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以丝状噬菌体作为模型抗原,制定增强和聚焦体液免疫反应的策略。

Developing strategies to enhance and focus humoral immune responses using filamentous phage as a model antigen.

作者信息

Henry Kevin A, Murira Armstrong, van Houten Nienke E, Scott Jamie K

机构信息

Department of Molecular Biology and Biochemistry, Simon Fraser University, 8888 University Drive, Burnaby, BC V5A1S6, Canada.

出版信息

Bioeng Bugs. 2011 Sep-Oct;2(5):275-83. doi: 10.4161/bbug.2.5.16559. Epub 2011 Sep 1.

Abstract

Filamentous bacteriophage are commonly used as immunogenic carriers for peptides and proteins displayed on the phage surface. Previously, we showed that immunization with phage to which peptides had been chemically conjugated can elicit a focused anti-peptide antibody response compared with traditional carrier molecules bearing the same peptide, perhaps due to the low surface complexity of the phage. The regularity of its surface also gives the phage other advantages as a carrier, including immunological simplicity and thousands of well-defined sites for chemical conjugation. More recently, we showed that focusing of antibody responses against 'target' peptides was enhanced when the phage's molecular surface was simplified by removal of immunodominant B-cell epitopes present on the minor coat protein, pIII. The pIII-truncated variant elicits an antibody response that is largely restricted to the exposed N-terminus of the major coat protein, pVIII, and to phage-associated bacterial lipopolysaccharide, and a significant fraction of this response cross-reacts with a 12-residue peptide covering the surface-exposed region of pVIII. This allows one to track antibody responses against the phage (and any associated haptens) as they develop over time, and characterize them using a combination of serological, flow cytometric, cellular and immunogenetic assays. The filamentous phage thus provides an excellent model system for studying various aspects of the antibody response, all with the goal of targeting antibody production against weakly immunogenic peptides, proteins and carbohydrates.

摘要

丝状噬菌体通常用作噬菌体表面展示的肽和蛋白质的免疫原性载体。此前,我们发现,与携带相同肽的传统载体分子相比,用化学偶联了肽的噬菌体进行免疫可引发集中的抗肽抗体反应,这可能是由于噬菌体表面复杂性较低。其表面的规则性也赋予噬菌体作为载体的其他优势,包括免疫学简单性以及数千个明确的化学偶联位点。最近,我们发现,当通过去除次要外壳蛋白pIII上存在的免疫显性B细胞表位来简化噬菌体的分子表面时,针对“靶标”肽的抗体反应聚焦得到增强。截短pIII的变体引发的抗体反应主要局限于主要外壳蛋白pVIII暴露的N端以及噬菌体相关的细菌脂多糖,并且该反应的很大一部分与覆盖pVIII表面暴露区域的12个残基肽发生交叉反应。这使得人们能够追踪随着时间推移针对噬菌体(以及任何相关半抗原)产生的抗体反应,并使用血清学、流式细胞术、细胞和免疫遗传学检测方法的组合对其进行表征。因此,丝状噬菌体为研究抗体反应的各个方面提供了一个出色的模型系统,所有这些都是为了针对弱免疫原性肽、蛋白质和碳水化合物靶向产生抗体。

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