Abstract
Bacteria commonly produce narrow spectrum bacteriocins as a means of inhibiting closely related species competing for similar resources in an environment. The increasing availability of genomic data means that it is becoming easier to identify bacteriocins encoded within genomes. Often, however, the presence of bacteriocin genes in a strain does not always translate into biological antimicrobial activity. For example, when analysing the Lactobacillus pangenome we identified strains encoding ten pediocin-like bacteriocin structural genes which failed to display inhibitory activity. Nine of these bacteriocins were novel whilst one was identified as the previously characterized bacteriocin “penocin A.” The composition of these bacteriocin operons varied between strains, often with key components missing which are required for bacteriocin production, such as dedicated bacteriocin transporters and accessory proteins. In an effort to functionally express these bacteriocins, the structural genes for the ten pediocin homologs were cloned alongside the dedicated pediocin PA-1 transporter in both Escherichia coli and Lactobacillus paracasei heterologous hosts. Each bacteriocin was cloned with its native leader sequence and as a fusion protein with the pediocin PA-1 leader sequence. Several of these bacteriocins displayed a broader spectrum of inhibition than the original pediocin PA-1. We show how potentially valuable bacteriocins can easily be “reincarnated” from in silico data and produced in vitro despite often lacking the necessary accompanying machinery. Moreover, the study demonstrates how genomic datasets such as the Lactobacilus pangenome harbor a potential “arsenal” of antimicrobial activity with the possibility of being activated when expressed in more genetically amenable hosts.
Highlights
Bacteria exist in complex communities, under constant competition from other strains and species for nutrients and space
This study focused on the class IIa bacteriocins; eight strains were found to encode ten of these pediocin-like bacteriocins but failed to display any antimicrobial production
Of these ten potential bacteriocins identified, nine were novel and one was identified as penocin A, a bacteriocin previously characterized from P. pentosaceus ATCC 25745 (Diep et al, 2006; Table 1)
Summary
Bacteria exist in complex communities, under constant competition from other strains and species for nutrients and space. The increasing availability of genomic data has changed the way we identify and study bacteriocins in communities Bioinformatic screening tools such as BAGEL (de Jong et al, 2010) and antiSMASH (Weber et al, 2015) can process vast amounts of genomic data to search for antimicrobial operons and genes (Letzel et al, 2014; Walsh et al, 2015). This allows us to identify previously uncharacterized bacteriocins and antibiotics, and to understand the extent of which strains encode these natural weapons for targeting competitors. This allows for the natural bacteriocin regulation to be circumvented and/or gene loss to be overcome, ensuring production of otherwise unavailable antimicrobials for further characterization and potential exploitation
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