IntroductionVascular cognitive impairment (VCI) is a syndrome of cognitive dysfunction attributable to vascular risk factors and cerebrovascular diseases, representing a major component of global dementia burden. Dysglycemia, encompassing diabetes mellitus and impaired glucose regulation, is increasingly recognized as a modifiable risk factor for cognitive decline, particularly VCI.
Chronic low-grade inflammation mediates the association between metabolic dysfunction and neurodegeneration. The lack of validated diagnostic tools for early VCI detection in high-risk dysglycemic populations highlights the urgent need for robust diagnostic models based on molecular signatures.MethodsWe analyzed serum samples from 94 participants, categorized into three groups: normal glucose with normal cognition (NG-NC), dysglycemia with normal cognition (Dys-NC), and dysglycemia with VCI (Dys-VCI).
Using the Olink Target 96 Inflammation Panel, we quantified 92 inflammation-related proteins. Differentially expressed proteins (DEPs) were identified as potential biomarkers, followed by functional enrichment analysis to explore associated biological pathways.
Logistic regression models, combined with ROC analysis, assessed the diagnostic utility of selected protein panels across groups.ResultsCompared with NG-NC, the Dys-NC group exhibited upregulated pro-inflammatory mediators (CXCL1, CXCL5, OSM) and downregulated anti-inflammatory proteins (FGF-21, AXIN1).
Frontiers in Immunology published a clinical update in Infectious Disease on 22 May 2026.
The item focuses on OLINK proteomics identifies inflammatory protein signatures associated with vascular cognitive impairment in diabetes.
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