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应用从头设计工作流程设计靶向特异性抗体(单链抗体片段):以马来布鲁线虫的BmR1抗原为例的研究

The design of target specific antibodies (scFv) by applying de novo workflow: Case study on BmR1 antigen from Brugia malayi.

作者信息

Khor Bee Yin, Lim Theam Soon, Noordin Rahmah, Choong Yee Siew

机构信息

Institute for Research in Molecular Medicine (INFORMM), Universiti Sains Malaysia, Minden 11800, Penang, Malaysia.

Institute for Research in Molecular Medicine (INFORMM), Universiti Sains Malaysia, Minden 11800, Penang, Malaysia.

出版信息

J Mol Graph Model. 2017 Sep;76:543-550. doi: 10.1016/j.jmgm.2017.07.004. Epub 2017 Jul 19.

DOI:10.1016/j.jmgm.2017.07.004
PMID:28811153
Abstract

De novo approach was applied to design single chain fragment variable (scFv) for BmR1, a recombinant antigen from Bm17DIII gene which is the primary antigen used for the detection of anti-BmR1 IgG4 antibodies in the diagnostic of lymphatic filariasis. Three epitopes of the BmR1 was previously predicted form an ab initio derived three-dimensional structure. A collection of energetically favourable conformations was generated via hot-spot-centric approach. This resulted in a set of three different scFv scaffolds used to compute the high shape complementary conformations via dock-and-design approach with the predicted epitopes of BmR1. A total of 4227 scFv designs were generated where 200 scFv designs produced binding energies of less than -20 R.E.U with shape complementarity higher than 0.5. We further selected the design with at least one hydrogen bond and one salt bridge with the epitope, thus resulted in a total of 10, 1 and 19 sFv designs for epitope 1, 2 and 3, respectively. The results thus showed that de novo design can be an alternative approach to yield high affinity in silico scFv designs as a starting point for antibody or specific binder discovery processes.

摘要

采用从头设计方法为BmR1设计单链可变片段(scFv),BmR1是一种来自Bm17DIII基因的重组抗原,是在淋巴丝虫病诊断中用于检测抗BmR1 IgG4抗体的主要抗原。先前从从头推导的三维结构预测了BmR1的三个表位。通过以热点为中心的方法生成了一组能量有利的构象。这产生了一组三种不同的scFv支架,用于通过对接和设计方法与预测的BmR1表位计算高形状互补构象。总共生成了4227个scFv设计,其中200个scFv设计产生的结合能小于-20 R.E.U,形状互补性高于0.5。我们进一步选择了与表位至少有一个氢键和一个盐桥的设计,因此分别为表位1、2和3产生了总共10个、1个和19个scFv设计。结果表明,从头设计可以作为一种替代方法,在计算机上产生高亲和力的scFv设计,作为抗体或特异性结合物发现过程的起点。

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