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一种具有可调发射波长和斯托克斯位移的近红外荧光染料,可用作监测缺血性中风的高灵敏度半胱氨酸纳米探针。

A Near-Infrared Fluorescent Dye with Tunable Emission Wavelength and Stokes Shift as a High-Sensitivity Cysteine Nanoprobe for Monitoring Ischemic Stroke.

机构信息

State Key Laboratory of Digital Medical Engineering, Jiangsu Laboratory for Biomaterials and Devices, School of Biological Science and Medical Engineering, Southeast University, Nanjing 210096, PR China.

出版信息

ACS Nano. 2024 Jun 18;18(24):15978-15990. doi: 10.1021/acsnano.4c04211. Epub 2024 Jun 7.

DOI:10.1021/acsnano.4c04211
PMID:38847448
Abstract

Sulfur-substituted dicyanomethylene-4-chromene (DCM) derivatives based on the intramolecular charge transfer (ICT) mechanism were designed as near-infrared (NIR) fluorescent dyes. Using the Knoevenagel condensation method, the S-DCM-OH fluorescence dye was synthesized, which had an emission wavelength exceeding 800 nm and 220 nm of a Stokes shift. Compared to commercial ICG, S-DCM-OH was not only synchronized in emission wavelength but also far superior in Stokes shifts. These advantages made the design of S-DCM-NIR based on this dye potentially valuable for biological applications. Based on this chemical structure, a fluorescent S-DCM-NIR nanoprobe with a mean diameter of 17.69 nm was fabricated as the NIR imaging nanoprobe. Results showed that the nanoprobe maintained the high-specificity identification of cysteine (Cys) via the Michael addition reaction, with the detection limitation of 0.11 μM endogenous Cys. More importantly, in an ischemic stroke mouse model, the S-DCM-NIR nanoprobe could monitor the Cys concentration change at stroke lesion due to the disruption of Cys metabolism under the ischemic stroke condition. Such a S-DCM-NIR nanoprobe could not only differentiate the severity of the ischemic stroke using response time but also quantify the concentration of Cys in real-time .

摘要

基于分子内电荷转移(ICT)机制的硫取代二氰基亚甲基-4-色烯(DCM)衍生物被设计为近红外(NIR)荧光染料。通过Knoevenagel 缩合方法合成了 S-DCM-OH 荧光染料,其发射波长超过 800nm,Stokes 位移为 220nm。与商业 ICG 相比,S-DCM-OH 的发射波长不仅同步,而且 Stokes 位移也远优于 ICG。这些优势使得基于这种染料的 S-DCM-NIR 的设计在生物应用方面具有潜在的价值。基于这种化学结构,制备了平均直径为 17.69nm 的荧光 S-DCM-NIR 纳米探针作为 NIR 成像纳米探针。结果表明,该纳米探针通过迈克尔加成反应保持了对半胱氨酸(Cys)的高特异性识别,检测限为 0.11μM 内源性 Cys。更重要的是,在缺血性中风小鼠模型中,由于缺血性中风条件下 Cys 代谢的破坏,S-DCM-NIR 纳米探针可以监测中风病变处 Cys 浓度的变化。这种 S-DCM-NIR 纳米探针不仅可以通过响应时间来区分缺血性中风的严重程度,还可以实时定量 Cys 的浓度。

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