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一种针对鸟嘌呤-胞嘧啶(G.C)特异性的DNA小沟结合肽的设计。

Design of a G.C-specific DNA minor groove-binding peptide.

作者信息

Geierstanger B H, Mrksich M, Dervan P B, Wemmer D E

机构信息

Graduate Group in Biophysics, University of California, Berkeley 94720.

出版信息

Science. 1994 Oct 28;266(5185):646-50. doi: 10.1126/science.7939719.

Abstract

A four-ring tripeptide containing alternating imidazole and pyrrole carboxamides specifically binds six-base pair 5'-(A,T)GCGC(A,T)-3' sites in the minor groove of DNA. The designed peptide has a specificity completely reversed from that of the tripyrrole distamycin, which binds A,T sequences. Structural studies with nuclear magnetic resonance revealed that two peptides bound side-by-side and in an antiparallel orientation in the minor groove. Each of the four imidazoles in the 2:1 ligand-DNA complex recognized a specific guanine amino group in the GCGC core through a hydrogen bond. Targeting a designated four-base pair G.C tract by this synthetic ligand supports the generality of the 2:1 peptide-DNA motif for sequence-specific minor groove recognition of DNA.

摘要

一种含有交替咪唑和吡咯羧酰胺的四环三肽特异性结合DNA小沟中六碱基对5'-(A,T)GCGC(A,T)-3'位点。设计的肽具有与结合A、T序列的三吡咯放线菌素完全相反的特异性。核磁共振结构研究表明,两个肽在小沟中并排且以反平行方向结合。在2:1配体-DNA复合物中,四个咪唑中的每一个都通过氢键识别GCGC核心中的特定鸟嘌呤氨基。通过这种合成配体靶向指定的四碱基对G.C片段,支持了2:1肽-DNA基序对DNA序列特异性小沟识别的普遍性。

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