Abstract

In recent decades, evidence has confirmed the crucial role of albumin in the progression of renal disease. However, the possible role of signaling pathways triggered by physiologic concentrations of albumin in the modulation of proximal tubule (PT) sodium reabsorption has not been considered. In the present work, we have shown that a physiologic concentration of albumin increases the expression of the α1 subunit of (Na(+) + K(+))-ATPase in LLC-PK1 cells leading to an increase in enzyme activity. This process involves the sequential activation of PI3K/protein kinase B and protein kinase C pathways promoting inhibition of protein kinase A. This integrative network is inhibited when albumin concentration is increased, similar to renal disease, leading to a decrease in the α1 subunit of (Na(+) + K(+))-ATPase expression. Together, the results indicate that variation in albumin concentration in PT cells has an important effect on PT sodium reabsorption and, consequently, on renal sodium excretion.

Highlights

  • Albumin interacts with megalin and triggers cellular responses in proximal tubule cells

  • Our results reveal an important role of albumin in proximal tubule (PT) sodium reabsorption

  • Albumin increases (Naϩ ϩ Kϩ)-ATPase activity by increasing ␣1 subunits. This effect of lower albumin concentration on PT (Naϩ ϩ Kϩ)-ATPase activity agrees with the high level of sodium reabsorption in this segment

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Summary

Introduction

Albumin interacts with megalin and triggers cellular responses in proximal tubule cells. We have shown that a physiologic concentration of albumin increases the expression of the ␣1 subunit of (Na؉ ؉ K؉)ATPase in LLC-PK1 cells leading to an increase in enzyme activity. This process involves the sequential activation of PI3K/ protein kinase B and protein kinase C pathways promoting inhibition of protein kinase A. This integrative network is inhibited when albumin concentration is increased, similar to renal disease, leading to a decrease in the ␣1 subunit of (Na؉ ؉ K؉)ATPase expression. The results indicate that variation in albumin concentration in PT cells has an important effect on PT sodium reabsorption and, on renal sodium excretion

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