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设计并合成一类新型的膜渗透性三氮硼吡咯吡啶荧光探针。

Design and synthesis of a new class of membrane-permeable triazaborolopyridinium fluorescent probes.

机构信息

Department of Chemistry and Biochemistry, New Mexico State University, MSC 3C, Las Cruces, New Mexico 88003, USA.

出版信息

J Am Chem Soc. 2011 May 4;133(17):6780-90. doi: 10.1021/ja2005175. Epub 2011 Apr 7.

Abstract

A new class of fluorescent triazaborolopyridinium compounds was synthesized from hydrazones of 2-hydrazinylpyridine (HPY) and evaluated as potential dyes for live-cell imaging applications. The HPY dyes are small, their absorption/emission properties are tunable through variation of pyridyl or hydrazone substituents, and they offer favorable photophysical characteristics featuring large Stokes shifts and general insensitivity to solvent or pH. The stability, neutral charge, cell membrane permeability, and favorable relative influences on the water solubility of HPY conjugates are complementary to existing fluorescent dyes and offer advantages for the development of receptor-targeted small-molecule probes. This potential was assessed through the development of a new class of cysteine-derived HPY-conjugate imaging agents for the kinesin spindle protein (KSP) that is expressed in the cytoplasm during mitosis and is a promising chemotherapeutic target. Conjugates possessing the neutral HPY or charged Alexa Fluor dyes that function as potent, selective allosteric inhibitors of the KSP motor were compared using biochemical and cell-based phenotypic assays and live-cell imaging. These results demonstrate the effectiveness of the HPY dye moiety as a component of probes for an intracellular protein target and highlight the importance of dye structure in determining the pathway of cell entry and the overall performance of small-molecule conjugates as imaging agents.

摘要

一类新型的荧光三嗪硼吡啶化合物是由 2-腙基吡啶(HPY)的腙与评估作为用于活细胞成像应用的潜在染料。HPY 染料体积小,通过吡啶基或腙取代基的变化可调节其吸收/发射特性,并且具有较大的斯托克斯位移和对溶剂或 pH 值的普遍不敏感性等有利的光物理特性。稳定性,中性电荷,细胞膜通透性以及对 HPY 缀合物水溶性的有利相对影响与现有荧光染料互补,并为开发受体靶向小分子探针提供了优势。通过开发一类新的胱氨酸衍生的 HPY 缀合成像剂来评估这种潜力,该成像剂用于有丝分裂期间在细胞质中表达的驱动蛋白纺锤体蛋白(KSP),并且是有前途的化学治疗靶标。使用生化和基于细胞的表型测定法和活细胞成像比较了具有中性 HPY 或带电荷的 Alexa Fluor 染料的缀合物,这些染料作为 KSP 马达的有效,选择性变构抑制剂。这些结果证明了 HPY 染料部分作为细胞内蛋白质靶标探针的组成部分的有效性,并强调了染料结构在确定细胞进入途径和小分子缀合物作为成像剂的整体性能方面的重要性。

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