaissance of gold nanoparticle technology makes Raman scattering intensities competitive with traditional fluorescence methods while offering the added benefit of unsurpassed multiplexing capabilities. Here, we present an expanded library of individually distinct SERS nanoparticles to arm researchers and clinicians. Our nanoparticles consist of a ∼60 nm gold core, a Raman reporter molecule, and a final inert silica coating. Using density functional theory, we have selected Raman reporters that meet the key criterion of high spectral uniqueness to facilitate unmixing of up to 26 components in a single imaging pixel and . We also demonstrated the utility of our SERS nanoparticles for targeting cultured cells and profiling cancerous human tissue sections for highly multiplexed optical imaging. This study showcases the far-reaching capabilities of SERS-based Raman imaging in molecular profiling to improve personalized medicine and overcome the major challenges of functional and structural diversity in proteomic imaging.

摘要

剖析细胞类型和生物分子的异质性景观正迅速被用于解决当前紧迫的研究问题。精准医学追求在具有高度多路复用成像能力和亚细胞分辨率的分子空间剖析技术方面取得进展,而这仍然是一项极其复杂的任务。表面增强拉曼光谱(SERS)成像通过利用基于纳米颗粒的造影剂展现出了前景,这些造影剂具有窄光谱特征和分子特异性。当前金纳米颗粒技术的复兴使拉曼散射强度与传统荧光方法具有竞争力,同时还具有无与伦比的多路复用能力这一额外优势。在此,我们展示了一个扩展的、包含单个独特SERS纳米颗粒的文库,以助力研究人员和临床医生。我们的纳米颗粒由一个约60纳米的金核、一个拉曼报告分子和一层最终的惰性二氧化硅涂层组成。利用密度泛函理论,我们选择了符合高光谱独特性这一关键标准的拉曼报告分子,以便在单个成像像素中实现多达26种成分的解混。我们还展示了我们的SERS纳米颗粒在靶向培养细胞以及对癌性人体组织切片进行高度多路复用光学成像分析方面的效用。这项研究展示了基于SERS的拉曼成像在分子剖析方面的深远能力,以改善个性化医疗并克服蛋白质组学成像中功能和结构多样性的重大挑战。

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