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铜催化近红外荧光花菁染料的共价二聚化:用于肿瘤分子成像的光声信号协同增强

Copper-Catalyzed Covalent Dimerization of Near-Infrared Fluorescent Cyanine Dyes: Synergistic Enhancement of Photoacoustic Signals for Molecular Imaging of Tumors.

作者信息

Maji Dolonchampa, Oh Donghyeon, Gautam Krishna Sharmah, Zhou Mingzhou, Zhang Haini, Kao Jeff, Giblin Daryl, Smith Matthew, Lim Junha, Lee Seunghyun, Kang Youngnam, Kim Won Jong, Kim Chulhong, Achilefu Samuel

机构信息

Optical Radiology Lab, Department of Radiology Washington University School of Medicine St. Louis, MO 63110 (USA).

Department of Biomedical Engineering Washington University in St. Louis St. Louis, MO 63130 (USA).

出版信息

Anal Sens. 2022 Jan;2(1). doi: 10.1002/anse.202100045. Epub 2021 Oct 15.

Abstract

Photoacoustic (PA) imaging relies on the absorption of light by chromophores to generate acoustic waves used to delineate tissue structures and physiology. Here, we demonstrate that Cu(II) efficiently catalyzes the dimerization of diverse near-infrared (NIR) cyanine molecules, including a peptide conjugate. NMR spectroscopy revealed a C-C covalent bond along the heptamethine chains, creating stable molecules under conditions such as a wide range of solvents and pH mediums. Dimerization achieved >90% fluorescence quenching, enhanced photostability, and increased PA signals by a factor of about 4 at equimolar concentrations compared to the monomers. study with a mouse cancer model revealed that dimerization enhanced tumor retention and PA signal, allowing cancer detection at doses where the monomers are less effective. While the dye dimers highlighted peritumoral blood vessels, the PA signal for dimeric tumor-targeting dye-peptide conjugate, LS301, was diffuse throughout the entire tumor mass. A combination of the ease of synthesis, diversity of molecules that are amenable to Cu(II)-catalyzed dimerization, and the high acoustic wave amplification by these stable dimeric small molecules ushers a new strategy to develop clinically translatable PA molecular amplifiers for the emerging field of molecular photoacoustic imaging.

摘要

光声(PA)成像依靠发色团对光的吸收来产生用于描绘组织结构和生理特征的声波。在此,我们证明了铜(II)能有效催化多种近红外(NIR)花菁分子(包括一种肽缀合物)的二聚化。核磁共振光谱显示沿着七甲川链存在碳 - 碳共价键,在诸如多种溶剂和pH介质等条件下形成稳定分子。与单体相比,二聚化实现了>90%的荧光猝灭、增强的光稳定性,并在等摩尔浓度下使光声信号增加约4倍。对小鼠癌症模型的研究表明,二聚化增强了肿瘤滞留和光声信号,使得在单体效果较差的剂量下也能检测到癌症。虽然染料二聚体突出了肿瘤周围血管,但二聚体肿瘤靶向染料 - 肽缀合物LS301的光声信号在整个肿瘤块中是弥散的。铜(II)催化二聚化易于合成、分子多样性以及这些稳定二聚体小分子的高声波放大相结合,为分子光声成像这一新兴领域开发临床可转化的光声分子放大器带来了一种新策略。

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