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一种新型的、更小的 Affitins 支架:与 EpCAM 特异性结合的配体展示。

A novel, smaller scaffold for Affitins: Showcase with binders specific for EpCAM.

机构信息

CRCINA, Inserm, CNRS, Université d'Angers, Université de Nantes, Nantes, France.

Université Catholique de Louvain, Louvain Drug Research Institute, Advanced Drug Delivery and Biomaterials, Brussels, Belgium.

出版信息

Biotechnol Bioeng. 2018 Feb;115(2):290-299. doi: 10.1002/bit.26463. Epub 2017 Nov 6.

DOI:10.1002/bit.26463
PMID:28976545
Abstract

Affitins are highly stable engineered affinity proteins, originally derived from Sac7d and Sso7d, two 7 kDa DNA-binding polypeptides from Sulfolobus genera. Their efficiency as reagents for intracellular targeting, enzyme inhibition, affinity purification, immunolocalization, and various other applications has been demonstrated. Recently, we have characterized the 7 kDa DNA-binding family, and Aho7c originating from Acidianus hospitalis was shown to be its smallest member with thermostability comparable to those of Sac7d and Sso7d. Here, after four rounds of selection by ribosome display against the human recombinant Epithelial Cell Adhesion Molecule (hrEpCAM), we obtained novel Aho7c-based Affitins. The binders were expressed in soluble form in Escherichia coli, displayed high stability (up to 74°C; pH 0-12) and were shown to be specific for the hrEpCAM extracellular domain with picomolar affinities (K  = 110 pM). Thus, we propose Aho7c as a good candidate for the creation of Affitins with a 10% smaller size than the Sac7d-based ones (60 vs. 66 amino acids).

摘要

亲和素是高度稳定的工程化亲和蛋白,最初来源于 Sac7d 和 Sso7d,这两种蛋白分别来自 Sulfolobus 属的两个 7 kDa DNA 结合多肽。它们作为细胞内靶向、酶抑制、亲和纯化、免疫定位和各种其他应用的试剂的效率已经得到了证明。最近,我们对 7 kDa DNA 结合家族进行了表征,发现源自 Acidianus hospitalis 的 Aho7c 是其最小的成员,其热稳定性可与 Sac7d 和 Sso7d 相媲美。在这里,我们通过核糖体展示技术对人重组上皮细胞黏附分子(hrEpCAM)进行了四轮筛选,得到了基于 Aho7c 的新型亲和素。这些结合物以可溶形式在大肠杆菌中表达,具有很高的稳定性(高达 74°C;pH0-12),并显示出对 hrEpCAM 细胞外结构域的特异性,亲和力为皮摩尔级(Kd=110 pM)。因此,我们提出 Aho7c 是一种很好的候选蛋白,可以用来构建比基于 Sac7d 的亲和素小 10%的亲和素(60 对 66 个氨基酸)。

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