Dysbiosis of gut microbiota and its correlation with dysregulation of cytokines in psoriasis patients

Mar 9, 2021BMC microbiology

Imbalance of Gut Bacteria Linked to Immune System Changes in Psoriasis Patients

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Abstract

Alterations in gut microbiome composition were observed in 30 psoriasis patients compared to 30 healthy individuals.

  • Specific bacterial taxa, such as Faecalibacterium and Megamonas, showed increased relative abundance in psoriasis patients.
  • Variations in gut microbiome were associated with abnormal inflammation-related indicators in psoriasis.
  • Interleukin-2 receptor levels exhibited a positive correlation with Phascolarctobacterium and a negative correlation with Dialister.
  • The relative abundance of Phascolarctobacterium and Dialister may serve as predictors of psoriasis activity.
  • Microbiota dysbiosis could potentially induce an abnormal immune response in psoriasis.

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Key numbers

30
Patients with Psoriasis
Total number of psoriasis patients included in the study
30
Healthy Controls
Total number of healthy individuals included in the study

Full Text

What this is

  • This research investigates the gut microbiota composition in psoriasis patients compared to healthy individuals.
  • It explores the relationship between microbial dysbiosis and inflammation-related cytokines in psoriasis.
  • Findings suggest altered gut microbiota may influence the immune response in psoriasis.

Essence

  • Psoriasis patients exhibit significant differences in gut microbiota composition compared to healthy controls, with specific taxa correlated to inflammatory cytokines. Dysbiosis may play a role in the disease's immune-mediated pathology.

Key takeaways

  • Faecalibacterium and Megamonas are more abundant in psoriasis patients compared to healthy individuals, indicating a potential link to disease activity.
  • Correlation analysis shows a positive relationship between Phascolarctobacterium and interleukin-2 receptor levels, suggesting its role as a predictor of psoriasis activity.
  • The study finds no significant difference in alpha diversity between psoriasis patients and healthy controls, but beta diversity indicates distinct microbiota profiles.

Caveats

  • The study's cross-sectional design limits conclusions about causality between gut microbiota changes and psoriasis severity.
  • Further mechanistic studies are needed to clarify the role of gut microbiota in psoriasis pathogenesis.

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