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Aggregation-induced emission spectral shift as a measure of local concentration of a pH-activatable rhodamine-based smart probe

机译:聚集诱导的发射光谱变化作为基于pH激活的罗丹明的智能探针的局部浓度的量度

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AbstractGenerating activatable probes that report about molecular vicinity through contact-based mechanisms such as aggregation can be very convenient. Specifically, such probes change a particular spectral property only at the intended biologically relevant target. Xanthene derivatives, for example rhodamines, are able to form aggregates. It is typical to examine aggregation by absorption spectroscopy but for microscopy applications utilizing fluorescent probes it is very important to perform characterization by measuring fluorescence spectra. First we show that excitation spectra of aqueous solutions of rhodamine 6G can be very informative about the aggregation features. Next we establish the dependence of the fluorescence emission spectral maximum shift on the dimer concentration. The obtained information helped us confirm the possibility of aggregation of a recently designed and synthesized rhodamine 6G-based pH-activatable fluorescent probe and to study its pH and concentration dependence. The size of the aggregation-induced emission spectral shift at specific position on the sample can be measured by fluorescence microspectroscopy, which at particular pH allows estimation of the local concentration of the observed probe at microscopic level. Therefore, we show that besides aggregation-caused quenching and aggregation-induced emission also aggregation-induced emission spectral shift can be a useful photophysical phenomenon.Graphical Abs
机译:<![cdata [ 抽象 生成通过基于接触的机制(例如聚合)的分子附近报告的可激活探头可能非常方便。具体地,这种探针仅在预期的生物学相关目标处改变特定的光谱特性。 Xanthene衍生物,例如罗丹明,能够形成聚集体。通过吸收光谱检查聚集是典型的,但是利用荧光探针的显微镜应用,通过测量荧光光谱来进行表征是非常重要的。首先,我们表明罗丹明6g水溶液的激发光谱可以非常有信息地对聚集特征提供信息。接下来,我们建立荧光发射光谱最大变化对二聚体浓度的依赖性。所获得的信息有助于我们确认了最近设计和合成的罗丹明6G基的pH-活化荧光探针的聚集的可能性,并研究其pH和浓度依赖性。可以通过荧光微谱检测样品上的特定位置处的聚集诱导的发射光谱偏移的尺寸,特别是pH允许在显微镜水平下估计观察到的探针的局部浓度。因此,我们表明除了聚集导致的淬火和聚集诱导的发射之外,聚集诱导的发射光谱偏移也可以是有用的光药现象。 图形ABS

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