| Literature DB >> 29395338 |
Laetitia Dou1, Stéphane Poitevin1, Marion Sallée2, Tawfik Addi1, Bertrand Gondouin3, Nathalie McKay1, Michael S Denison4, Noémie Jourde-Chiche2, Ariane Duval-Sabatier5, Claire Cerini1, Philippe Brunet2, Françoise Dignat-George1, Stéphane Burtey6.
Abstract
Patients with chronic kidney disease (CKD) are exposed to uremic toxins and have an increased risk of cardiovascular disease. Some uremic toxins, like indoxyl sulfate, are agonists of the transcription factor aryl hydrocarbon receptor (AHR). These toxins induce a vascular procoagulant phenotype. Here we investigated AHR activation in patients with CKD and in a murine model of CKD. We performed a prospective study in 116 patients with CKD stage 3 to 5D and measured the AHR-Activating Potential of serum by bioassay. Compared to sera from healthy controls, sera from CKD patients displayed a strong AHR-Activating Potential; strongly correlated with eGFR and with the indoxyl sulfate concentration. The expression of the AHR target genes Cyp1A1 and AHRR was up-regulated in whole blood from patients with CKD. Survival analyses revealed that cardiovascular events were more frequent in CKD patients with an AHR-Activating Potential above the median. In mice with 5/6 nephrectomy, there was an increased serum AHR-Activating Potential, and an induction of Cyp1a1 mRNA in the aorta and heart, absent in AhR-/- CKD mice. After serial indoxyl sulfate injections, we observed an increase in serum AHR-AP and in expression of Cyp1a1 mRNA in aorta and heart in WT mice, but not in AhR-/- mice. Thus, the AHR pathway is activated both in patients and mice with CKD. Hence, AHR activation could be a key mechanism involved in the deleterious cardiovascular effects observed in CKD.Entities:
Keywords: aryl hydrocarbon receptor; cardiovascular disease; chronic kidney disease; indoxyl sulfate; mouse model
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Year: 2018 PMID: 29395338 DOI: 10.1016/j.kint.2017.11.010
Source DB: PubMed Journal: Kidney Int ISSN: 0085-2538 Impact factor: 10.612