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基于吲哚嗪分子框架的全彩色可调聚集诱导发光生色团用于生物成像。

Full Color Tunable Aggregation-Induced Emission Luminogen for Bioimaging Based on an Indolizine Molecular Framework.

机构信息

Department of Molecular Science and Technology, Ajou University, Suwon 16499, Korea.

Department of Chemistry, Ajou University, Suwon 16499, Korea.

出版信息

Bioconjug Chem. 2020 Nov 18;31(11):2522-2532. doi: 10.1021/acs.bioconjchem.0c00467. Epub 2020 Oct 8.

Abstract

By taking advantage of a unique mechanism of aggregation-induced emission (AIE) phenomena, AIE luminogens (AIEgens) have been provided as a solution to overcome the limitations of conventional fluorophores bearing the feature of aggregation-caused quenching (ACQ) phenomena. Especially, AIEgens paved the way to develop fluorogenic probes ideal for fluorescent imaging in live cell conditions. Despite the high demand for discovery of new AIEgens, it is still challenging to find a versatile molecular platform to generate diverse AIEgens. Herein, we report a new colorful molecular framework, Kaleidolizine (KIz), as a molecular platform for AIEgen generation. The KIz system allows systematic tuning of the emission wavelength from 455 to 564 nm via perturbation of the electron density of substituents on the indolizine core. Increasing the water fraction of the KIz solution in the THF/water mixture induces the fluorescence intensity increase up to 120-fold. Crystal structure analysis, computational calculations, and solvatochromism studies suggest that a synergistic effect between the intramolecular charge transfer and restriction of intramolecular rotation acts as the AIE mechanism in the KIz system. Conjugation of the triphenylphosphonium moiety to KIz allows successful development of triphenylphosphonium (TPP)-KIz for real-time bioimaging of innate mitochondria in live cells, thereby revealing the potential of KIz as a versatile molecular platform to generate fluorogenic probes based on AIE phenomena. We do believe the KIz system could serve as a new, reliable, and generally applicable molecular platform to develop various AIEgens having desired photophysical properties along with an excellent signal-to-noise ratio and with experimental convenience especially for fluorogenic live cell imaging.

摘要

通过利用聚集诱导发光(AIE)现象的独特机制,AIE 发光体(AIEgens)已被用作克服具有聚集诱导猝灭(ACQ)现象特征的传统荧光团的局限性的解决方案。特别是,AIEgens 为开发适用于活细胞条件下荧光成像的荧光探针铺平了道路。尽管对发现新的 AIEgens 的需求很高,但仍然很难找到一个通用的分子平台来生成各种 AIEgens。在此,我们报告了一种新的多彩分子框架,Kaleidolizine(KIz),作为生成 AIEgen 的分子平台。通过扰动吲哚嗪核心上取代基的电子密度,KIz 系统允许从 455nm 到 564nm 的发射波长进行系统调谐。在 THF/水混合物中增加 KIz 溶液的水分数可将荧光强度增加高达 120 倍。晶体结构分析、计算计算和溶剂化变色研究表明,分子内电荷转移和分子内旋转限制之间的协同效应是 KIz 系统中的 AIE 机制。将三苯基膦部分与 KIz 共轭允许成功开发三苯基膦(TPP)-KIz,用于实时生物成像活细胞中的天然线粒体,从而揭示了 KIz 作为基于 AIE 现象生成荧光探针的通用分子平台的潜力。我们相信,KIz 系统可以作为一个新的、可靠的和普遍适用的分子平台,用于开发具有所需光物理性质的各种 AIEgens,以及具有出色的信噪比和实验便利性的 AIEgens,特别是用于荧光活细胞成像。

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