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Rationally Designed TLR4 Ligands for Vaccine Adjuvant Discovery.用于疫苗佐剂发现的合理设计的TLR4配体
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Lipid A structural modifications in extreme conditions and identification of unique modifying enzymes to define the Toll-like receptor 4 structure-activity relationship.在极端条件下脂 A 结构的修饰以及鉴定独特的修饰酶来定义 Toll 样受体 4 的结构-活性关系。
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Autopiquer - a Robust and Reliable Peak Detection Algorithm for Mass Spectrometry.Autopiquer——一种用于质谱分析的强大且可靠的峰检测算法。
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Rapid lipid a structure determination via surface acoustic wave nebulization and hierarchical tandem mass spectrometry algorithm.通过表面声波雾化和分级串联质谱算法快速确定脂质A结构
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Analysis of Bacterial Lipooligosaccharides by MALDI-TOF MS with Traveling Wave Ion Mobility.基质辅助激光解吸电离飞行时间质谱联用行波离子淌度分析细菌脂寡糖。
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21 Tesla Fourier Transform Ion Cyclotron Resonance Mass Spectrometer: A National Resource for Ultrahigh Resolution Mass Analysis.21 特斯拉傅里叶变换离子回旋共振质谱仪:超高分辨率质谱分析的国家资源。
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Absorption mode Fourier transform mass spectrometry with no baseline correction using a novel asymmetric apodization function.采用新型非对称变迹函数且无基线校正的吸收模式傅里叶变换质谱法。
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Producing Isotopic Distribution Models for Fully Apodized Absorption Mode FT-MS.为全变迹吸收模式傅里叶变换质谱仪生成同位素分布模型。
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Non-canonical activation of inflammatory caspases by cytosolic LPS in innate immunity.天然免疫中胞质脂多糖对炎症性半胱天冬酶的非经典激活
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Top-Down Strategies for the Structural Elucidation of Intact Gram-negative Bacterial Endotoxins.用于完整革兰氏阴性菌内毒素结构解析的自上而下策略。
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化学修饰粗糙型脂多糖疫苗候选物的自上而下串联质谱分析。

Top Down Tandem Mass Spectrometric Analysis of a Chemically Modified Rough-Type Lipopolysaccharide Vaccine Candidate.

机构信息

School of Medicine, University of Maryland, Baltimore, MD, 21201, USA.

National High Magnetic Field Laboratory, Florida State University, Tallahassee, FL, 32310, USA.

出版信息

J Am Soc Mass Spectrom. 2018 Jun;29(6):1221-1229. doi: 10.1007/s13361-018-1897-y. Epub 2018 Feb 20.

DOI:10.1007/s13361-018-1897-y
PMID:29464544
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8294406/
Abstract

Recent advances in lipopolysaccharide (LPS) biology have led to its use in drug discovery pipelines, including vaccine and vaccine adjuvant discovery. Desirable characteristics for LPS vaccine candidates include both the ability to produce a specific antibody titer in patients and a minimal host inflammatory response directed by the innate immune system. However, in-depth chemical characterization of most LPS extracts has not been performed; hence, biological activities of these extracts are unpredictable. Additionally, the most widely adopted workflow for LPS structure elucidation includes nonspecific chemical decomposition steps before analyses, making structures inferred and not necessarily biologically relevant. In this work, several different mass spectrometry workflows that have not been previously explored were employed to show proof-of-principle for top down LPS primary structure elucidation, specifically for a rough-type mutant (J5) E. coli-derived LPS component of a vaccine candidate. First, ion mobility filtered precursor ions were subjected to collision induced dissociation (CID) to define differences in native J5 LPS v. chemically detoxified J5 LPS (dLPS). Next, ultra-high mass resolving power, accurate mass spectrometry was employed for unequivocal precursor and product ion empirical formulae generation. Finally, MS analyses in an ion trap instrument showed that previous knowledge about dissociation of LPS components can be used to reconstruct and sequence LPS in a top down fashion. A structural rationale is also explained for differential inflammatory dose-response curves, in vitro, when HEK-Blue hTLR4 cells were administered increasing concentrations of native J5 LPS v. dLPS, which will be useful in future drug discovery efforts. Graphical Abstract ᅟ.

摘要

脂多糖 (LPS) 生物学的最新进展使其在药物发现管道中得到应用,包括疫苗和疫苗佐剂的发现。LPS 疫苗候选物的理想特征包括在患者中产生特定抗体滴度的能力和由固有免疫系统指导的最小宿主炎症反应。然而,大多数 LPS 提取物的深入化学表征尚未进行;因此,这些提取物的生物学活性是不可预测的。此外,最广泛采用的 LPS 结构阐明工作流程包括在分析之前进行非特异性化学分解步骤,从而使推断的结构不一定具有生物学相关性。在这项工作中,采用了几种以前未探索过的不同质谱工作流程,以证明用于 LPS 一级结构阐明的自上而下方法的原理,特别是对于候选疫苗的粗糙型突变 (J5) 大肠杆菌衍生 LPS 成分。首先,对离子迁移过滤的前体离子进行碰撞诱导解离 (CID),以定义天然 J5 LPS 与化学解毒 J5 LPS (dLPS) 的差异。接下来,采用超高质量分辨率、精确质量质谱法生成明确的前体和产物离子经验公式。最后,在离子阱仪器中进行的 MS 分析表明,可以使用关于 LPS 成分解离的先前知识以自上而下的方式重构和测序 LPS。还解释了体外 HEK-Blue hTLR4 细胞给予天然 J5 LPS 与 dLPS 时,不同炎症剂量反应曲线的结构原理,这将对未来的药物发现工作有用。