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使用与乳糖阻遏物C末端相连的肽的大型文库筛选受体配体。

Screening for receptor ligands using large libraries of peptides linked to the C terminus of the lac repressor.

作者信息

Cull M G, Miller J F, Schatz P J

机构信息

Affymax Research Institute, Palo Alto, CA 94304.

出版信息

Proc Natl Acad Sci U S A. 1992 Mar 1;89(5):1865-9. doi: 10.1073/pnas.89.5.1865.

Abstract

We have constructed a large library of random peptides fused to the C terminus of the lac repressor. The DNA binding activity of the repressor protein physically links the peptides to the plasmid encoding them by binding to lac operator sequences on the plasmid. This linkage allows efficient enrichment for specific peptide ligands in the random population of peptides by affinity purification of the peptide-repressor-plasmid complexes with an immobilized receptor. After transformation of Escherichia coli with recovered plasmids, the library can be amplified for additional rounds of affinity enrichment or specific plasmids can be sequenced to determine the primary structure of the peptides. We used a monoclonal antibody specific for the peptide dynorphin B as a model receptor to screen a random dodecamer library. After only two rounds of enrichment, the majority of the plasmids in the selected population encoded fusion peptides that bound specifically to the antibody. These peptides contain a consensus sequence similar to a segment of dynorphin B (RQFKVV). This technique should be useful to find peptide ligands for a variety of biological receptors.

摘要

我们构建了一个与乳糖阻遏物C末端融合的随机肽大型文库。阻遏蛋白的DNA结合活性通过与质粒上的乳糖操纵序列结合,将肽物理连接到编码它们的质粒上。这种连接通过用固定化受体对肽 - 阻遏物 - 质粒复合物进行亲和纯化,能够在随机肽群体中高效富集特定的肽配体。用回收的质粒转化大肠杆菌后,文库可进行扩增以进行更多轮的亲和富集,或者可以对特定质粒进行测序以确定肽的一级结构。我们使用对肽强啡肽B特异的单克隆抗体作为模型受体来筛选随机十二聚体文库。仅经过两轮富集后,所选群体中的大多数质粒编码的融合肽能与抗体特异性结合。这些肽含有与强啡肽B的一段序列(RQFKVV)相似的共有序列。该技术对于寻找多种生物受体的肽配体应该是有用的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/26ca/48554/ab5d50c79255/pnas01079-0359-a.jpg

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