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Screening and Identification of a Targeting Peptide to nGLP-1R from Phage Display Peptide Library

Screening and Identification of a Targeting Peptide to nGLP-1R from Phage Display Peptide Library
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摘要 In order to provide the structure information for designing new exendin-4 analogues, a phage display peptide library was screened by targeting the N-terminal extracellular domain of GLP-1R(nGLP-1R). After four rounds of selection, nine sequences were obtained, four of them have higher affinity for nGLP-1R than the others. We chose two of them named X and Y peptides. Islet β-cell proliferation assay suggested that X and Y peptides didn't have any activity to increase islet β-cell proliferation. In other words, X and Y peptides were not agonists to GLP-1R. However, the conservative motifs of X and Y peptides provided us useful information to design new exendin-4 analogues. In order to provide the structure information for designing new exendin-4 analogues, a phage display peptide library was screened by targeting the N-terminal extracellular domain of GLP-1R(nGLP-1R). After four rounds of selection, nine sequences were obtained, four of them have higher affinity for nGLP-1R than the others. We chose two of them named X and Y peptides. Islet β-cell proliferation assay suggested that X and Y peptides didn't have any activity to increase islet β-cell proliferation. In other words, X and Y peptides were not agonists to GLP-1R. However, the conservative motifs of X and Y peptides provided us useful information to design new exendin-4 analogues.
出处 《Chemical Research in Chinese Universities》 SCIE CAS CSCD 2010年第4期604-607,共4页 高等学校化学研究(英文版)
关键词 GLP-1 receptor Phage display peptide library EXENDIN-4 GLP-1 receptor Phage display peptide library Exendin-4
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