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多价性——一种增强结合亲和力和生物活性的方法——对促红细胞生成素的初步应用。

Multivalency - a way to enhance binding avidities and bioactivity - preliminary applications to EPO.

作者信息

Vadas Oscar, Rose Keith

机构信息

Department of Structural Biology and Bioinformatics, University Medical Center (CMU), University of Geneva, CH-1211 Geneva 4, Switzerland.

出版信息

J Pept Sci. 2007 Sep;13(9):581-7. doi: 10.1002/psc.794.

Abstract

Multivalency has advantages over monovalency for binding interactions and even for activity. In particular, avidity is higher since the off-rate of a multivalent species is much slower than that of a monomer. This is particularly profitable for ligand-binding receptors that require dimerization for activity, such as the receptor of erythropoietin (EPOR). Peptides that mimic the action of erythropoietin (EPO) have been described with no sequence similarity with the human hormone: erythropoietin mimetic peptide (EMP) and EPO receptor peptide (ERP). These two peptides have similar activity but interact through different sites on the EPOR. Here, we describe the construction of several new synthetic homo- and hetero-dimers based on EMP-ERP sequences. To link the monomeric molecules together, several monodisperse polyamide linkers of different lengths were synthesized with dialdehyde functionalities. Chemoselective oxime chemistry was used to obtain homogeneous constructs. Certain chemical incompatibilities were dealt with via a protection approach. The oximes are stable under normal conditions and so lend themselves to biological testing.

摘要

对于结合相互作用甚至活性而言,多价性比单价性具有优势。特别是,由于多价物种的解离速率比单体慢得多,所以亲和力更高。这对于需要二聚化才能发挥活性的配体结合受体(如促红细胞生成素受体(EPOR))尤为有利。已经描述了与人类激素没有序列相似性的模拟促红细胞生成素(EPO)作用的肽:促红细胞生成素模拟肽(EMP)和EPO受体肽(ERP)。这两种肽具有相似的活性,但通过EPOR上的不同位点相互作用。在这里,我们描述了基于EMP-ERP序列构建几种新的合成同二聚体和异二聚体。为了将单体分子连接在一起,合成了几种具有不同长度的带有二醛官能团的单分散聚酰胺连接体。采用化学选择性肟化学来获得均一的构建体。通过保护方法处理了某些化学不相容性问题。肟在正常条件下是稳定的,因此适合进行生物学测试。

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