d -鼠李糖基转移酶WbpX和WbpY合成铜绿假单胞菌多糖共同抗原

IF 2.7 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Glycoconjugate Journal Pub Date : 2022-06-01 Epub Date: 2022-02-15 DOI:10.1007/s10719-022-10040-4
Jacob Melamed, Alexander Kocev, Vladimir Torgov, Vladimir Veselovsky, Inka Brockhausen
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引用次数: 3

摘要

革兰氏阴性细菌铜绿假单胞菌同时表达两种o -抗原糖型。虽然o特异性抗原(OSA)在组成上是可变的,但普通多糖抗原(CPA)是高度保守的,由三糖重复单位中的d -鼠李糖(D-Rha)的均聚物[D-Rhaα1-2-D-Rhaα1-3-D-Rha]n组成。我们之前报道过α3-D-Rha转移酶WbpZ将一个D-Rha残基从GDP-D-Rha转移到D-GlcNAcα-O-PO3-PO3-(CH2)11- o -苯基。在O抗原基因簇(wbpX和wbpY)中发现了另外两个编码d - rhad转移酶的基因。本研究表明,在大肠杆菌中重组表达的WbpX和WbpY在供体和受体特异性上存在差异,并具有GT4糖基转移酶家族中GT-B折叠酶的特性。WbpY反应产物的核磁共振波谱分析表明,WbpY将α- 1-3链上的1个D-Rha残基转移合成了D-Rhaα1-3-D-GlcNAcα-O-PO3-PO3-(CH2)11- o -苯基受体。WbpX合成了几个α1-2和α1-3键均含有D-Rha的产物。质谱分析表明,WbpX和WbpY的混合物以非过程机制有效催化了D-Rha低聚物的合成。由于O抗原是毒力因子,这些发现为推进抗菌药物发现和疫苗开发技术打开了大门。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Biosynthesis of the Pseudomonas aeruginosa common polysaccharide antigen by D-Rhamnosyltransferases WbpX and WbpY.

Biosynthesis of the Pseudomonas aeruginosa common polysaccharide antigen by D-Rhamnosyltransferases WbpX and WbpY.

Biosynthesis of the Pseudomonas aeruginosa common polysaccharide antigen by D-Rhamnosyltransferases WbpX and WbpY.

Biosynthesis of the Pseudomonas aeruginosa common polysaccharide antigen by D-Rhamnosyltransferases WbpX and WbpY.

The Gram-negative bacterium Pseudomonas aeruginosa simultaneously expresses two O-antigenic glycoforms. While the O-specific antigen (OSA) is variable in composition, the common polysaccharide antigen (CPA) is highly conserved and is composed of a homopolymer of D-rhamnose (D-Rha) in trisaccharide repeating units [D-Rhaα1-2-D-Rhaα1-3-D-Rhaɑ1-3]n. We have previously reported that α3-D-Rha-transferase WbpZ transfers a D-Rha residue from GDP-D-Rha to D-GlcNAcα-O-PO3-PO3-(CH2)11-O-phenyl. Genes encoding two more D-Rha-transferases are found in the O antigen gene cluster (wbpX and wbpY). In this study we showed that WbpX and WbpY recombinantly expressed in E. coli differ in their donor and acceptor specificities and have properties of GT-B folded enzymes of the GT4 glycosyltransferase family. NMR spectroscopic analysis of the WbpY reaction product showed that WbpY transferred one D-Rha residue in α1-3 linkage to synthetic D-Rhaα1-3-D-GlcNAcα-O-PO3-PO3-(CH2)11-O-phenyl acceptor. WbpX synthesized several products that contained D-Rha in both α1-2 and α1-3 linkages. Mass spectrometry indicated that the mixture of WbpX and WbpY efficiently catalyzed the synthesis of D-Rha oligomers in a non-processive mechanism. Since O antigens are virulence factors, these findings open the door to advancing technology for antibacterial drug discovery and vaccine development.

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来源期刊
Glycoconjugate Journal
Glycoconjugate Journal 生物-生化与分子生物学
CiteScore
6.00
自引率
3.30%
发文量
63
审稿时长
1 months
期刊介绍: Glycoconjugate Journal publishes articles and reviews on all areas concerned with: function, composition, structure, biosynthesis, degradation, interactions, recognition and chemo-enzymatic synthesis of glycoconjugates (glycoproteins, glycolipids, oligosaccharides, polysaccharides and proteoglycans), biochemistry, molecular biology, biotechnology, immunology and cell biology of glycoconjugates, aspects related to disease processes (immunological, inflammatory, arthritic infections, metabolic disorders, malignancy, neurological disorders), structural and functional glycomics, glycoimmunology, glycovaccines, organic synthesis of glycoconjugates and the development of methodologies if biologically relevant, glycosylation changes in disease if focused on either the discovery of a novel disease marker or the improved understanding of some basic pathological mechanism, articles on the effects of toxicological agents (alcohol, tobacco, narcotics, environmental agents) on glycosylation, and the use of glycotherapeutics. Glycoconjugate Journal is the official journal of the International Glycoconjugate Organization, which is responsible for organizing the biennial International Symposia on Glycoconjugates.
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