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超稳定合成微型蛋白作为有效的配体支架

Hyperstable Synthetic Mini-Proteins as Effective Ligand Scaffolds.

作者信息

Blanchard Paul L, Knick Brandon J, Whelan Sarah A, Hackel Benjamin J

机构信息

Department of Chemical Engineering and Materials Science, University of Minnesota─Twin Cities, 421 Washington Avenue SE, Minneapolis, Minnesota 55455, United States.

出版信息

ACS Synth Biol. 2023 Dec 15;12(12):3608-3622. doi: 10.1021/acssynbio.3c00409. Epub 2023 Nov 27.

Abstract

Small, single-domain protein scaffolds are compelling sources of molecular binding ligands with the potential for efficient physiological transport, modularity, and manufacturing. Yet, mini-proteins require a balance between biophysical robustness and diversity to enable new functions. We tested the developability and evolvability of millions of variants of 43 designed libraries of synthetic 40-amino acid βαββ proteins with diversified sheet, loop, or helix paratopes. We discovered a scaffold library that yielded hundreds of binders to seven targets while exhibiting high stability and soluble expression. Binder discovery yielded 6-122 nM affinities without affinity maturation and s averaging ≥78 °C. Broader βαββ libraries exhibited varied developability and evolvability. Sheet paratopes were the most consistently developable, and framework 1 was the most evolvable. Paratope evolvability was dependent on target, though several libraries were evolvable across many targets while exhibiting high stability and soluble expression. Select βαββ proteins are strong starting points for engineering performant binders.

摘要

小型单结构域蛋白质支架是分子结合配体的重要来源,具有高效生理转运、模块化和可制造性的潜力。然而,微型蛋白质需要在生物物理稳健性和多样性之间取得平衡,以实现新功能。我们测试了43个设计库中数百万个合成40氨基酸βαββ蛋白质变体的可开发性和可进化性,这些变体具有多样化的β折叠、环或螺旋互补决定区。我们发现了一个支架库,它能产生数百种针对七个靶标的结合物,同时表现出高稳定性和可溶性表达。在没有亲和力成熟的情况下,结合物发现产生了6 - 122 nM的亲和力,且热稳定性平均≥78°C。更广泛的βαββ库表现出不同的可开发性和可进化性。β折叠互补决定区是最具一致性可开发性的,而框架1是最具可进化性的。互补决定区的可进化性取决于靶标,不过有几个库在许多靶标上都具有可进化性,同时表现出高稳定性和可溶性表达。选定的βαββ蛋白质是工程化高性能结合物的有力起点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/db36/10822706/c9c6bb5728e6/nihms-1960700-f0002.jpg

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