Binding Epitope of Somatostatin Defined by Phage-Displayed Peptide Libraries

We have developed a versatile phagemid system to display peptides on the surface of M13 bacteriophage at a copy number which approaches monovalency. In this system, a phagemid encodes a peptide fused to the ammo-terminus of the second domain (dII) of the minor coat protein pIII under control of the...

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Bibliographic Details
Published in:Bio/Technology 1995-02, Vol.13 (2), p.165-169
Main Authors: Wright, Richard M, Gram, Hermann, Vattay, Anthony, Byrne, Susan, Lake, Phil, Dottavio, Diane
Format: Article
Language:English
Subjects:
Agriculture
Amino Acid Sequence
Antibodies, Monoclonal
Bacteriophages - genetics
Bioinformatics
Biological and medical sciences
Biomedical and Life Sciences
Biomedical Engineering/Biotechnology
Biomedicine
Biotechnology
Capsid Proteins
DNA-Binding Proteins - chemistry
DNA-Binding Proteins - genetics
Epitopes - genetics
Epitopes - metabolism
Escherichia coli - genetics
Fundamental and applied biological sciences. Psychology
Genetic engineering
Genetic technics
Genetic Vectors
Lac Operon
Life Sciences
Methods. Procedures. Technologies
Mutagenesis
Peptide Library
Receptors, Somatostatin - metabolism
Recombinant Fusion Proteins
Somatostatin - chemistry
Somatostatin - genetics
Somatostatin - immunology
Vectors (cloning, transfer, expression). Insertion sequences and transposons
Viral Fusion Proteins - chemistry
Viral Fusion Proteins - genetics
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Description
Summary:We have developed a versatile phagemid system to display peptides on the surface of M13 bacteriophage at a copy number which approaches monovalency. In this system, a phagemid encodes a peptide fused to the ammo-terminus of the second domain (dII) of the minor coat protein pIII under control of the inducible lac promoter. The fusion protein is displayed in combination with several copies of wild-type pIII on the surface of phage. Two diverse random octapeptide libraries, one linear and one which contained flanking cysteines capable of forming disulflde bridges, were were generated using an in vitro mutagenesis approach and affinity selected on an anti-somatostatin mAb. Peptides with high affinity for the mAb were enriched only from the cyclic library and the tetrapeptide, FWKT, was identified by consensus as the binding epitope. The selected peptides exhibited not only the primary amino acid sequence but also shared structural features with somatostatin. One peptide, CRFWKTWC, also exhibited nanomolar affinities for the five known somatostatin receptor subtypes. This system can easily be adapted to display individual peptides or a wide range of custom peptide libraries.
ISSN:0733-222X
1087-0156
2331-3684
1546-1696
DOI:10.1038/nbt0295-165