Publications by authors named "Thi Thu Hang Le"

Article Synopsis
  • Four isolates of Elizabethkingia anophelis were identified in a Vietnamese hospital and underwent extensive testing for antibiotic resistance and genomic analysis.
  • Three of the four isolates were found to be genetically distinct, indicating multiple strain emergence rather than a single outbreak strain.
  • The isolates showed resistance to a wide range of antibiotics and contained nine resistance genes within a predicted Integrative and Conjugative Element, suggesting a complex mechanism of resistance that warrants further research.
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  • This study focuses on Burkholderia dolosa, a dangerous pathogen that can cause infections in hospitalized patients, especially those with strokes. A specific isolate, B. dolosa N149, was characterized as highly resistant to many antibiotics and exceptionally virulent.
  • Using advanced genetic techniques, the researchers identified that this strain had resistance to 31 antibiotics and showcased various mechanisms like multidrug efflux pumps that contribute to its drug resistance.
  • The genome analysis revealed numerous virulence genes linked to its ability to cause disease, and B. dolosa N149 was classified as a new sequence type, furthering understanding of its genetic diversity and potential threat in clinical settings.
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  • The study focuses on the emergence of multidrug-resistant bacteria in Vietnamese hospitals due to the spread of antimicrobial resistance (AMR) genes on plasmids.
  • Using whole-genome sequencing data from 751 clinical isolates, researchers found that plasmids containing AMR genes are prevalent, especially in carbapenem-resistant strains.
  • The findings highlight the role of horizontal gene transfer in increasing antibiotic resistance and emphasize the need for strategies to prevent plasmid transmission and reduce antibiotic misuse.
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The type VI secretion system (T6SS) delivers enzymatic effectors into target cells to destroy them. Cells of the same strain protect themselves against effectors with immunity proteins that specifically inhibit effectors. Here, we report the identification and characterization of a Tle3 phospholipase effector and its cognate immunity protein Tli3-an outer membrane lipoprotein from adherent-invasive (AIEC).

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To date, endophytic actinomycetes have been well-documented as great producers of novel antibiotics and important pharmaceutical leads. The present study aimed to evaluate potent bioactivities of metabolites synthesized by the strain LCP18 residing in the Vietnamese medicinal plant Litsea cubeba (Lour.) Pers towards human pathogenic bacteria and human cancer cell lines.

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The Type VI secretion system (T6SS) is a multiprotein machine that delivers protein effectors in both prokaryotic and eukaryotic cells, allowing interbacterial competition and virulence. The mechanism of action of the T6SS requires the contraction of a sheath-like structure that propels a needle towards target cells, allowing the delivery of protein effectors. Here, we provide evidence that the entero-aggregative Escherichia coli Sci-1 T6SS is required to eliminate competitor bacteria.

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The type VI secretion system (T6SS) is a secretion pathway widespread in Gram-negative bacteria that targets toxins in both prokaryotic and eukaryotic cells. Although most T6SSs identified so far are involved in inter-bacterial competition, a few are directly required for full virulence of pathogens. The T6SS comprises 13 core proteins that assemble a large complex structurally and functionally similar to a phage contractile tail structure anchored to the cell envelope by a trans-membrane spanning stator.

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The type VI secretion system (T6SS) is a machine evolved by Gram-negative bacteria to deliver toxin effectors into target bacterial or eukaryotic cells. The T6SS is functionally and structurally similar to the contractile tail of the Myoviridae family of bacteriophages and can be viewed as a syringe anchored to the bacterial membrane by a transenvelope complex. The membrane complex is composed of three proteins: the TssM and TssL inner membrane components and the TssJ outer membrane lipoprotein.

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