Synthesis of a MUC1 Mucin Cyclic Dimer Peptide and Its Antibody Binding Properties as Revealed by STD-NMR

C. Her, T. Yang
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Abstract

In a previous study we showed that the shortened MUC1 mucin peptide GVTSAPD could bind monoclonal antibody (mAb). We proceeded on to make a cyclic peptide of the same sequence to see if it would be more effective in binding antibody. We were able to synthesize and isolate two different cyclic mucin peptides: 1) a monomer cyclic peptide with sequence GVTSAPD which we did not study due to difficulties in achieving homogeneity, and 2) a dimer cyclic peptide with sequence GVTSAPDGVTSAPD that was successfully isolated and studied. We describe here the results of the dimer cyclic peptide-antibody interactions obtained by Saturation Transfer Difference NMR (STDNMR). The results indicated that the protons of all residues experienced STD effects, notably being more pronounced at Pro, Val, Ala and Asp compared to the linear peptide GVTSAPD. The Pro residue exhibited STD peaks for all its side chain protons with stronger intensity at ProHγ while Ala, Val and Thr are localized to methyl groups.
MUC1粘蛋白环二聚肽的合成及其STD-NMR抗体结合特性研究
在之前的研究中,我们发现缩短的MUC1粘蛋白肽GVTSAPD可以结合单克隆抗体(mAb)。我们继续制作相同序列的环状肽,看看它是否能更有效地结合抗体。我们合成并分离了两种不同的环粘蛋白肽:1)一个序列为GVTSAPD的单体环肽,由于难以实现均匀性,我们没有进行研究;2)一个序列为GVTSAPDGVTSAPD的二聚体环肽,我们成功分离并研究了。我们在这里描述二聚体环肽抗体相互作用的结果获得饱和转移差核磁共振(STDNMR)。结果表明,与线性肽GVTSAPD相比,所有残基的质子都经历了STD效应,特别是在Pro、Val、Ala和Asp上更为明显。Pro残基的所有侧链质子均呈现STD峰,且在ProHγ处强度较强,而Ala、Val和Thr则定位在甲基上。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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