Bacteria Use Lactic Acid to Suppress Immune Response in Chronic Wounds

Mechanisms of Immune Evasion by E. faecalis

Bacteria in prolonged wound infections have developed advanced strategies to evade immune detection. A study in Cell Host & Microbe reveals that Enterococcus faecalis, linked to chronic infections like diabetic foot ulcers, releases lactic acid to lower the wound environment’s pH. This acidic condition disrupts the NF-κB signaling pathway in macrophages, a critical pathway for triggering inflammatory responses. By blocking NF-κB activation, the bacteria hinder immune recognition of pathogens. This immune suppression allows E. faecalis to persist in wounds, creating conditions for other bacteria like Escherichia coli to thrive. Strains unable to produce lactic acid were swiftly eliminated from mouse wound models, underscoring the importance of this mechanism.

The Dual Role of the Skin Microbiome

The skin microbiome functions as both a protective barrier and a regulator of immune responses. Beneficial bacteria such as Staphylococcus epidermidis and Propionibacterium acnes contribute to tissue repair by generating antimicrobial peptides and short-chain fatty acids (SCFAs). These metabolites influence macrophage polarization, shifting them from pro-inflammatory M1 to anti-inflammatory M2 states. This shift promotes wound closure by reducing inflammation and enhancing extracellular matrix remodeling. However, imbalances in microbial communities—dysbiosis—can worsen chronic wounds. For example, overgrowth of pathogenic bacteria like E. faecalis can outcompete beneficial microbes, leading to persistent inflammation and delayed healing.

Microbiome-Targeted Therapies for Chronic Wounds

Research published in PMC (PubMed Central) highlights the potential of microbiome-targeted therapies for managing chronic wounds. Probiotics like Lactobacillus reuteri have shown promise in reducing inflammation and improving healing in murine models. These interventions aim to restore microbial balance by reintroducing beneficial bacteria or their metabolites. Advanced delivery systems, such as hydrogels and nanomaterials, are being developed to sustain microbial activity and release bioactive compounds at the wound site. These innovations position microbiome engineering as a complementary strategy to traditional antimicrobial treatments.

Clinical Implications of Lactic Acid-Mediated Immune Suppression

The clinical impact of lactic acid-mediated immune suppression is significant, particularly in patients with weakened immune systems or chronic conditions like diabetes. A study notes that E. faecalis’ ability to acidify wounds weakens immune responses, allowing infections to persist and complicate treatment. In diabetic patients, this immune suppression is especially detrimental, as 6.2% of diabetics in India suffer from diabetic foot ulcers, many of which become chronic due to persistent bacterial infections. Data from PMC indicates that chronic wounds affect over 6 million people annually in the U.S., highlighting the widespread public health burden.

Post-Surgical Infections and Emerging Therapies

The findings also have broader implications for post-surgical infections, where E. faecalis is a common cause. The bacterium’s ability to manipulate immune responses creates an environment favorable for co-infecting pathogens like E. coli to thrive. Researchers are exploring treatments targeting acidity or lactic acid signaling, such as pH-neutralizing agents or GPR81 antagonists. These approaches aim to restore immune function without relying solely on antibiotics, which are increasingly ineffective due to rising antimicrobial resistance.

Innovations in Wound Care

Researchers are developing innovative therapies targeting microbial interactions and immune modulation. Probiotics and postbiotics are being tested to restore microbial balance. For instance, Lactobacillus reuteri has been shown to reduce inflammation and improve healing in murine models. Clinical trials are underway to evaluate probiotic formulations in reducing inflammation and enhancing tissue repair. Another frontier involves smart biomaterials that respond to environmental cues like pH or temperature. These materials can release antimicrobial agents or modulate immune responses in real time, offering targeted treatment for persistent infections. Hydrogels infused with probiotics or nanomaterials designed to neutralize lactic acid are being tested in preclinical models.

Challenges in Translating Research to Clinical Practice

While progress has been made in understanding bacterial immune evasion, challenges remain. Most studies rely on murine models, necessitating human trials to confirm therapeutic potential. The Cell Host & Microbe study, funded by the National Research Foundation Singapore, emphasizes the need for human trials to validate targeting lactic acid or GPR81 signaling. Developing scalable delivery systems for probiotics and smart biomaterials requires further research to optimize efficacy and safety. Personalized microbiome therapies also demand deeper understanding of genetic and environmental factors shaping microbial communities in wounds. As the global burden of chronic wounds rises, integrating microbiome-based strategies with traditional wound care remains a critical step forward.