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用于检测人血清白蛋白的两性离子荧光探针的原位生成

In situ generation of a Zwitterionic fluorescent probe for detection of human serum albumin protein.

作者信息

Choudhury Rajib, Sharma Arun K, Paudel Pratikshya, Wilson Preston, Pereira Andres Barboza

机构信息

Department of Physical Sciences, Arkansas Tech University, Russellville, AR, 72801, United States.

School of Natural Sciences, California State University, Monterey Bay, Seaside, CA, 93955, United States.

出版信息

Anal Biochem. 2022 Jun 1;646:114630. doi: 10.1016/j.ab.2022.114630. Epub 2022 Mar 4.

Abstract

In this article, a new approach for human serum albumin selective fluorophore design has been reported. The fluorophore reported here comprises a substituted phenol donor and a cationic benzo[e]indolium acceptor connected with a π bond. Originally, the cationic fluorophore did not bind with human serum albumin. Upon deprotonation of the phenolic-OH by a water molecule the cationic form was transformed into an active zwitterionic form. Spectroscopic studies and theoretical calculations revealed that the new active form remained in a zwitterionic state in neutral aqueous solution, and it formed a strong supramolecular complex with human serum albumin. The spontaneous complexation resulted multi-fold increase of fluorescence intensity which increased linearly with the concentrations of the protein, thus giving an analytical tool to monitor human serum albumin in aqueous samples. We believe, this simple strategy applied on appropriate fluorogenic scaffolds would prove useful to develop new and improved turn-on fluorescent probes for pH regulated biological applications.

摘要

在本文中,报道了一种用于人血清白蛋白选择性荧光团设计的新方法。此处报道的荧光团由一个取代酚供体和一个通过π键连接的阳离子苯并[e]吲哚鎓受体组成。最初,阳离子荧光团不与人血清白蛋白结合。当酚羟基被水分子去质子化后,阳离子形式转变为活性两性离子形式。光谱研究和理论计算表明,新的活性形式在中性水溶液中保持两性离子状态,并与人血清白蛋白形成强超分子复合物。这种自发络合导致荧光强度增加数倍,且与蛋白质浓度呈线性增加,从而提供了一种监测水性样品中人血清白蛋白的分析工具。我们相信,将这种简单策略应用于合适的荧光支架上,将被证明有助于开发用于pH调节生物应用的新型且改进的开启式荧光探针。

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本文引用的文献

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