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通过定制氨基酸多样性来进化抗体亲和力。

Tailored amino acid diversity for the evolution of antibody affinity.

机构信息

MedImmune Ltd., Cambridge, UK.

出版信息

MAbs. 2012 Nov-Dec;4(6):664-72. doi: 10.4161/mabs.21728. Epub 2012 Aug 27.

Abstract

Antibodies are a unique class of proteins with the ability to adapt their binding sites for high affinity and high specificity to a multitude of antigens. Many analyses have been performed on antibody sequences and structures to elucidate which amino acids have a predominant role in antibody interactions with antigens. These studies have generally not distinguished between amino acids selected for broad antigen specificity in the primary immune response and those selected for high affinity in the secondary immune response. By studying a large data set of affinity matured antibodies derived from in vitro directed evolution experiments, we were able to specifically highlight a subset of amino acids associated with affinity improvements. In a comparison of affinity maturations using either tailored or full amino acid diversification, the tailored approach was found to be at least as effective at improving affinity while requiring fewer mutagenesis libraries than the traditional method. The resulting sequence data also highlight the potential for further reducing amino acid diversity for high affinity binding interactions.

摘要

抗体是一类具有独特功能的蛋白质,能够使结合部位具有高度亲和力和特异性,从而识别多种抗原。人们对抗体序列和结构进行了大量分析,以阐明哪些氨基酸在抗体与抗原的相互作用中起主要作用。这些研究通常没有区分在初级免疫反应中选择具有广泛抗原特异性的氨基酸和在次级免疫反应中选择具有高亲和力的氨基酸。通过研究大量来自体外定向进化实验的亲和力成熟抗体的数据集,我们能够专门突出与亲和力提高相关的氨基酸亚群。在使用定制或全氨基酸多样化进行亲和力成熟比较时,发现定制方法在提高亲和力方面至少同样有效,同时所需的诱变文库比传统方法少。所得的序列数据还突出了进一步降低高亲和力结合相互作用中氨基酸多样性的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0d41/3502233/781e04045892/mabs-4-664-g1.jpg

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