Literature DB >> 23394375

Synthetic molecular evolution of pore-forming peptides by iterative combinatorial library screening.

Aram J Krauson1, Jing He, Andrew W Wimley, Andrew R Hoffmann, William C Wimley.   

Abstract

We previously reported the de novo design of a combinatorial peptide library that was subjected to high-throughput screening to identify membrane-permeabilizing antimicrobial peptides that have β-sheet-like secondary structure. Those peptides do not form discrete pores in membranes but instead partition into membrane interfaces and cause transient permeabilization by membrane disruption, but only when present at high concentration. In this work, we used a consensus sequence from that initial screen as a template to design an iterative, second generation library. In the 24-26-residue, 16,200-member second generation library we varied six residues. Two diad repeat motifs of alternating polar and nonpolar amino acids were preserved to maintain a propensity for non-helical secondary structure. We used a new high-throughput assay to identify members that self-assemble into equilibrium pores in synthetic lipid bilayers. This screen was done at a very stringent peptide to lipid ratio of 1:1000 where most known membrane-permeabilizing peptides, including the template peptide, are not active. In a screen of 10,000 library members we identified 16 (~0.2%) that are equilibrium pore-formers at this high stringency. These rare and highly active peptides, which share a common sequence motif, are as potent as the most active pore-forming peptides known. Furthermore, they are not α-helical, which makes them unusual, as most of the highly potent pore-forming peptides are amphipathic α-helices. Here we demonstrate that this synthetic molecular evolution-based approach, taken together with the new high-throughput tools we have developed, enables the identification, refinement, and optimization of unique membrane active peptides.

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Year:  2013        PMID: 23394375      PMCID: PMC3644507          DOI: 10.1021/cb300598k

Source DB:  PubMed          Journal:  ACS Chem Biol        ISSN: 1554-8929            Impact factor:   5.100


  55 in total

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2.  Rational combinatorial design of pore-forming beta-sheet peptides.

Authors:  Joshua M Rausch; Jessica R Marks; William C Wimley
Journal:  Proc Natl Acad Sci U S A       Date:  2005-07-14       Impact factor: 11.205

Review 3.  Peptide antimicrobial agents.

Authors:  Håvard Jenssen; Pamela Hamill; Robert E W Hancock
Journal:  Clin Microbiol Rev       Date:  2006-07       Impact factor: 26.132

Review 4.  Antimicrobial and host-defense peptides as new anti-infective therapeutic strategies.

Authors:  Robert E W Hancock; Hans-Georg Sahl
Journal:  Nat Biotechnol       Date:  2006-12       Impact factor: 54.908

Review 5.  Advances in antimicrobial peptide immunobiology.

Authors:  Nannette Y Yount; Arnold S Bayer; Yan Q Xiong; Michael R Yeaman
Journal:  Biopolymers       Date:  2006       Impact factor: 2.505

Review 6.  The history of alamethicin: a review of the most extensively studied peptaibol.

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Review 7.  alpha-Hemolysin from Staphylococcus aureus: an archetype of beta-barrel, channel-forming toxins.

Authors:  E Gouaux
Journal:  J Struct Biol       Date:  1998       Impact factor: 2.867

8.  Folding of beta-sheet membrane proteins: a hydrophobic hexapeptide model.

Authors:  W C Wimley; K Hristova; A S Ladokhin; L Silvestro; P H Axelsen; S H White
Journal:  J Mol Biol       Date:  1998-04-17       Impact factor: 5.469

9.  The structure of the antimicrobial active center of lactoferricin B bound to sodium dodecyl sulfate micelles.

Authors:  D J Schibli; P M Hwang; H J Vogel
Journal:  FEBS Lett       Date:  1999-03-12       Impact factor: 4.124

10.  AMPer: a database and an automated discovery tool for antimicrobial peptides.

Authors:  Christopher D Fjell; Robert E W Hancock; Artem Cherkasov
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  17 in total

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2.  pH-Triggered, Macromolecule-Sized Poration of Lipid Bilayers by Synthetically Evolved Peptides.

Authors:  Gregory Wiedman; Sarah Y Kim; Elmer Zapata-Mercado; William C Wimley; Kalina Hristova
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3.  Host Cell Interactions Are a Significant Barrier to the Clinical Utility of Peptide Antibiotics.

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Journal:  ACS Chem Biol       Date:  2016-11-07       Impact factor: 5.100

4.  Broad-Spectrum Antiviral Entry Inhibition by Interfacially Active Peptides.

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Journal:  J Virol       Date:  2020-11-09       Impact factor: 5.103

Review 5.  Application of Synthetic Molecular Evolution to the Discovery of Antimicrobial Peptides.

Authors:  William C Wimley
Journal:  Adv Exp Med Biol       Date:  2019       Impact factor: 2.622

6.  Synthetic Molecular Evolution of Cell Penetrating Peptides.

Authors:  William C Wimley
Journal:  Methods Mol Biol       Date:  2022

Review 7.  Applications and evolution of melittin, the quintessential membrane active peptide.

Authors:  Shantanu Guha; Ryan P Ferrie; Jenisha Ghimire; Cristina R Ventura; Eric Wu; Leisheng Sun; Sarah Y Kim; Gregory R Wiedman; Kalina Hristova; Wimley C Wimley
Journal:  Biochem Pharmacol       Date:  2021-09-17       Impact factor: 6.100

8.  Synthetic molecular evolution of host cell-compatible, antimicrobial peptides effective against drug-resistant, biofilm-forming bacteria.

Authors:  Charles G Starr; Jenisha Ghimire; Shantanu Guha; Joseph P Hoffmann; Yihui Wang; Leisheng Sun; Brooke N Landreneau; Zachary D Kolansky; Isabella M Kilanowski-Doroh; Mimi C Sammarco; Lisa A Morici; William C Wimley
Journal:  Proc Natl Acad Sci U S A       Date:  2020-04-02       Impact factor: 11.205

9.  Toward the de novo design of antimicrobial peptides: Lack of correlation between peptide permeabilization of lipid vesicles and antimicrobial, cytolytic, or cytotoxic activity in living cells.

Authors:  Jing He; Aram J Krauson; William C Wimley
Journal:  Biopolymers       Date:  2014-01       Impact factor: 2.505

Review 10.  Mechanism Matters: A Taxonomy of Cell Penetrating Peptides.

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Journal:  Trends Biochem Sci       Date:  2015-11-03       Impact factor: 13.807

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