Rational Designed Hybrid Peptides Show up to a 6-Fold Increase in Antimicrobial Activity and Demonstrate Different Ultrastructural Changes as the Parental Peptides Measured by BioSAXS

Antimicrobial peptides (AMPs) are a promising class of compounds being developed against multi-drug resistant bacteria. Hybridization has been reported to increase antimicrobial activity. Here, two proline-rich peptides (consP1: VRKPPYLPRPRPRPL-CONH(2) and Bac5-v291: RWRRPIRRRPIRPPFWR-CONH(2)) were...

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Autores principales: Hilpert, Kai, Gani, Jurnorain, Rumancev, Christoph, Simpson, Nathan, Lopez-Perez, Paula Matilde, Garamus, Vasil M., von Gundlach, Andreas Robert, Markov, Petar, Scocchi, Marco, Mikut, Ralf, Rosenhahn, Axel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8711299/
https://www.ncbi.nlm.nih.gov/pubmed/34966279
http://dx.doi.org/10.3389/fphar.2021.769739
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author Hilpert, Kai
Gani, Jurnorain
Rumancev, Christoph
Simpson, Nathan
Lopez-Perez, Paula Matilde
Garamus, Vasil M.
von Gundlach, Andreas Robert
Markov, Petar
Scocchi, Marco
Mikut, Ralf
Rosenhahn, Axel
author_facet Hilpert, Kai
Gani, Jurnorain
Rumancev, Christoph
Simpson, Nathan
Lopez-Perez, Paula Matilde
Garamus, Vasil M.
von Gundlach, Andreas Robert
Markov, Petar
Scocchi, Marco
Mikut, Ralf
Rosenhahn, Axel
author_sort Hilpert, Kai
collection PubMed
description Antimicrobial peptides (AMPs) are a promising class of compounds being developed against multi-drug resistant bacteria. Hybridization has been reported to increase antimicrobial activity. Here, two proline-rich peptides (consP1: VRKPPYLPRPRPRPL-CONH(2) and Bac5-v291: RWRRPIRRRPIRPPFWR-CONH(2)) were combined with two arginine-isoleucine-rich peptides (optP1: KIILRIRWR-CONH(2) and optP7: KRRVRWIIW-CONH(2)). Proline-rich antimicrobial peptides (PrAMPs) are known to inhibit the bacterial ribosome, shown also for Bac5-v291, whereas it is hypothesized a “dirty drug” model for the arginine-isoleucine-rich peptides. That hypothesis was underpinned by transmission electron microscopy and biological small-angle X-ray scattering (BioSAXS). The strength of BioSAXS is the power to detect ultrastructural changes in millions of cells in a short time (seconds) in a high-throughput manner. This information can be used to classify antimicrobial compounds into groups according to the ultrastructural changes they inflict on bacteria and how the bacteria react towards that assault. Based on previous studies, this correlates very well with different modes of action. Due to the novelty of this approach direct identification of the target of the antimicrobial compound is not yet fully established, more research is needed. More research is needed to address this limitation. The hybrid peptides showed a stronger antimicrobial activity compared to the proline-rich peptides, except when compared to Bac5-v291 against E. coli. The increase in activity compared to the arginine-isoleucine-rich peptides was up to 6-fold, however, it was not a general increase but was dependent on the combination of peptides and bacteria. BioSAXS experiments revealed that proline-rich peptides and arginine-isoleucine-rich peptides induce very different ultrastructural changes in E. coli, whereas a hybrid peptide (hyP7B5GK) shows changes, different to both parental peptides and the untreated control. These different ultrastructural changes indicated that the mode of action of the parental peptides might be different from each other as well as from the hybrid peptide hyP7B5GK. All peptides showed very low haemolytic activity, some of them showed a 100-fold or larger therapeutic window, demonstrating the potential for further drug development.
