A new variant of ASIC2 mediates sodium retention in nephrotic syndrome Article Swipe

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Epithelial sodium channel Aldosterone Endocrinology Internal medicine Nephrotic syndrome Chemistry Amiloride Sodium Proteinuria Kidney Context (archaeology) Medicine Biology Organic chemistry Paleontology

Marc Fila , Ali Sassi , Gaëlle Brideau , Lydie Cheval , Luciana Morla , Pascal Houillier , Christine Walter , Michel Gennaoui , Laure Collignon L , Mathilde Keck , Gabrielle Planelles , Naziha Bakouh , Michel Peuchmaur , Georges Deschênes , Ignacio Anegón , Séverine Remy , Bruno Vogt , Gilles Crambert , Alain Doucet ·

YOU? · · 2021 · Open Access · · DOI: https://doi.org/10.1101/2021.02.09.430231 · OA: W3128218059

Idiopathic nephrotic syndrome (INS) is characterized by proteinuria and renal Na retention leading to oedema. This Na retention is usually attributed to epithelial sodium channel (ENaC) activation following plasma aldosterone increase. However, most nephrotic patients show normal aldosterone levels. Using a corticosteroid-clamped rat model of INS (CC-PAN), we showed that the observed electrogenic and amiloride-sensitive Na retention could not be attributed to ENaC. We, then, identified a truncated variant of acid sensing ion channel 2b (ASIC2b) that induced sustained acid-stimulated sodium currents when co-expressed with ASIC2a. Interestingly, CC-PAN nephrotic ASIC2b-null rats did not develop sodium retention. We finally showed that expression of the truncated ASIC2b in kidney was dependent on the presence of albumin in the tubule lumen and activation of ERK in renal cells. Finally, the presence of ASIC2 mRNA was also detected in kidney biopsies from patients with INS but in any of the patients with other renal diseases. We have, therefore, identified a novel variant of ASIC2b responsible for the renal Na retention in the pathological context of INS.