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The Antimicrobial Peptide Pipeline: A Bacteria-Centric AMP Predictor
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Introduction:
Antimicrobial peptides (AMPs), unlike antibiotics, are encoded in genomes.
AMPs are exported from the cell after expression and translation. In the case of bacteria, the
exported peptides target other microbes to give the producing bacterium a competitive edge. While
AMPs are sought after for their similar antimicrobial activity to traditional antibiotics, it is difficult
to predict which combinations of amino acids will confer antimicrobial activity. Many computer algorithms
have been designed to predict whether a sequence of amino acids will exhibit antimicrobial
activity, but the vast majority of validated AMPs in databases are still of eukaryotic origin. This
defies common sense since the vast majority of life on Earth is prokaryotic.
Methods:
The antimicrobial peptide pipeline, presented here, is a bacteria-centric AMP predictor
that predicts AMPs by taking design inspiration from the sequence properties of bacterial genomes
with the intention to improve the detection of naturally occurring bacterial AMPs. The pipeline integrates
multiple concepts of comparative biology to search for candidate AMPs at the primary,
secondary, and tertiary peptide structure levels.
Results:
Results showed that the antimicrobial peptide pipeline identifies known AMPs that are
missed by state-of-the-art AMP predictors and that the pipeline yields more AMP candidates from
real bacterial genomes than from fake genomes, with the rate of AMP detection being significantly
higher in the genomes of six nosocomial pathogens than in the fake genomes.
Conclusion:
This bacteria-centric AMP pipeline enhances the detection of bacterial AMPs by incorporating
sequence properties unique to bacterial genomes. It complements existing tools, addressing
gaps in AMP detection and providing a promising avenue for discovering novel antimicrobial
peptides.
Bentham Science Publishers Ltd.
Title: The Antimicrobial Peptide Pipeline: A Bacteria-Centric AMP Predictor
Description:
Introduction:
Antimicrobial peptides (AMPs), unlike antibiotics, are encoded in genomes.
AMPs are exported from the cell after expression and translation.
In the case of bacteria, the
exported peptides target other microbes to give the producing bacterium a competitive edge.
While
AMPs are sought after for their similar antimicrobial activity to traditional antibiotics, it is difficult
to predict which combinations of amino acids will confer antimicrobial activity.
Many computer algorithms
have been designed to predict whether a sequence of amino acids will exhibit antimicrobial
activity, but the vast majority of validated AMPs in databases are still of eukaryotic origin.
This
defies common sense since the vast majority of life on Earth is prokaryotic.
Methods:
The antimicrobial peptide pipeline, presented here, is a bacteria-centric AMP predictor
that predicts AMPs by taking design inspiration from the sequence properties of bacterial genomes
with the intention to improve the detection of naturally occurring bacterial AMPs.
The pipeline integrates
multiple concepts of comparative biology to search for candidate AMPs at the primary,
secondary, and tertiary peptide structure levels.
Results:
Results showed that the antimicrobial peptide pipeline identifies known AMPs that are
missed by state-of-the-art AMP predictors and that the pipeline yields more AMP candidates from
real bacterial genomes than from fake genomes, with the rate of AMP detection being significantly
higher in the genomes of six nosocomial pathogens than in the fake genomes.
Conclusion:
This bacteria-centric AMP pipeline enhances the detection of bacterial AMPs by incorporating
sequence properties unique to bacterial genomes.
It complements existing tools, addressing
gaps in AMP detection and providing a promising avenue for discovering novel antimicrobial
peptides.
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