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人Lyn酪氨酸激酶SH3结构域高特异性FN3单域抗体的定向进化

Directed Evolution of a Highly Specific FN3 Monobody to the SH3 Domain of Human Lyn Tyrosine Kinase.

作者信息

Huang Renhua, Fang Pete, Hao Zengping, Kay Brian K

机构信息

Department of Biological Sciences, University of Illinois at Chicago, Chicago, Illinois, United States of America.

出版信息

PLoS One. 2016 Jan 5;11(1):e0145872. doi: 10.1371/journal.pone.0145872. eCollection 2016.

Abstract

Affinity reagents of high affinity and specificity are very useful for studying the subcellular locations and quantities of individual proteins. To generate high-quality affinity reagents for human Lyn tyrosine kinase, a phage display library of fibronectin type III (FN3) monobodies was affinity selected with a recombinant form of the Lyn SH3 domain. While a highly specific monobody, TA8, was initially isolated, we chose to improve its affinity through directed evolution. A secondary library of 1.2 × 109 variants was constructed and screened by affinity selection, yielding three variants, two of which have affinities of ~ 40 nM, a 130-fold increase over the original TA8 monobody. One of the variants, 2H7, displayed high specificity to the Lyn SH3 domain, as shown by ELISA and probing arrays of 150 SH3 domains. Furthermore, the 2H7 monobody was able to pull down endogenous Lyn from a lysate of Burkitt's lymphoma cells, thereby demonstrating its utility as an affinity reagent for detecting Lyn in a complex biological mixture.

摘要

具有高亲和力和特异性的亲和试剂对于研究单个蛋白质的亚细胞定位和数量非常有用。为了生成用于人Lyn酪氨酸激酶的高质量亲和试剂,用重组形式的Lyn SH3结构域对纤连蛋白III型(FN3)单域抗体的噬菌体展示文库进行亲和筛选。虽然最初分离出了一种高度特异性的单域抗体TA8,但我们选择通过定向进化来提高其亲和力。构建了一个包含1.2×10⁹个变体的二级文库,并通过亲和筛选进行筛选,得到了三个变体,其中两个变体的亲和力约为40 nM,比原始的TA8单域抗体增加了130倍。其中一个变体2H7对Lyn SH3结构域表现出高特异性,如ELISA和150个SH3结构域的探针阵列所示。此外,2H7单域抗体能够从伯基特淋巴瘤细胞裂解物中拉下内源性Lyn,从而证明了其作为在复杂生物混合物中检测Lyn的亲和试剂的实用性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b97c/4701441/6d4c34f8be7f/pone.0145872.g001.jpg

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