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Enzymatic activity of albumin shown by coelenterazine chemiluminescence

生物发光 化学发光 萤光素酶类 生物化学 化学 荧光素酶 发光细菌 光发射 荧光素 明亮发光杆菌 生物 细菌 色谱法 有机化学 基因 遗传学 物理 弧菌 转染 光电子学 毒性
作者
Nasrin Vassel,Charles D. Cox,R Naseem,Valerie Jane Morse,RT Evans,RL Power,Andrea Brancale,Kenneth T. Wann,Anthony K. Campbell
出处
期刊:Luminescence [Wiley]
卷期号:27 (3): 234-241 被引量:49
标识
DOI:10.1002/bio.2357
摘要

Bioluminescence, the emission of light from live organisms, occurs in 18 phyla and is the major communication system in the deep sea. It has appeared independently many times during evolution but its origins remain unknown. Coelenterazine bioluminescence discovered in luminous jellyfish is the most common chemistry causing bioluminescence in the sea, occurring in seven phyla. Sequence similarities between coelenterazine luciferases and photoproteins from different phyla are poor (often < 5%). The aim of this study was to examine albumin that binds organic substances as a coelenterazine luciferase to test the hypothesis that the evolutionary origin of a bioluminescent protein was the result of the formation of a solvent cage containing just a few key amino acids. The results show for the first time that bovine and human albumin catalysed coelenterazine chemiluminescence consistent with a mono-oxygenase, whereas gelatin and haemoglobin, an oxygen carrier, had very weak activity. Insulin also catalysed coelenterazine chemiluminescence and was increased by Zn(2+). Albumin chemiluminescence was heat denaturable, exhibited saturable substrate characteristics and was inhibited by cations that bound these proteins and by drugs that bind to human albumin drug site I. Molecular modelling confirmed the coelenterazine binding site and identified four basic amino acids: lys195, arg222, his242 and arg257, potentially important in binding and catalysis similar to naturally occurring coelenterazine bioluminescent proteins. These results support the 'solvent cage' hypothesis for the evolutionary origin of enzymatic coelenterazine bioluminescent proteins. They also have important consequences in diseases such as diabetes, gut disorders and food intolerance where a mono-oxygenase could affect cell surface proteins.
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