Primers Used in This Study.

Primers Used in This Study.

<div><p>The growing prevalence of methicillin-resistant <i>Staphylococcus aureus</i> (MRSA) infections, coupled with the increasing resistance to existing antibiotics, underscores the critical need for novel therapeutic approaches to combat this pathogen. In this study, the r...

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Xehetasun bibliografikoak
Egile nagusia: Jianhua Liao (1393228) (author)
Beste egile batzuk: Jun Cheng (194158) (author), Baoqing Liu (1508821) (author), Yuzhi Shao (22683349) (author), Chunyan Meng (5993228) (author)
Argitaratua: 2025
Gaiak:
Medicine
Microbiology
Cell Biology
Biotechnology
Evolutionary Biology
Ecology
Science Policy
Infectious Diseases
Virology
Environmental Sciences not elsewhere classified
Biological Sciences not elsewhere classified
therapeutic strategies aimed
novel therapeutic approaches
murine infection model
div >< p
defense mechanisms employed
conserved gene encoding
compromising membrane stability
affect biofilm formation
staphylococcus aureus </
reduced bacterial burden
improved host survival
maintaining mrsa ’
oxidative stress resistance
yqhg </
withstand host
reduced motility
oxidative stress
increasing resistance
stress adaptation
potential target
periplasmic protein
mrsa virulence
mrsa pathogenesis
key determinant
infected organs
increased sensitivity
imposed stresses
growing prevalence
findings highlight
existing antibiotics
critical need
attenuates virulence
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Deskribapena
Gaia:<div><p>The growing prevalence of methicillin-resistant <i>Staphylococcus aureus</i> (MRSA) infections, coupled with the increasing resistance to existing antibiotics, underscores the critical need for novel therapeutic approaches to combat this pathogen. In this study, the role of <i>yqhG</i>, a conserved gene encoding a periplasmic protein, in MRSA virulence and stress adaptation was investigated. <i>yqhG</i> deletion in MRSA significantly attenuated virulence in a murine infection model, leading to reduced bacterial burden in infected organs and improved host survival. In vitro, the <i>yqhG</i> mutant exhibited impaired membrane integrity, reduced motility, and increased sensitivity to oxidative stress, but did not affect biofilm formation. These defects were fully restored upon genetic complementation. These findings highlight the critical role of <i>yqhG</i> in maintaining MRSA’s ability to withstand host-imposed stresses, suggesting that <i>yqhG</i> is a key determinant of MRSA pathogenesis. The study provides new insights into the stress-defense mechanisms employed by MRSA and underscores <i>yqhG</i> as a potential target for therapeutic strategies aimed at combating MRSA infections.</p></div>

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