Study on peptide-peptide interaction using high-performance affinity chromatography and quartz cryst Study on peptide-peptide interaction using high-performance affinity chromatography and quartz cryst

Study on peptide-peptide interaction using high-performance affinity chromatography and quartz cryst

  • 期刊名字:科学通报(英文版)
  • 文件大小:
  • 论文作者:LUO Jia,HUANG YanYan,XIONG Sha
  • 作者单位:Beijing National Laboratory for Molecular Sciences
  • 更新时间:2023-01-17
  • 下载次数:
论文简介

The specific interaction between sense and antisense peptides was studied by high-performance affinity chromatography (HPAC) and quartz crystal microbalance (QCM) biosensor. Fragment 1-14 of human interferon-β (hlFN-β) was chosen as sense peptide and its three antisense peptides (AS-IFN 1,AS-IFN 2, and AS-IFN 3) were designed according to the degeneracy of genetic codes. The affinity column was prepared with sense peptide as ligand and the affinity chromatographic behavior was evaluated. Glu-substituted antisense peptide (AS-IFN 3) showed the strongest binding to immobilized sense peptide at pH 7.5. A quartz crystal microbalance-flow injection analysis (QCM-FIA) system was introduced to investigate the recognition process in real-time. The equilibrium dissociation constants between sense peptide and AS-IFN 1, AS-IFN 2 and AS-IFN 3 measured 2.08×10-4, 1.31×10-4 and 2.22×10-5 mol/L, respectively. The mechanism study indicated that the specific recognition between sense peptide and AS-IFN 3 was due to sequence-dependent and multi-modal affinity interaction.

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