Literature DB >> 27486796

Live-Cell Bioorthogonal Chemical Imaging: Stimulated Raman Scattering Microscopy of Vibrational Probes.

Lu Wei1, Fanghao Hu1, Zhixing Chen1, Yihui Shen1, Luyuan Zhang1, Wei Min1,2.   

Abstract

Innovations in light microscopy have tremendously revolutionized the way researchers study biological systems win class="Chemical">th subcellular resolution. In particular, fluorescence microscopy with the expanding choices of fluorescent probes has provided a comprehensive toolkit to tag and visualize various molecules of interest with exquisite specificity and high sensitivity. Although fluorescence microscopy is currently the method of choice for cellular imaging, it faces fundamental limitations for studying the vast number of small biomolecules. This is because common fluorescent labels, which are relatively bulky, could introduce considerable perturbation to or even completely alter the native functions of vital small biomolecules. Hence, despite their immense functional importance, these small biomolecules remain largely undetectable by fluorescence microscopy. To address this challenge, a bioorthogonal chemical imaging platform has recently been introduced. By coupling stimulated Raman scattering (SRS) microscopy, an emerging nonlinear Raman microscopy technique, with tiny and Raman-active vibrational probes (e.g., alkynes and stable isotopes), bioorthogonal chemical imaging exhibits superb sensitivity, specificity, and biocompatibility for imaging small biomolecules in live systems. In this Account, we review recent technical achievements for visualizing a broad spectrum of small biomolecules, including ribonucleosides and deoxyribonucleosides, amino acids, fatty acids, choline, glucose, cholesterol, and small-molecule drugs in live biological systems ranging from individual cells to animal tissues and model organisms. Importantly, this platform is compatible with live-cell biology, thus allowing real-time imaging of small-molecule dynamics. Moreover, we discuss further chemical and spectroscopic strategies for multicolor bioorthogonal chemical imaging, a valuable technique in the era of "omics". As a unique tool for biological discovery, this platform has been applied to studying various metabolic processes under both physiological and pathological states, including protein synthesis activity of neuronal systems, protein aggregations in Huntington disease models, glucose uptake in tumor xenografts, and drug penetration through skin tissues. We envision that the coupling of SRS microscopy with vibrational probes would do for small biomolecules what fluorescence microscopy of fluorophores has done for larger molecular species.

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Year:  2016        PMID: 27486796      PMCID: PMC5704954          DOI: 10.1021/acs.accounts.6b00210

Source DB:  PubMed          Journal:  Acc Chem Res        ISSN: 0001-4842            Impact factor:   22.384


  51 in total

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Review 3.  Chemistry in living systems.

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4.  Live-cell stimulated Raman scattering imaging of alkyne-tagged biomolecules.

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5.  Highly Sensitive Vibrational Imaging by Femtosecond Pulse Stimulated Raman Loss.

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Review 6.  The need for speed.

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8.  Measuring electric fields and noncovalent interactions using the vibrational stark effect.

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9.  Noninvasive imaging of protein metabolic labeling in single human cells using stable isotopes and Raman microscopy.

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Review 10.  Chemical contrast for imaging living systems: molecular vibrations drive CARS microscopy.

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  32 in total

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3.  Determination of the Subcellular Localization and Mechanism of Action of Ferrostatins in Suppressing Ferroptosis.

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Review 7.  Applications of vibrational tags in biological imaging by Raman microscopy.

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9.  Bioorthogonal chemical imaging of metabolic changes during epithelial-mesenchymal transition of cancer cells by stimulated Raman scattering microscopy.

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10.  Stimulated Raman Scattering: From Bulk to Nano.

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