| Literature DB >> 29846108 |
Roel Bijkerk1,2, Christiane Trimpert3, Coen van Solingen1,4, Ruben G de Bruin1, Barend W Florijn1, Sander Kooijman5, Rosa van den Berg5, Eric P van der Veer1, Edwin O W Bredewold1, Patrick C N Rensen5, Ton J Rabelink1, Benjamin D Humphreys2,6, Peter M T Deen3, Anton Jan van Zonneveld1.
Abstract
Fine-tuning of the body's water balance is regulated by vasopressin (AVP), which induces the expression and apical membrane insertion of aquaporin-2 water channels and subsequent water reabsorption in the kidney. Here we demonstrate that silencing of microRNA-132 (miR-132) in mice causes severe weight loss due to acute diuresis coinciding with increased plasma osmolality, reduced renal total and plasma membrane expression of aquaporin-2, and abrogated increase in AVP levels. Infusion with synthetic AVP fully reversed the antagomir-132-induced diuresis, and low-dose intracerebroventricular administration of antagomir-132 similarly caused acute diuresis. Central and intracerebroventricular antagomir-132 injection both decreased hypothalamic AVP mRNA levels. At the molecular level, antagomir-132 increased the in vivo and in vitro mRNA expression of methyl-CpG-binding protein-2 (MECP2), which is a miR-132 target and which blocks AVP gene expression by binding its enhancer region. In line with this, treatment of hypothalamic N6 cells with a high-salt solution increased its miR-132 levels, whereas it attenuated endogenous Mecp2 mRNA levels. In conclusion, we identified miR-132 as a first miRNA regulating the osmotic balance by regulating the hypothalamic AVP gene mRNA expression.Entities:
Keywords: microRNA; osmotic balance; posttranscriptional regulation; vasopressin
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Year: 2018 PMID: 29846108 DOI: 10.1152/ajprenal.00087.2018
Source DB: PubMed Journal: Am J Physiol Renal Physiol ISSN: 1522-1466