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首页> 外文期刊>Vaccine >Mannosamine-biotin as a novel masking agent for coating IgG for immune response silencing and augmentation of antibody-antigen interaction.
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Mannosamine-biotin as a novel masking agent for coating IgG for immune response silencing and augmentation of antibody-antigen interaction.

机译:甘露糖胺-生物素作为一种新型的掩蔽剂,用于包被IgG,以实现免疫应答沉默和抗体-抗原相互作用的增强。

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摘要

A variety of protein-coating procedures are used to modify proteins' properties. The principle coating agent used is PEGylation, in which proteins are coated by conjunction to polyethylene glycol (PEG). In the present study, we describe a novel approach that makes use of small molecules with multifunctional groups as the protein-coating agent. The new coating molecule was produced by reacting two endogenous molecules, mannosamine and biotin, to form mannose-biotin adducts (MBA). hIgG was coated with MBA at various MBA/protein ratios. The immunogenicity of MBA-coated hIgG was tested in chickens. A dose-responsive effect of MBA/hIgG ratio on immune response suppression was detected, with an optimal masking effect at a 12:1 ratio. The immune response to MBA-coated hIgG was about eightfold lower than that to PEG-coated hIgG. MBA also increased antibody-antigen-binding affinity, and decreased recognition of the Fc domain of MBA-coated hIgG by Fc receptor and secondary antibodies. While the PEG molecule consists of inert repeating units of ethylene oxide with no additional functional group to allow for potentially desirable modifications, the MBA has several functional groups, including vicinal hydroxyls, which can easily be converted to active residues such as aldehydes or carboxyls. This may be of importance for developing passive immunizations or for achieving tolerance of the immune response to an immunogenic molecule or virus. In summary, we developed a new protein-coating molecule with the ability to mask foreign antigens and in the case of antibodies, to enhance activity.
机译:多种蛋白质包被程序可用于修饰蛋白质的特性。所用的主要包衣剂是PEG化,其中蛋白质通过与聚乙二醇(PEG)结合被包被。在本研究中,我们描述了一种新颖的方法,该方法利用具有多功能基团的小分子作为蛋白质涂层剂。通过使两个内源性分子甘露糖胺和生物素反应形成甘露糖-生物素加合物(MBA),可以生产出新的涂层分子。 hIgG用各种MBA /蛋白质比率的MBA包被。在鸡中测试了MBA包被的hIgG的免疫原性。检测了MBA / hIgG比例对免疫应答抑制的剂量反应效应,最佳掩盖效应为12:1。对MBA包被的hIgG的免疫应答比对PEG包被的hIgG的免疫应答低约八倍。 MBA还增加了抗体-抗原结合亲和力,并降低了Fc受体和二抗对MBA包被的hIgG的Fc结构域的识别。尽管PEG分子由环氧乙烷的惰性重复单元组成,没有额外的官能团以允许潜在的修饰,但MBA具有几个官能团,包括邻位羟基,可以轻松转化为活性残基,例如醛或羧基。这对于开发被动免疫或实现对免疫原性分子或病毒的免疫应答的耐受性可能是重要的。总之,我们开发了一种新的蛋白质涂层分子,能够掩盖外源抗原,并且在抗体的情况下具有增强活性的能力。

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