Principles, modulation, and applications of fluorescent protein chromophores

IF 6.1 Q2 CHEMISTRY, PHYSICAL
Songtao Ye, Yuqi Tang, Xin Zhang
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引用次数: 2

Abstract

Fluorescent proteins (FPs) have gained much attention over the last few decades as powerful tools in bioimaging since the discovery of green fluorescent protein (GFP) in the 1960s. The mechanism of FP bioluminenscence has been well-studied, and new variants with improved photophysical properties are being constantly generated. In this review, a brief history of GFP along with its biogenesis is first provided. Next, the fluorescent and quenching mechanism governing the photophysical property of GFP is elaborated. Most importantly, we seek to introduce the expanding family of FP derivatives that mimics the chromophore core structure of FPs. Multiple physical and chemical strategies have been discussed to minimize the inherent fluorescence quenching effect of FP derivatives. Finally, we briefly overview the biological application of FP derivatives, with a focus on fluorescent RNA aptamer and recently reported protein aggregation detection probes. Through citing and discussing the most important works in this field, this review aims to provide a general photophysical understanding regarding the luminescence phenomenon of GFP and its derivatives, as well as chemical strategies to design functional FP derivatives.
荧光蛋白发色团的原理、调制及其应用
自20世纪60年代发现绿色荧光蛋白(GFP)以来,荧光蛋白(FP)作为生物成像的有力工具,在过去几十年中受到了广泛关注。FP生物发光的机制已经得到了很好的研究,并且不断产生具有改进的光物理性质的新变体。在这篇综述中,首先提供了GFP及其生物发生的简要历史。接下来,阐述了控制GFP光物理性质的荧光和猝灭机制。最重要的是,我们试图引入FP衍生物的扩展家族,该家族模拟FP的发色团核心结构。已经讨论了多种物理和化学策略来最小化FP衍生物固有的荧光猝灭效应。最后,我们简要概述了FP衍生物的生物学应用,重点介绍了荧光RNA适体和最近报道的蛋白质聚集检测探针。通过引用和讨论该领域最重要的工作,本综述旨在提供对GFP及其衍生物发光现象的一般光物理理解,以及设计功能性FP衍生物的化学策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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