AI Article Synopsis

  • Thyroid eye disease (TED) shows a link between dysregulated immune responses and brain activity, specifically in the insular cortex.
  • Researchers studied 34 active and 30 inactive TED patients, along with 45 healthy controls, using brain imaging techniques to evaluate neural activity and its correlation with immune markers.
  • Findings indicated that active TED patients had increased neural activity in the insular cortex and altered connectivity to the cerebellum compared to inactive patients and controls, highlighting the insular cortex's potential role in the disease's central and peripheral interactions.

Article Abstract

Background: Thyroid eye disease (TED) is highly correlated with dysregulated immunoendocrine status. The insular cortex was found to regulate peripheral inflammation and immunomodulation in mice. This study aimed to explore whether the insular cortex in patients with TED played a modulatory role including the aberrant brain functional alteration and its association with immunoendocrine status.

Methods: This study included 34 active patients (AP), 30 inactive patients (IP) with TED, and 45 healthy controls (HC) matched for age, sex, and educational level. Comprehensive clinical details (especially immunoendocrine markers) and resting-state functional magnetic resonance imaging data were collected from each participant. The amplitude of low-frequency fluctuation (ALFF) was used to probe the aberrant alterations of local neural activity. The seed-based functional connectivity (FC) analysis was used to explore the relationship between the insular cortex and each voxel throughout the whole brain. The correlation analysis was conducted to assess the association between insular neurobiomarkers and immunoendocrine parameters.

Results: When compared with the IP and HC groups, the AP group displayed significantly higher ALFF values in the right insular cortex (INS.R) and lower FC values between the INS.R and the bilateral cerebellum. None of the neurobiomarkers differed between the IP and HC groups. Besides, correlations between insular neurobiomarkers and immunoendocrine markers (free thyroxine, the proportion of T cells, and natural killer cells) were identified in both AP and IP groups.

Conclusions: This study was novel in reporting that the dysregulation of the insular cortex activity in TED was associated with abnormal peripheral immunoendocrine status. The insular cortex might play a key role in central-peripheral system interaction in TED. Further research is crucial to enhance our understanding of the central-peripheral system interaction mechanisms involved in autoimmune diseases.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10874024PMC
http://dx.doi.org/10.1186/s12974-024-03044-4DOI Listing

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