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用于将未硫酸化硫酸软骨素酶促硫酸化并生成3'-磷酸腺苷-5'-磷酰硫酸(PAPS)的生物催化级联反应的设计。

Design of a biocatalytic cascade for the enzymatic sulfation of unsulfated chondroitin with generation of PAPS.

作者信息

Monterrey Dianelis T, Benito-Arenas Raúl, Revuelta Julia, García-Junceda Eduardo

机构信息

Department Bio-Organic Chemistry, BioGlycoChem Group, Instituto de Química Orgánica General (IQOG-CSIC), Spanish National Research Council, Madrid, Spain.

出版信息

Front Bioeng Biotechnol. 2023 Jan 16;11:1099924. doi: 10.3389/fbioe.2023.1099924. eCollection 2023.

Abstract

Sulfation of molecules in living organisms is a process that plays a key role in their functionality. In mammals, the sulfation of polysaccharides (glycosaminoglycans) that form the proteoglycans present in the extracellular matrix is particularly important. These polysaccharides, through their degree and sulfation pattern, are involved in a variety of biological events as signal modulators in communication processes between the cell and its environment. Because of this great biological importance, there is a growing interest in the development of efficient and sustainable sulfation processes, such as those based on the use of sulfotransferase enzymes. These enzymes have the disadvantage of being 3'-phosphoadenosine 5'-phosphosulfate (PAPS) dependent, which is expensive and difficult to obtain. In the present study, a modular multienzyme system was developed to allow the synthesis of PAPS and its coupling to a chondroitin sulfation system. For this purpose, the bifunctional enzyme PAPS synthase 1 (PAPSS1) from , which contains the ATP sulfurylase and APS kinase activities in a single protein, and the enzyme chondroitin 4--sulfotransferase (C4ST-1) from were overexpressed in . The product formed after coupling of the PAPS generation system and the chondroitin sulfation module was analyzed by NMR.

摘要

生物体内分子的硫酸化是一个在其功能中起关键作用的过程。在哺乳动物中,构成细胞外基质中蛋白聚糖的多糖(糖胺聚糖)的硫酸化尤为重要。这些多糖通过其硫酸化程度和模式,作为细胞与其环境之间通讯过程中的信号调节剂,参与多种生物事件。由于其巨大的生物学重要性,人们对开发高效且可持续的硫酸化过程越来越感兴趣,例如基于使用硫酸转移酶的过程。这些酶的缺点是依赖3'-磷酸腺苷5'-磷酸硫酸酯(PAPS),而PAPS既昂贵又难以获得。在本研究中,开发了一种模块化多酶系统,以实现PAPS的合成及其与硫酸软骨素硫酸化系统的偶联。为此,来自 的双功能酶PAPS合酶1(PAPSS1)(其在单一蛋白质中包含ATP硫酸化酶和APS激酶活性)以及来自 的酶硫酸软骨素4-O-硫酸转移酶(C4ST-1)在 中过表达。通过核磁共振分析PAPS生成系统和硫酸软骨素硫酸化模块偶联后形成的产物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/169a/9885120/b0d2a4552f07/fbioe-11-1099924-g001.jpg

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