NSAIDs Alter Phosphorylated Forms of AQP2 in the Inner Medullary Tip.

Vasopressin increases urine concentration through activation of aquaporin-2 (AQP2) in the collecting duct. Nonsteroidal anti-inflammatory drugs (NSAIDs) block prostaglandin E2 synthesis, and may suppress AQP2 producing a urine concentrating defect. There are four serines in AQP2 that are phosphoryla...

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Main Authors: Huiwen Ren, Baoxue Yang, Patrick A Molina, Jeff M Sands, Janet D Klein
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2015-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4627840?pdf=render
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spelling doaj-c797510464cf4cad8fc6088593d5a04f2020-11-24T20:50:02ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-011010e014171410.1371/journal.pone.0141714NSAIDs Alter Phosphorylated Forms of AQP2 in the Inner Medullary Tip.Huiwen RenBaoxue YangPatrick A MolinaJeff M SandsJanet D KleinVasopressin increases urine concentration through activation of aquaporin-2 (AQP2) in the collecting duct. Nonsteroidal anti-inflammatory drugs (NSAIDs) block prostaglandin E2 synthesis, and may suppress AQP2 producing a urine concentrating defect. There are four serines in AQP2 that are phosphorylated by vasopressin. To determine if chronic use of NSAIDs changes AQP2's phosphorylation at any of these residues, the effects of a non-selective NSAID, ibuprofen, and a COX-2-selective NSAID, meloxicam, were investigated. Daily ibuprofen or meloxicam increased the urine output and decreased the urine osmolality significantly by days 7 through 14. Concomitantly, meloxicam significantly reduced total AQP2 protein abundance in inner medulla (IM) tip to 64% of control and base to 63%, respectively. Ibuprofen significantly decreased total AQP2 in IM tip to 70% of control, with no change in base. Meloxicam significantly increased the ratios of p256-AQP2 and p261-AQP2 to total AQP2 in IM tip (to 44% and 40%, respectively). Ibuprofen increased the ratio of p256-AQP2 to total AQP2 in IM tip but did not affect p261-AQP2/total AQP2 in tip or base. Both ibuprofen and meloxicam increased p264-AQP2 and p269-AQP2 ratios in both tip and base. Ibuprofen increased UT-A1 levels in IM tip, but not in base. We conclude that NSAIDs reduce AQP2 abundance, contributing to decreased urine concentrating ability. They also increase some phosphorylated forms of AQP2. These changes may partially compensate for the decrease in AQP2 abundance, thereby lessening the decrease in urine osmolality.http://europepmc.org/articles/PMC4627840?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Huiwen Ren
Baoxue Yang
Patrick A Molina
Jeff M Sands
Janet D Klein
spellingShingle Huiwen Ren
Baoxue Yang
Patrick A Molina
Jeff M Sands
Janet D Klein
NSAIDs Alter Phosphorylated Forms of AQP2 in the Inner Medullary Tip.
PLoS ONE
author_facet Huiwen Ren
Baoxue Yang
Patrick A Molina
Jeff M Sands
Janet D Klein
author_sort Huiwen Ren
title NSAIDs Alter Phosphorylated Forms of AQP2 in the Inner Medullary Tip.
title_short NSAIDs Alter Phosphorylated Forms of AQP2 in the Inner Medullary Tip.
title_full NSAIDs Alter Phosphorylated Forms of AQP2 in the Inner Medullary Tip.
title_fullStr NSAIDs Alter Phosphorylated Forms of AQP2 in the Inner Medullary Tip.
title_full_unstemmed NSAIDs Alter Phosphorylated Forms of AQP2 in the Inner Medullary Tip.
title_sort nsaids alter phosphorylated forms of aqp2 in the inner medullary tip.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2015-01-01
description Vasopressin increases urine concentration through activation of aquaporin-2 (AQP2) in the collecting duct. Nonsteroidal anti-inflammatory drugs (NSAIDs) block prostaglandin E2 synthesis, and may suppress AQP2 producing a urine concentrating defect. There are four serines in AQP2 that are phosphorylated by vasopressin. To determine if chronic use of NSAIDs changes AQP2's phosphorylation at any of these residues, the effects of a non-selective NSAID, ibuprofen, and a COX-2-selective NSAID, meloxicam, were investigated. Daily ibuprofen or meloxicam increased the urine output and decreased the urine osmolality significantly by days 7 through 14. Concomitantly, meloxicam significantly reduced total AQP2 protein abundance in inner medulla (IM) tip to 64% of control and base to 63%, respectively. Ibuprofen significantly decreased total AQP2 in IM tip to 70% of control, with no change in base. Meloxicam significantly increased the ratios of p256-AQP2 and p261-AQP2 to total AQP2 in IM tip (to 44% and 40%, respectively). Ibuprofen increased the ratio of p256-AQP2 to total AQP2 in IM tip but did not affect p261-AQP2/total AQP2 in tip or base. Both ibuprofen and meloxicam increased p264-AQP2 and p269-AQP2 ratios in both tip and base. Ibuprofen increased UT-A1 levels in IM tip, but not in base. We conclude that NSAIDs reduce AQP2 abundance, contributing to decreased urine concentrating ability. They also increase some phosphorylated forms of AQP2. These changes may partially compensate for the decrease in AQP2 abundance, thereby lessening the decrease in urine osmolality.
url http://europepmc.org/articles/PMC4627840?pdf=render
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