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重组抗体的表位特异性揭示了其混杂的肽结合特性。

Epitope-specificity of recombinant antibodies reveals promiscuous peptide-binding properties.

机构信息

Department of Immunotechnology, Lund University, Lund, Sweden.

出版信息

Protein Sci. 2012 Dec;21(12):1897-910. doi: 10.1002/pro.2173. Epub 2012 Oct 25.

DOI:10.1002/pro.2173
PMID:23034898
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3575919/
Abstract

Protein-peptide interactions are a common occurrence and essential for numerous cellular processes, and frequently explored in broad applications within biology, medicine, and proteomics. Therefore, understanding the molecular mechanism(s) of protein-peptide recognition, specificity, and binding interactions will be essential. In this study, we report the first detailed analysis of antibody-peptide interaction characteristics, by combining large-scale experimental peptide binding data with the structural analysis of eight human recombinant antibodies and numerous peptides, targeting tryptic mammalian and eukaryote proteomes. The results consistently revealed that promiscuous peptide-binding interactions, that is, both specific and degenerate binding, were exhibited by all antibodies, and the discovery was corroborated by orthogonal data, indicating that this might be a general phenomenon for low-affinity antibody-peptide interactions. The molecular mechanism for the degenerate peptide-binding specificity appeared to be executed through the use of 2-3 semi-conserved anchor residues in the C-terminal part of the peptides, in analogue to the mechanism utilized by the major histocompatibility complex-peptide complexes. In the long-term, this knowledge will be instrumental for advancing our fundamental understanding of protein-peptide interactions, as well as for designing, generating, and applying peptide specific antibodies, or peptide-binding proteins in general, in various biotechnical and medical applications.

摘要

蛋白质-肽相互作用是常见的,对于许多细胞过程都是必不可少的,并且在生物学、医学和蛋白质组学的广泛应用中经常被探索。因此,理解蛋白质-肽识别、特异性和结合相互作用的分子机制将是至关重要的。在这项研究中,我们通过将大规模的实验肽结合数据与对针对哺乳动物和真核生物蛋白酶切物的八种人源重组抗体和许多肽的结构分析相结合,首次详细分析了抗体-肽相互作用的特性。结果一致表明,所有抗体都表现出混杂的肽结合相互作用,即特异性和简并结合,正交数据也证实了这一点,这表明这可能是低亲和力抗体-肽相互作用的普遍现象。简并肽结合特异性的分子机制似乎是通过在肽的 C 末端使用 2-3 个半保守锚定残基来执行的,类似于主要组织相容性复合物-肽复合物所利用的机制。从长远来看,这一知识将有助于我们深入了解蛋白质-肽相互作用,以及设计、产生和应用肽特异性抗体,或一般的肽结合蛋白,在各种生物技术和医学应用中。

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本文引用的文献

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Quantitative proteomics targeting classes of motif-containing peptides using immunoaffinity-based mass spectrometry.基于免疫亲和的质谱法靶向含有基序肽类的定量蛋白质组学。
Mol Cell Proteomics. 2012 Aug;11(8):342-54. doi: 10.1074/mcp.M111.016238. Epub 2012 Apr 27.
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Targeting peptide termini, a novel immunoaffinity approach to reduce complexity in mass spectrometric protein identification.靶向肽末端,一种新的免疫亲和方法,可降低质谱蛋白质鉴定的复杂性。
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