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从……的脂多糖中获得的脂质A的质谱分析。 (你提供的原文不完整,这里只是根据现有内容翻译)

Mass spectrometric analysis of lipid A obtained from the lipopolysaccharide of .

作者信息

Tawab Abdul, Akbar Noor, Hasssan Mujtaba, Habib Fazale, Ali Aamir, Rahman Moazur, Jabbar Abdul, Rauf Waqar, Iqbal Mazhar

机构信息

Health Biotechnology Division, National Institute for Biotechnology and Genetic Engineering (NIBGE) P.O. Box 577, Jhang Road Faisalabad-38000 Pakistan

Department of Biotechnology NIBGE, Pakistan Institute of Engineering and Applied Sciences (PIEAS) Lehtrar Road Nilore Islamabad-45650 Pakistan.

出版信息

RSC Adv. 2020 Aug 20;10(51):30917-30933. doi: 10.1039/d0ra05463a. eCollection 2020 Aug 17.

DOI:10.1039/d0ra05463a
PMID:35516050
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9056370/
Abstract

Haemorrhagic septicaemia is mainly caused by an opportunistic pathogen, , a major threat to the livestock dependent economies. The main endotoxins are lipopolysaccharides. The lipid A, a key pathogenic part of lipopolysaccharides, anchors it into the bacterial cell membrane. Hence, profiling of the lipid A is important to understand toxicity of this pathogen. Despite a significant progress made on glycan analyses of core regions of lipopolysaccharides from various strains, the structure of lipid A has not been reported yet. The lipid A of type B:2 was analyzed using ESI-MS/MS to identify the acylation patterns, number and length of various acyl fatty acids, phosphorylation level and lipid A modifications. The MS data revealed the existence of multiple lipid A variants, mono and bisphosphorylated hepta-, hexa-, penta- and tetra-acylated structures, decorated with varied levels of 4-amino-4-deoxy-l-arabinose (Ara4N) on C-1 and/or C-4' phosphate groups of proximal and distal glucosamine lipid A backbone. The detailed mass spectrometric analyses revealed that even within the same class, lipid A exhibits several sub-variant structures. A primary and secondary myristoylation at C-2, C-3, C-2' and C-3' was observed in all variants except hepta-acylated lipid A that carried a secondary palmitate at C-2 position. The lipid A profiling described herein, may contribute in exploring the mechanisms involved in endotoxicity of type B:2 in haemorrhagic septicaemia disease.

摘要

出血性败血症主要由一种机会性病原体引起,对依赖畜牧业的经济体构成重大威胁。主要内毒素是脂多糖。脂多糖的关键致病部分脂质A将其锚定在细菌细胞膜中。因此,分析脂质A对于了解这种病原体的毒性很重要。尽管在对来自各种菌株的脂多糖核心区域的聚糖分析方面取得了重大进展,但脂质A的结构尚未见报道。使用电喷雾串联质谱(ESI-MS/MS)分析B:2型的脂质A,以确定酰化模式、各种酰基脂肪酸的数量和长度、磷酸化水平以及脂质A修饰。质谱数据揭示了多种脂质A变体的存在,即单磷酸化和双磷酸化的七酰化、六酰化、五酰化和四酰化结构,在近端和远端葡糖胺脂质A主链的C-1和/或C-4'磷酸基团上装饰有不同水平的4-氨基-4-脱氧-L-阿拉伯糖(Ara4N)。详细的质谱分析表明,即使在同一类别中,脂质A也呈现出几种亚变体结构。在所有变体中均观察到C-2、C-3、C-2'和C-3'处的一级和二级肉豆蔻酰化,除了在C-2位置带有二级棕榈酸酯的七酰化脂质A。本文所述的脂质A分析可能有助于探索B:2型在出血性败血症疾病中的内毒素毒性所涉及的机制。

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