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The identification of affinity peptide ligands specific to the variable region of human antibodies

机译:对人抗体可变区特异的亲和肽配体的鉴定

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Of all potential biological therapeutics, monoclonal antibody (mAb)-based therapies are becoming the dominant focus of clinical research. In particular, smaller recombinant antibody fragments such as single-chain variable fragments (scFv) have become the subject of intense focus. However, an efficient affinity ligand for antibody fragment purification has not been developed. In the present study, we designed a consensus sequence for the human antibody heavy or light chain-variable regions (Fv) based on the antibody sequences available in the ImMunoGeneTics information system (IMGT), and synthesized these consensus sequences as template Fv antibodies. We then screened peptide ligands that specifically bind to the repertoire-derived human Fv consensus antibody using a 12-mer-peptide library expressed-phage display method. Subsequently, 1 peptide for the VH template and 8 peptides for the VK template were selected as the candidate ligands after 4 rounds of panning the phage display. Using peptide-bead-based immunoprecipitation, the code-4 and code-13 peptides showed recovery rates of the VH and VK templates that were 20–30% and 40–50%, respectively. Both peptides exhibited better recovery rates for trastuzumab scFv (approximately 40%). If it were possible to identify the best combination of VH and VK-binding peptides among the ligand peptides suitable for the human mAb Fv sequence, the result could be a promising purification tool that might greatly improve the cost efficiencies of the purification process.
机译:在所有潜在的生物疗法中,基于单克隆抗体(mAb)的疗法正成为临床研究的重点。特别地,较小的重组抗体片段,例如单链可变片段(scFv),已经成为人们关注的焦点。然而,尚未开发出用于抗体片段纯化的有效亲和配体。在本研究中,我们基于ImMunoGeneTics信息系统(IMGT)中可用的抗体序列设计了人类抗体重链或轻链可变区(Fv)的共有序列,并将这些共有序列合成为模板Fv抗体。然后,我们使用12-mer-Peptide肽库表达的噬菌体展示方法筛选了特异性结合到库中衍生的人Fv共有抗体的肽配体。随后,在淘选噬菌体展示4轮之后,选择用于VH模板的1个肽和用于VK模板的8个肽作为候选配体。使用基于肽珠的免疫沉淀,代码4和代码13肽显示VH和VK模板的回收率分别为20–30%和40–50%。两种肽都显示出曲妥珠单抗scFv的回收率更高(约40%)。如果有可能在适用于人mAb Fv序列的配体肽中鉴定出VH和VK结合肽的最佳组合,则结果可能是一种很有前途的纯化工具,可大大提高纯化过程的成本效率。

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