Graphical abstract.

Graphical abstract.

<p>Overview of the experimental design and major findings. Eighteen Sprague–Dawley rats were randomly divided into three groups: uninfected control (CON), acute infection (AI, day 7 post-infection), and chronic infection (CI, day 40 post-infection). Rats in the AI and CI groups were orally ino...

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Bibliografiset tiedot
Päätekijä: Ji-Xin Zhao (22056386) (author)
Muut tekijät: Wen-Bin Zheng (3328680) (author), Shi-Chen Xie (10678094) (author), He Ma (583317) (author), Xiao-Tong Chen (4217488) (author), Ying-Qian Gao (22683622) (author), Lu-Yao Tang (22683625) (author), Meng-Ting Yang (10714266) (author), Fu-Long Nan (22056395) (author), Jing Jiang (130103) (author), Hany M. Elsheikha (6910232) (author), Xiao-Xuan Zhang (610969) (author)
Julkaistu: 2025
Aiheet:
Biochemistry
Microbiology
Cell Biology
Genetics
Physiology
Ecology
Immunology
Computational Biology
Biological Sciences not elsewhere classified
Chemical Sciences not elsewhere classified
showed negative associations
quality reads produced
oxidative stress response
conducted metagenomic sequencing
compositional changes coincided
bile acid transformation
aromatic compound processing
7 million genes
rothia nasimurium </
lactobacillus intestinalis </
de novo </
untargeted serum metabolomics
specific metabolic disruptions
amino acid metabolism
toxoplasma gondii </
limosilactobacillus reuteri </
lactobacillus johnsonii </
akkermansia muciniphila </
host systemic metabolism
disrupts intestinal microbiota
reuteri </
muciniphila </
johnsonii </
gondii </
host metabolism
untargeted lc
metabolic targets
energy metabolism
infection disrupts
significant shifts
reduced abundance
rat model
positively correlated
pathways related
novel microbial
microbial diversity
metabolites implicated
marked reduction
marked depletion
key role
immune modulation
gut microbiota
findings demonstrate
enhanced glycan
disease mechanisms
comprehensive non
community structure
chronic stages
active enzymes
18 sprague
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Yhteenveto:<p>Overview of the experimental design and major findings. Eighteen Sprague–Dawley rats were randomly divided into three groups: uninfected control (CON), acute infection (AI, day 7 post-infection), and chronic infection (CI, day 40 post-infection). Rats in the AI and CI groups were orally inoculated with 3,000 <i>T. gondii</i> PRU cysts, while controls received PBS. Small and large intestinal contents were collected for metagenomic sequencing, and serum was analyzed by untargeted metabolomics. The integrated multi-omics analysis revealed stage-specific alterations in gut microbial diversity, taxonomic composition, and functional potential, along with systemic metabolic perturbations. Spearman correlation analysis demonstrated coordinated associations between differential microbes and metabolites, illustrating the interaction network among <i>T. gondii</i>, the gut microbiota, and host metabolism. Created in BioRender. Jx, Z. (2025) <a href="https://BioRender.com/2rh0rbd" target="_blank">https://BioRender.com/2rh0rbd</a>.</p> <p>(TIF)</p>

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