CD14 in Salt‐Sensitive Hypertension‐Related Cognitive Impairments

Background Hypertension is a leading risk factor for the development of Alzheimer’s disease and Alzheimer’s disease‐related dementia (AD/ADRD), which is closely linked with cerebral vascular inflammation and dysfunction. We previously found that high‐salt‐treated Dahl Salt‐Sensitive (SS) rats displa...

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Published in:Alzheimer's & dementia 2024-12, Vol.20 (S1), p.n/a
Main Authors: Tang, Chengyun, Burns, Emily, Border, Jane J., Bunn, David, Cantwell, Cameron, Gregory, Andrew, Johnson, Claire, Dong, Yanbin, Roman, Richard J., Mattson, David L, Fan, Fan
Format: Article
Language:English
Subjects:
Basic Science and Pathogenesis
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Summary:Background Hypertension is a leading risk factor for the development of Alzheimer’s disease and Alzheimer’s disease‐related dementia (AD/ADRD), which is closely linked with cerebral vascular inflammation and dysfunction. We previously found that high‐salt‐treated Dahl Salt‐Sensitive (SS) rats displayed blood‐brain barrier (BBB) leakage, astrocyte activation, neurodegeneration, and cognitive impairments. CD14 functions in the Toll‐like receptor 4 (TLR4) complex to initiate proinflammatory signaling events in response to LPS. CD14 levels were elevated in the brains of human and animal AD/ADRD models. This study aims to explore the vascular contribution of CD14 to AD/ADRD. Method The expression of Cd14 was assessed through RT‐PCR in primary cerebral vascular smooth muscle cells (VSMCs) isolated from TgF344‐AD rats, and the results were compared to cells from control rats. The myogenic response of the middle cerebral artery (MCA) was compared between SS (SSCD14+/+), SSCD14‐/‐, and SD rats with and without the induction of hypertension with 4% NaCl diets. BBB function was detected by the leakage of injected Evans blue and fibrinogen. Brain cytokine levels were detected with Bio‐Plex Rat Cytokine 23‐Plex Assay. Result Cd14 emerged as one of the significantly upregulated top genes in high‐salt‐fed SSCD14+/+ rats, with a subsequent three‐fold increase observed specifically in cerebral VSMCs of AD compared with control rats. Hypertensive SSCD14+/+ rats exhibited an impaired myogenic response of the MCA compared to normotensive SSCD14+/+ rats and SD rats fed with both high‐ and low‐salt diets. Notably, the deletion of CD14 demonstrated a remarkable trend in enhancing the myogenic response of the MCA in female SSCD14‐/‐ rats. Furthermore, high salt‐fed 24‐week SSCD14+/+ rats displayed BBB dysfunction. An augmented pan‐cytokine panel was observed in low salt‐fed 12‐week SSCD14+/+ rats, and this effect was magnified in high salt‐fed 24‐week SSCD14+/+ rats. Conclusion These results collectively point to the potential role of CD14 in influencing vascular and immune responses, suggesting a link between CD14, hypertension, and cerebrovascular pathologies, particularly in the context of AD. Additional investigations are warranted to delve into the underlying mechanisms and ascertain whether CD14 exhibits a sex‐specific role in AD/ADRD.
ISSN:1552-5260
1552-5279
DOI:10.1002/alz.087018