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spelling pubmed-87112992021-12-28 Rational Designed Hybrid Peptides Show up to a 6-Fold Increase in Antimicrobial Activity and Demonstrate Different Ultrastructural Changes as the Parental Peptides Measured by BioSAXS Hilpert, Kai Gani, Jurnorain Rumancev, Christoph Simpson, Nathan Lopez-Perez, Paula Matilde Garamus, Vasil M. von Gundlach, Andreas Robert Markov, Petar Scocchi, Marco Mikut, Ralf Rosenhahn, Axel Front Pharmacol Pharmacology Antimicrobial peptides (AMPs) are a promising class of compounds being developed against multi-drug resistant bacteria. Hybridization has been reported to increase antimicrobial activity. Here, two proline-rich peptides (consP1: VRKPPYLPRPRPRPL-CONH(2) and Bac5-v291: RWRRPIRRRPIRPPFWR-CONH(2)) were combined with two arginine-isoleucine-rich peptides (optP1: KIILRIRWR-CONH(2) and optP7: KRRVRWIIW-CONH(2)). Proline-rich antimicrobial peptides (PrAMPs) are known to inhibit the bacterial ribosome, shown also for Bac5-v291, whereas it is hypothesized a “dirty drug” model for the arginine-isoleucine-rich peptides. That hypothesis was underpinned by transmission electron microscopy and biological small-angle X-ray scattering (BioSAXS). The strength of BioSAXS is the power to detect ultrastructural changes in millions of cells in a short time (seconds) in a high-throughput manner. This information can be used to classify antimicrobial compounds into groups according to the ultrastructural changes they inflict on bacteria and how the bacteria react towards that assault. Based on previous studies, this correlates very well with different modes of action. Due to the novelty of this approach direct identification of the target of the antimicrobial compound is not yet fully established, more research is needed. More research is needed to address this limitation. The hybrid peptides showed a stronger antimicrobial activity compared to the proline-rich peptides, except when compared to Bac5-v291 against E. coli. The increase in activity compared to the arginine-isoleucine-rich peptides was up to 6-fold, however, it was not a general increase but was dependent on the combination of peptides and bacteria. BioSAXS experiments revealed that proline-rich peptides and arginine-isoleucine-rich peptides induce very different ultrastructural changes in E. coli, whereas a hybrid peptide (hyP7B5GK) shows changes, different to both parental peptides and the untreated control. These different ultrastructural changes indicated that the mode of action of the parental peptides might be different from each other as well as from the hybrid peptide hyP7B5GK. All peptides showed very low haemolytic activity, some of them showed a 100-fold or larger therapeutic window, demonstrating the potential for further drug development. Frontiers Media S.A. 2021-12-03 /pmc/articles/PMC8711299/ /pubmed/34966279 http://dx.doi.org/10.3389/fphar.2021.769739 Text en Copyright © 2021 Hilpert, Gani, Rumancev, Simpson, Lopez-Perez, Garamus, von Gundlach, Markov, Scocchi, Mikut and Rosenhahn. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Hilpert, Kai
Gani, Jurnorain
Rumancev, Christoph
Simpson, Nathan
Lopez-Perez, Paula Matilde
Garamus, Vasil M.
von Gundlach, Andreas Robert
Markov, Petar
Scocchi, Marco
Mikut, Ralf
Rosenhahn, Axel
Rational Designed Hybrid Peptides Show up to a 6-Fold Increase in Antimicrobial Activity and Demonstrate Different Ultrastructural Changes as the Parental Peptides Measured by BioSAXS
title Rational Designed Hybrid Peptides Show up to a 6-Fold Increase in Antimicrobial Activity and Demonstrate Different Ultrastructural Changes as the Parental Peptides Measured by BioSAXS
title_full Rational Designed Hybrid Peptides Show up to a 6-Fold Increase in Antimicrobial Activity and Demonstrate Different Ultrastructural Changes as the Parental Peptides Measured by BioSAXS
title_fullStr Rational Designed Hybrid Peptides Show up to a 6-Fold Increase in Antimicrobial Activity and Demonstrate Different Ultrastructural Changes as the Parental Peptides Measured by BioSAXS
title_full_unstemmed Rational Designed Hybrid Peptides Show up to a 6-Fold Increase in Antimicrobial Activity and Demonstrate Different Ultrastructural Changes as the Parental Peptides Measured by BioSAXS
title_short Rational Designed Hybrid Peptides Show up to a 6-Fold Increase in Antimicrobial Activity and Demonstrate Different Ultrastructural Changes as the Parental Peptides Measured by BioSAXS
title_sort rational designed hybrid peptides show up to a 6-fold increase in antimicrobial activity and demonstrate different ultrastructural changes as the parental peptides measured by biosaxs
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8711299/
https://www.ncbi.nlm.nih.gov/pubmed/34966279
http://dx.doi.org/10.3389/fphar.2021.769739
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