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抗体文库中对选择反应的参数和决定因素。

Parameters and determinants of responses to selection in antibody libraries.

机构信息

Center for Interdisciplinary Research in Biology (CIRB), Collège de France, CNRS UMR 7241, INSERM U1050, PSL University, Paris, France.

Département de biochimie, Faculté de Médecine, Université de Montréal, Montréal, Canada.

出版信息

PLoS Comput Biol. 2021 Mar 25;17(3):e1008751. doi: 10.1371/journal.pcbi.1008751. eCollection 2021 Mar.

Abstract

The sequences of antibodies from a given repertoire are highly diverse at few sites located on the surface of a genome-encoded larger scaffold. The scaffold is often considered to play a lesser role than highly diverse, non-genome-encoded sites in controlling binding affinity and specificity. To gauge the impact of the scaffold, we carried out quantitative phage display experiments where we compare the response to selection for binding to four different targets of three different antibody libraries based on distinct scaffolds but harboring the same diversity at randomized sites. We first show that the response to selection of an antibody library may be captured by two measurable parameters. Second, we provide evidence that one of these parameters is determined by the degree of affinity maturation of the scaffold, affinity maturation being the process by which antibodies accumulate somatic mutations to evolve towards higher affinities during the natural immune response. In all cases, we find that libraries of antibodies built around maturated scaffolds have a lower response to selection to other arbitrary targets than libraries built around germline-based scaffolds. We thus propose that germline-encoded scaffolds have a higher selective potential than maturated ones as a consequence of a selection for this potential over the long-term evolution of germline antibody genes. Our results are a first step towards quantifying the evolutionary potential of biomolecules.

摘要

在位于基因组编码较大支架表面的少数几个位置上,给定抗体库的序列高度多样化。支架通常被认为在控制结合亲和力和特异性方面的作用比高度多样化的非基因组编码位置要小。为了评估支架的影响,我们进行了定量噬菌体展示实验,我们比较了三个基于不同支架但在随机位置具有相同多样性的抗体文库对四种不同靶标的结合选择的响应。我们首先表明,抗体文库的选择响应可以用两个可测量的参数来捕获。其次,我们提供的证据表明,这些参数之一取决于支架亲和力成熟的程度,亲和力成熟是指在自然免疫反应过程中,抗体通过积累体细胞突变向更高亲和力进化的过程。在所有情况下,我们发现,围绕成熟支架构建的抗体文库对其他任意靶标的选择响应低于围绕基于种系的支架构建的文库。因此,我们提出,由于种系抗体基因的长期进化中对这种潜力的选择,种系编码的支架比成熟的支架具有更高的选择潜力。我们的结果是量化生物分子进化潜力的第一步。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3a9f/7993935/f7bcc9b9cae6/pcbi.1008751.g001.jpg

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