[HTML][HTML] Indoxyl sulfate in uremia: an old idea with updated concepts
The Journal of Clinical Investigation, 2022•Am Soc Clin Investig
Patients with end-stage kidney disease (ESKD) have increased vascular disease. While
protein-bound molecules that escape hemodialysis may contribute to uremic toxicity, specific
contributing toxins remain ambiguous. In this issue of the JCI, Arinze et al. explore the role of
tryptophan metabolites in chronic kidney disease–associated (CKD-associated) peripheral
arterial disease. The authors used mouse and zebrafish models to show that circulating
indoxyl sulfate (IS) blocked endothelial Wnt signaling, which impaired angiogenesis. Plasma …
protein-bound molecules that escape hemodialysis may contribute to uremic toxicity, specific
contributing toxins remain ambiguous. In this issue of the JCI, Arinze et al. explore the role of
tryptophan metabolites in chronic kidney disease–associated (CKD-associated) peripheral
arterial disease. The authors used mouse and zebrafish models to show that circulating
indoxyl sulfate (IS) blocked endothelial Wnt signaling, which impaired angiogenesis. Plasma …
Patients with end-stage kidney disease (ESKD) have increased vascular disease. While protein-bound molecules that escape hemodialysis may contribute to uremic toxicity, specific contributing toxins remain ambiguous. In this issue of the JCI, Arinze et al. explore the role of tryptophan metabolites in chronic kidney disease–associated (CKD-associated) peripheral arterial disease. The authors used mouse and zebrafish models to show that circulating indoxyl sulfate (IS) blocked endothelial Wnt signaling, which impaired angiogenesis. Plasma levels of IS and other tryptophan metabolites correlated with adverse peripheral vascular disease events in humans. These findings suggest that lowering IS may benefit individuals with CKD and ESKD.
The Journal of Clinical Investigation