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配体引导的靶向特异性适配体筛选:一种用于鉴定针对细胞表面蛋白的特异性适配体的筛选技术。

Ligand-Guided Selection of Target-Specific Aptamers: A Screening Technology for Identifying Specific Aptamers Against Cell-Surface Proteins.

作者信息

Zumrut Hasan E, Ara Mst Naznin, Fraile Maria, Maio George, Mallikaratchy Prabodhika

机构信息

1 Department of Chemistry, Lehman College, City University of New York , Bronx, New York.

2 Biochemistry Graduate Program, City University of New York , New York, New York.

出版信息

Nucleic Acid Ther. 2016 Jun;26(3):190-8. doi: 10.1089/nat.2016.0611. Epub 2016 May 5.

Abstract

We report on a new strategy for identifying highly specific aptamers against a predetermined epitope of a target. Termed "ligand-guided selection" (LIGS), this method uniquely exploits the selection step, the core of SELEX (Systematic Evolution Exponential enrichment). LIGS uses a naturally occurring stronger and highly specific bivalent binder, an antibody (Ab) interacting with its cognate antigen to outcompete specific aptamers from a partially enriched SELEX pool, as a strategy. We demonstrate the hypothesis of LIGS by utilizing an Ab binding to membrane-bound Immunoglobulin M (mIgM) to selectively elute aptamers that are specific for mIgM from a SELEX pool that is partially enriched toward mIgM expressing Ramos cells. The selected aptamers show specificity toward Ramos cells. We identified three aptamer candidates utilizing LIGS that could be outcompeted by mIgM Ab, demonstrating that LIGS can be successfully applied to select aptamers from a partially evolved cell-SELEX library, against predetermined receptor proteins using a cognate ligand. This proof-of-concept study introduces a new biochemical-screening platform that exploits the binding of a secondary stronger molecular entity to its target as a partition step, to identify highly specific artificial nucleic acid ligands.

摘要

我们报告了一种针对靶标预定表位鉴定高特异性适配体的新策略。这种方法被称为“配体导向筛选”(LIGS),它独特地利用了筛选步骤,即指数富集的系统进化技术(SELEX)的核心。LIGS采用一种天然存在的更强且高度特异性的二价结合剂,即一种与其同源抗原相互作用的抗体(Ab),从部分富集的SELEX文库中竞争出特异性适配体。我们通过利用一种与膜结合免疫球蛋白M(mIgM)结合的抗体,从一个针对表达mIgM的拉莫斯细胞部分富集的SELEX文库中选择性洗脱对mIgM特异的适配体,来验证LIGS的假设。所选的适配体对拉莫斯细胞显示出特异性。我们利用LIGS鉴定出了三种适配体候选物,它们可被mIgM抗体竞争取代,这表明LIGS可以成功应用于从部分进化的细胞SELEX文库中针对预定的受体蛋白利用同源配体筛选适配体。这项概念验证研究引入了一种新的生化筛选平台,该平台利用二级更强分子实体与其靶标的结合作为分离步骤,以鉴定高度特异性的人工核酸配体。

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