从噬菌体上表达的随机肽库中筛选出的生物素结合剂。
Biotin binders selected from a random peptide library expressed on phage.
作者信息
Saggio I, Laufer R
机构信息
Istituto di Ricerche di Biologia Molecolare P. Angeletti, Pomezia Roma, Italy.
出版信息
Biochem J. 1993 Aug 1;293 ( Pt 3)(Pt 3):613-6. doi: 10.1042/bj2930613.
Abstract
Recombinant biotin-binding phages were affinity-selected from a random peptide library expressed on the surface of filamentous phage. Phage binding to biotinylated proteins was half-maximally inhibited by micromolar concentrations of a monobiotinylated molecule. Sequencing of the peptide inserts of selected phages led to the identification of a previously unknown biotin-binding motif, CXWXPPF(K or R)XXC. A synthetic peptide containing this sequence motif inhibited streptavidin binding to biotinylated BSA with an IC50 of 50 microM. This compound represents the shortest non-avidin biotin-binding peptide identified to date. Our results illustrate that phage display technology can be used to identify novel ligands for a small non-proteinaceous molecule.
摘要
重组生物素结合噬菌体是从丝状噬菌体表面表达的随机肽库中通过亲和筛选获得的。噬菌体与生物素化蛋白的结合被微摩尔浓度的单生物素化分子半最大程度地抑制。对所选噬菌体的肽插入片段进行测序,从而鉴定出一个以前未知的生物素结合基序CXWXPPF(K或R)XXC。含有该序列基序的合成肽以50微摩尔的半数抑制浓度(IC50)抑制链霉亲和素与生物素化牛血清白蛋白(BSA)的结合。该化合物是迄今为止鉴定出的最短的非抗生物素蛋白生物素结合肽。我们的结果表明,噬菌体展示技术可用于鉴定一种小的非蛋白质分子的新型配体。
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