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人黏蛋白(MUC-1)蛋白核心的单串联、双串联和三串联重复序列的生物物理特性分析

Biophysical characterization of one-, two-, and three-tandem repeats of human mucin (muc-1) protein core.

作者信息

Fontenot J D, Tjandra N, Bu D, Ho C, Montelaro R C, Finn O J

机构信息

Department of Molecular Genetics and Biochemistry, University of Pittsburgh School of Medicine 15261.

出版信息

Cancer Res. 1993 Nov 15;53(22):5386-94.

PMID:8221676
Abstract

Until recently mucin tandem repeat protein cores were believed to exist in random-coil conformations and to attain structure solely by the addition of carbohydrates to serine and threonine residues. Matsushima et al. (Proteins Struct. Funct. Genet., 7: 125-155, 1990) recently proposed a model of the secondary structure of proline rich tandem repeat proteins that has challenged this idea, especially for the case of the human polymorphic epithelial mucin encoded by the muc-1 gene. We report here results of structural analyses of the muc-1 protein core by using synthetic peptide analogues. Synthetic peptides were prepared to correspond to one-, two-, and three-tandem repeats of muc-1. Results of one- and two-dimensional 1H NMR correlation spectroscopy on these peptides confirm that the muc-1 protein core is not a random-coil secondary structure. Long-lived amide protons are protected in D2O, and increasing spectral complexity in the region of the beta-protons of Asp2 and His 15 reveals that structural changes are occurring as the number of repeats increases. The greatest changes occur when the number of repeats increases from one to two. These results are supported by the reactivity of a panel of monoclonal antibodies raised against tumor associated muc-1 with these synthetic peptides in enzyme-linked immunosorbent assay. The primary immunodominant mucin epitope, PDTRP, does not appear to attain a native conformation in the single repeat peptide (20 amino acids, starting with P), but is expressed on peptides with multiple repeats. Intrinsic viscosity measurements of the peptide containing three repeats indicate that an ordered structure present in solution is rod shaped. The circular dichroism spectrum of the same peptide is dominated by proline in the trans conformation. These results are all consistent with the prediction that the muc-1 tandem repeat polypeptide core forms a polyproline beta-turn helix.

摘要

直到最近,人们还认为粘蛋白串联重复蛋白核心以无规卷曲构象存在,并且仅通过向丝氨酸和苏氨酸残基添加碳水化合物来获得结构。松岛等人(《蛋白质结构、功能与遗传学》,7: 125 - 155,1990)最近提出了富含脯氨酸串联重复蛋白二级结构的模型,这一模型对上述观点提出了挑战,特别是对于由muc - 1基因编码的人多态性上皮粘蛋白的情况。我们在此报告使用合成肽类似物对muc - 1蛋白核心进行结构分析的结果。制备了与muc - 1的一、二和三个串联重复相对应的合成肽。对这些肽进行的一维和二维1H NMR相关光谱分析结果证实,muc - 1蛋白核心不是无规卷曲二级结构。在D2O中长寿命酰胺质子受到保护,并且随着重复次数增加,Asp2和His 15的β - 质子区域光谱复杂性增加,这表明结构发生了变化。当重复次数从一增加到二时,变化最为显著。这些结果得到了一组针对肿瘤相关muc - 1产生的单克隆抗体在酶联免疫吸附测定中与这些合成肽反应性的支持。主要的免疫显性粘蛋白表位PDTRP在单重复肽(20个氨基酸,以P开头)中似乎未达到天然构象,但在具有多个重复的肽上表达。含有三个重复的肽的特性粘度测量表明,溶液中存在的有序结构呈棒状。同一肽的圆二色光谱以反式构象的脯氨酸为主。这些结果都与muc - 1串联重复多肽核心形成聚脯氨酸β - 转角螺旋的预测一致。

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