Reutericin

Reutericin is a bacteriocin — a ribosomally synthesized antimicrobial peptide — produced by certain strains of Lactobacillus reuteri (reclassified as Limosilactobacillus reuteri in 2020). Multiple reutericin variants have been identified, including reutericin 6, reutericin A, and a circular bacteriocin (reutericin produced by L. reuteri LA6), each with distinct structural features and spectra of activity.

Overview

Lactobacillus reuteri is among the most extensively studied probiotic species, with a well-documented presence in the gastrointestinal tract of humans and other vertebrates. The species deploys multiple antimicrobial strategies for ecological competition: organic acid production (lactic and acetic acid), reuterin (3-hydroxypropionaldehyde, a non-peptide antimicrobial produced from glycerol by glycerol dehydratase), and bacteriocins including reutericin.

The distinction between reutericin (peptide bacteriocin) and reuterin (small-molecule antimicrobial) is important. Reuterin is a three-carbon aldehyde produced from glycerol via the pdu (propanediol utilization) operon-encoded glycerol dehydratase. It is not a peptide and acts through broad-spectrum protein crosslinking and oxidative damage. Reutericin, by contrast, is a gene-encoded peptide with receptor-mediated killing activity and a narrower spectrum.

Several reutericin variants have been characterized:

Reutericin 6: Originally isolated from L. reuteri LA6 by Kabuki et al. (1997), this is a circular (head-to-tail cyclized) bacteriocin classified as Class IIc. Circular bacteriocins are characterized by their enhanced thermostability and protease resistance relative to linear counterparts. Reutericin 6 consists of 58 amino acids with a molecular mass of approximately 5.6 kDa and is active against Lactobacillus delbrueckii, L. helveticus, and other closely related LAB species Kabuki et al. (1997).

Reutericin A: A heat-stable, protease-sensitive bacteriocin produced by L. reuteri LA6 with activity against Listeria monocytogenes and other Gram-positive pathogens. Its structural classification places it among Class IIa (pediocin-like) bacteriocins containing the conserved YGNGV/L N-terminal motif that characterizes anti-listerial bacteriocins.

Other L. reuteri bacteriocins: Additional antimicrobial peptides have been identified from various L. reuteri strains through genome mining, including potential lantibiotics and two-peptide bacteriocins, reflecting the genomic diversity of this species.

Mechanism of Action

The antimicrobial mechanism of reutericin involves membrane disruption through several coordinated steps:

• Target cell recognition: Reutericin interacts with the target cell membrane, likely through electrostatic attraction between the cationic peptide and anionic phospholipids in the bacterial membrane. Specific receptor molecules (e.g., mannose PTS components for Class IIa bacteriocins) may also mediate initial binding, conferring spectrum specificity.
• Membrane insertion: Following binding, the amphipathic helical structure of reutericin inserts into the lipid bilayer. Circular bacteriocins such as reutericin 6 are particularly effective at membrane insertion due to their compact, stable fold and defined hydrophobic surface.
• Pore formation and ion leakage: Reutericin oligomerizes in the membrane to form transient pores, causing efflux of potassium ions, dissipation of the proton motive force (PMF), and depletion of intracellular ATP. The collapse of PMF halts energy-dependent processes including nutrient uptake and biosynthesis Gálvez et al. (2007).
• Cell death: The combined effects of ion leakage, PMF dissipation, and ATP depletion lead to rapid bactericidal killing. Unlike bacteriolytic enzymes, bacteriocins do not typically lyse target cells — death occurs through energy depletion rather than cell wall destruction.
• Producer self-immunity: L. reuteri strains producing reutericin co-express dedicated immunity proteins that protect the producer from its own bacteriocin. These immunity proteins are typically small membrane-associated peptides that interfere with pore formation or expel the bacteriocin from the producer cell membrane.

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Safety Profile

Reutericin inherits the favorable safety profile associated with L. reuteri and LAB bacteriocins generally:

• GRAS status of producer: L. reuteri has GRAS status and Qualified Presumption of Safety (QPS) status in the EU. Multiple strains (DSM 17938, ATCC PTA 5289, ATCC 55730) have been used in clinical trials involving neonates, infants, children, and adults with no serious adverse events attributable to the probiotic.
• Proteolytic inactivation: Like most Class II bacteriocins, reutericin is susceptible to degradation by gastrointestinal proteases (pepsin, trypsin, chymotrypsin), limiting systemic exposure and confining activity to the luminal environment.
• No cytotoxicity to eukaryotic cells: At concentrations relevant to antimicrobial activity, bacteriocins from LAB species do not damage mammalian cell membranes. The selectivity arises from the fundamental difference between prokaryotic (anionic phospholipid-rich) and eukaryotic (cholesterol-stabilized, zwitterionic phospholipid) membranes.
• Narrow spectrum: The primarily anti-LAB spectrum of reutericin 6 limits collateral damage to the commensal microbiota. However, broader-spectrum variants (reutericin A) could potentially affect beneficial lactobacilli if delivered at high concentrations.
• No known allergenicity: No allergic or hypersensitivity reactions have been reported in association with bacteriocin-producing L. reuteri strains in clinical or food-use settings.

Pharmacokinetic Profile