Literature DB >> 34596853

MOrPH-PhD: A Phage Display System for the Functional Selection of Genetically Encoded Macrocyclic Peptides.

Yu Gu1, Jacob A Iannuzzelli1, Rudi Fasan2.   

Abstract

Macrocyclic peptides represent promising scaffolds for targeting biomolecules with high affinity and selectivity, making methods for the diversification and functional selection of these macrocycles highly valuable for drug discovery purposes. We recently reported a novel phage display platform (called MOrPH-PhD) for the creation and functional exploration of combinatorial libraries of genetically encoded cyclic peptides. In this system, spontaneous, posttranslational peptide cyclization by means of a cysteine-reactive non-canonical amino acid is integrated with M13 bacteriophage display, enabling the creation of genetically encoded macrocyclic peptide libraries displayed on phage particles. Using this system, it is possible to rapidly generate and screen large libraries of phage-displayed macrocyclic peptides (up to 108 to 1010 members) in order to identify high-affinity binders of a target protein of interest. Herein, we describe step-by-step protocols for the production of MOrPH-PhD libraries, the screening of these libraries against an immobilized protein target, and the isolation and characterization of functional macrocyclic peptides from these genetically encoded libraries.
© 2022. Springer Science+Business Media, LLC, part of Springer Nature.

Entities:  

Keywords:  Drug discovery; Macrocyclic peptides; Noncanonical amino acids; Phage display; Protein–protein interactions

Mesh:

Substances:

Year:  2022        PMID: 34596853      PMCID: PMC8493807          DOI: 10.1007/978-1-0716-1689-5_14

Source DB:  PubMed          Journal:  Methods Mol Biol        ISSN: 1064-3745


  55 in total

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Journal:  Nat Biotechnol       Date:  2001-01       Impact factor: 54.908

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Journal:  Biochemistry       Date:  1998-06-23       Impact factor: 3.162

Review 4.  Macrocycles are great cycles: applications, opportunities, and challenges of synthetic macrocycles in drug discovery.

Authors:  Eric Marsault; Mark L Peterson
Journal:  J Med Chem       Date:  2011-03-07       Impact factor: 7.446

5.  Synthetic peptides derived from the fourth domain of CD4 antagonize off function and inhibit T cell activation.

Authors:  T Satoh; S Li; T M Friedman; R Wiaderkiewicz; R Korngold; Z Huang
Journal:  Biochem Biophys Res Commun       Date:  1996-07-16       Impact factor: 3.575

Review 6.  Synthesis and screening of one-bead-one-compound cyclic peptide libraries.

Authors:  Ziqing Qian; Punit Upadhyaya; Dehua Pei
Journal:  Methods Mol Biol       Date:  2015

7.  Effect of signal peptide changes on the extracellular processing of streptokinase from Escherichia coli: requirement for secondary structure at the cleavage junction.

Authors:  J Pratap; K L Dikshit
Journal:  Mol Gen Genet       Date:  1998-05

8.  α1-FANGs: Protein Ligands Selective for the α-Bungarotoxin Site of the α1-Nicotinic Acetylcholine Receptor.

Authors:  Aaron L Nichols; Kaori Noridomi; Christopher R Hughes; Farzad Jalali-Yazdi; J Brek Eaton; Lan Huong Lai; Gaurav Advani; Ronald J Lukas; Henry A Lester; Lin Chen; Richard W Roberts
Journal:  ACS Chem Biol       Date:  2018-08-13       Impact factor: 5.100

9.  Bioinspired strategy for the ribosomal synthesis of thioether-bridged macrocyclic peptides in bacteria.

Authors:  Nina Bionda; Abby L Cryan; Rudi Fasan
Journal:  ACS Chem Biol       Date:  2014-08-01       Impact factor: 5.100

10.  Expanded toolbox for directing the biosynthesis of macrocyclic peptides in bacterial cells.

Authors:  Jacob A Iannuzzelli; Rudi Fasan
Journal:  Chem Sci       Date:  2020-05-27       Impact factor: 9.825

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