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发色团异构体的稳定对青色荧光蛋白的高效荧光至关重要。

Chromophore Isomer Stabilization Is Critical to the Efficient Fluorescence of Cyan Fluorescent Proteins.

作者信息

Gotthard Guillaume, von Stetten David, Clavel Damien, Noirclerc-Savoye Marjolaine, Royant Antoine

机构信息

European Synchrotron Radiation Facility , F-38043 Grenoble, France.

Univ. Grenoble Alpes, CNRS, CEA, IBS (Institut de Biologie Structurale), F-38000 Grenoble, France.

出版信息

Biochemistry. 2017 Dec 12;56(49):6418-6422. doi: 10.1021/acs.biochem.7b01088. Epub 2017 Nov 27.

Abstract

ECFP, the first usable cyan fluorescent protein (CFP), was obtained by adapting the tyrosine-based chromophore environment in green fluorescent protein to that of a tryptophan-based one. This first-generation CFP was superseded by the popular Cerulean, CyPet, and SCFP3A that were engineered by rational and random mutagenesis, yet the latter CFPs still exhibit suboptimal properties of pH sensitivity and reversible photobleaching behavior. These flaws were serendipitously corrected in the third-generation CFP mTurquoise and its successors without an obvious rationale. We show here that the evolution process had unexpectedly remodeled the chromophore environment in second-generation CFPs so they would accommodate a different isomer, whose formation is favored by acidic pH or light irradiation and which emits fluorescence much less efficiently. Our results illustrate how fluorescent protein engineering based solely on fluorescence efficiency optimization may affect other photophysical or physicochemical parameters and provide novel insights into the rational evolution of fluorescent proteins with a tryptophan-based chromophore.

摘要

增强型青色荧光蛋白(ECFP)是首个可用的青色荧光蛋白(CFP),它是通过将绿色荧光蛋白中基于酪氨酸的发色团环境调整为基于色氨酸的发色团环境而获得的。第一代CFP已被通过理性和随机诱变工程改造的流行的天蓝蛋白(Cerulean)、CyPet和SCFP3A所取代,但后几种CFP仍表现出pH敏感性和可逆光漂白行为等次优特性。这些缺陷在第三代CFP mTurquoise及其后续变体中意外地得到了纠正,且没有明显的理论依据。我们在此表明,进化过程意外地重塑了第二代CFP中的发色团环境,使其能够容纳一种不同的异构体,该异构体的形成在酸性pH或光照条件下更有利,且发出的荧光效率要低得多。我们的结果说明了仅基于荧光效率优化的荧光蛋白工程可能如何影响其他光物理或物理化学参数,并为基于色氨酸发色团的荧光蛋白的合理进化提供了新的见解。

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