AI Article Synopsis
- * Sodium interacts with tissue glycosaminoglycans, affecting local tonicity and activating TonEBP, which is linked to macrophage infiltration and inflammatory responses in various tissues, particularly the heart.
- * Reducing salt intake through diuretics or tap water can lower inflammation and macrophage activity, suggesting that managing sodium levels might be key in preventing organ dysfunction in CKD patients; further research is needed to refine treatment strategies.
Article Abstract
High salt intake is a primary cause of over-hydration in chronic kidney disease (CKD) patients. Inflammatory markers are predictors of CKD mortality; however, the pathogenesis of inflammation remains unclear. Sodium storage in tissues has recently emerged as an issue of concern. The binding of sodium to tissue glycosaminoglycans and its subsequent release regulates local tonicity. Many cell types express tonicity-responsive enhancer-binding protein (TonEBP), which is activated in a tonicity-dependent or tonicity-independent manner. Macrophage infiltration was observed in the heart, peritoneal wall, and para-aortic tissues in salt-loading subtotal nephrectomized mice, whereas macrophages were not prominent in tap water-loaded subtotal nephrectomized mice. TonEBP was increased in the heart and peritoneal wall, leading to the upregulation of inflammatory mediators associated with cardiac fibrosis and peritoneal membrane dysfunction, respectively. Reducing salt loading by a diuretic treatment or changing to tap water attenuated macrophage infiltration, TonEBP expression, and inflammatory marker expression. The role of TonEBP may be crucial during the cardiac fibrosis and peritoneal deterioration processes induced by sodium overload. Anti-interleukin-6 therapy improved cardiac inflammation and fibrosis and peritoneal membrane dysfunction. Further studies are necessary to establish a strategy to regulate organ dysfunction induced by TonEBP activation in CKD patients.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10179540 | PMC |
| http://dx.doi.org/10.3390/ijms24098329 | DOI Listing |
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