体外筛选得到的高亲和力配体:复杂靶点
High affinity ligands from in vitro selection: complex targets.
作者信息
Morris K N, Jensen K B, Julin C M, Weil M, Gold L
机构信息
Department of Molecular, Cellular, and Developmental Biology, University of Colorado, Boulder, CO 80309, USA.
出版信息
Proc Natl Acad Sci U S A. 1998 Mar 17;95(6):2902-7. doi: 10.1073/pnas.95.6.2902.
Abstract
Human red blood cell membranes were used as a model system to determine if the systematic evolution of ligands by exponential enrichment (SELEX) methodology, an in vitro protocol for isolating high-affinity oligonucleotides that bind specifically to virtually any single protein, could be used with a complex mixture of potential targets. Ligands to multiple targets were generated simultaneously during the selection process, and the binding affinities of these ligands for their targets are comparable to those found in similar experiments against pure targets. A secondary selection scheme, deconvolution-SELEX, facilitates rapid isolation of the ligands to targets of special interest within the mixture. SELEX provides high-affinity compounds for multiple targets in a mixture and might allow a means for dissecting complex biological systems.
摘要
人类红细胞膜被用作一个模型系统,以确定指数富集配体系统进化(SELEX)方法(一种用于分离能特异性结合几乎任何单一蛋白质的高亲和力寡核苷酸的体外方案)是否可用于潜在靶点的复杂混合物。在筛选过程中同时产生了针对多个靶点的配体,并且这些配体对其靶点的结合亲和力与针对纯靶点的类似实验中所发现的亲和力相当。一种二级筛选方案,即去卷积SELEX,有助于快速从混合物中分离出针对特别感兴趣靶点的配体。SELEX为混合物中的多个靶点提供高亲和力化合物,并且可能提供一种剖析复杂生物系统的方法。
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