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Purification of polyclonal anti-conformational antibodies for use in affinity selection from random peptide phage display libraries: A study using the hydatid vaccine EG95

机译:用于从随机肽噬菌体展示库进行亲和力选择的多克隆抗构象抗体的纯化:使用the虫疫苗EG95的研究

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摘要

The use of polyclonal antibodies to screen random peptide phage display libraries often results in the recognition of a large number of peptides that mimic linear epitopes on various proteins. There appears to be a bias in the use of this technology toward the selection of peptides that mimic linear epitopes. In many circumstances the correct folding of a protein immunogen is required for conferring protection. The use of random peptide phage display libraries to identify peptide mimics of conformational epitopes in these cases requires a strategy for overcoming this bias. Conformational epitopes on the hydatid vaccine EG95 have been shown to result in protective immunity in sheep, whereas linear epitopes are not protective. In this paper we describe a strategy that results in the purification of polyclonal antibodies directed against conformational epitopes while eliminating antibodies directed against linear epitopes. These affinity purified antibodies were then used to select a peptide from a random peptide phage display library that has the capacity to mimic conformational epitopes on EG95. This peptide was subsequently used to affinity purify monospecific antibodies against EG95.
机译:使用多克隆抗体筛选随机的肽噬菌体展示文库通常会导致识别出模仿各种蛋白质线性表位的大量肽。在使用该技术时,似乎倾向于选择模拟线性表位的肽。在许多情况下,需要赋予蛋白质免疫原正确的折叠才能提供保护。在这些情况下,使用随机肽噬菌体展示文库鉴定构象表位的肽模拟物需要一种克服这一偏见的策略。已证明,包虫疫苗EG95上的构象表位可在绵羊中产生保护性免疫,而线性表位则无保护性。在本文中,我们描述了一种策略,该策略可纯化针对构象表位的多克隆抗体,同时消除针对线性表位的抗体。然后将这些亲和纯化的抗体用于从随机肽噬菌体展示文库中选择具有模拟EG95构象表位能力的肽。该肽随后用于亲和纯化针对EG95的单特异性抗体。

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