AI Article Synopsis
- Healthcare-associated methicillin-resistant infections (MRSA) have high rates of illness and death globally, prompting research on potential treatments.
- This study examined the synergistic effects of Epigalocatenin-3-gallate (EGCG) combined with various antibiotics on different resistant bacterial strains isolated from patients in a Lisbon hospital.
- Results indicated that EGCG exposure significantly impacted the expression of genes related to drug resistance and epigenetics, suggesting its potential as a novel antimicrobial agent or supportive treatment against antibiotic-resistant infections.
Article Abstract
Healthcare-associated methicillin-resistant infections represent extremely high morbidity and mortality rates worldwide. We aimed to assess the antimicrobial potential and synergistic effect between Epigalocatenin-3-gallate (EGCG) and different antibiotics in strains with divergent resistance phenotypes. EGCG exposure effects in epigenetic and drug resistance key modulators were also evaluated. strains ( = 32) were isolated from infected patients in a Lisbon hospital. The identification of the resistance phenotype was performed through automatized methods. The antibiotic synergistic assay was performed through disk diffusion according to EUCAST guidelines with co-exposure to EGCG (250, 100, 50 and 25 µg/mL). The bacteria's molecular profile was assessed through FTIR spectroscopy. The transcriptional expression of , and was performed by using qRT-PCR. FTIR-spectroscopy analysis enabled the clear discrimination of MRSA/MSSA strains and the EGCG exposure effect in the bacteria's molecular profiles. Divergent resistant phenotypes were associated with divergent transcriptional expression of the epigenetic modulator , particularly in MRSA strains, as well as the key drug response modulators and . These results clearly demonstrate that EGCG exposure alters the expression patterns of key epigenetic and drug response genes with associated divergent-resistant profiles, which supports its potential for antimicrobial treatment and/or therapeutic adjuvant against antibiotic-resistant microorganisms.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10044528 | PMC |
| http://dx.doi.org/10.3390/antibiotics12030519 | DOI Listing |
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