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一种与碳水化合物特异性单克隆抗体B3结合的肽的鉴定。

Identification of a peptide which binds to the carbohydrate-specific monoclonal antibody B3.

作者信息

Hoess R, Brinkmann U, Handel T, Pastan I

机构信息

DuPont-Merck Pharmaceutical Company, Wilmington, DE 19980-0328.

出版信息

Gene. 1993 Jun 15;128(1):43-9. doi: 10.1016/0378-1119(93)90151-r.

Abstract

The monoclonal antibody (mAb) B3 recognizes an antigen found on the surface of many adenocarcinoma cells. While the structure of the cellular antigen is unknown, epitope mapping using neoglycoproteins with known carbohydrate moieties indicates that the mAb B3 reacts with the LewisY (LeY) antigen [Pastan et al., Cancer Res. 51 (1991) 3781-3787]. We have used mAb B3 to select for peptides that mimic the carbohydrate structure using libraries of filamentous phage displaying random peptides on their surface. Phage that were selected coded for the sequence APWLYGPA. The corresponding peptide was synthesized and tested for its ability to bind to mAb B3. The peptide was found to inhibit specifically the binding of 111In-labeled mAb B3 to A431 adenocarcinoma cells, as well as to inhibit killing of these cells by a B3 immunotoxin. In addition, the LeY carbohydrate, lactodifucotetraose, was able to compete with the phage displaying this peptide for binding to mAb B3. Alanine-scanning mutagenesis of the sequence coding for this peptide indicates that four residues, PWLY, were critical for binding to the mAb. The sequence is similar to other sequences known to mimic carbohydrate structures.

摘要

单克隆抗体(mAb)B3可识别许多腺癌细胞表面存在的一种抗原。虽然细胞抗原的结构尚不清楚,但使用具有已知碳水化合物部分的新糖蛋白进行表位作图表明,mAb B3与LewisY(LeY)抗原发生反应[帕斯坦等人,《癌症研究》51(1991)3781 - 3787]。我们利用mAb B3从丝状噬菌体文库中筛选能够模拟碳水化合物结构的肽段,这些丝状噬菌体在其表面展示随机肽段。筛选出的噬菌体编码序列为APWLYGPA。合成了相应的肽段,并测试其与mAb B3结合的能力。发现该肽段能特异性抑制111In标记的mAb B3与A431腺癌细胞的结合,还能抑制B3免疫毒素对这些细胞的杀伤作用。此外,LeY碳水化合物——乳糖二岩藻四糖,能够与展示该肽段的噬菌体竞争结合mAb B3。对编码该肽段的序列进行丙氨酸扫描诱变表明,四个残基PWLY对于与mAb的结合至关重要。该序列与其他已知的模拟碳水化合物结构的序列相似。

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