Abstract
BackgroundGenetic disruption of slc4a10, which encodes the sodium-dependent chloride/bicarbonate exchanger Ncbe, leads to a major decrease in Na+-dependent HCO3− import into choroid plexus epithelial cells in mice and to a marked reduction in brain intraventricular fluid volume. This suggests that Ncbe functionally is a key element in vectorial Na+ transport and thereby for cerebrospinal fluid secretion in the choroid plexus. However, slc4a10 disruption results in severe changes in expression of Na+,K+-ATPase complexes and other major transport proteins, indicating that profound cellular changes accompany the genetic manipulation.MethodsA tandem mass tag labeling strategy was chosen for quantitative mass spectrometry. Alterations in the broader patterns of protein expression in the choroid plexus in response to genetic disruption of Ncbe was validated by semi-quantitative immunoblotting, immunohistochemistry and morphometry.ResultsThe abundance of 601 proteins were found significantly altered in the choroid plexus from Ncbe ko mice relative to Ncbe wt. In addition to a variety of transport proteins, particularly large changes in the abundance of proteins involved in cellular energy metabolism were detected in the Ncbe ko mice. In general, the abundance of rate limiting glycolytic enzymes and several mitochondrial enzymes were reduced following slc4a10 disruption. Surprisingly, this was accompanied by increased ATP levels in choroid plexus cells, indicating that the reduction in capacity for energy metabolism was adaptive to high ATP rather than causal for a decreased capacity for ion and water transport. Ncbe-deficient cells also had a reduced cell area and decreased K+ content.ConclusionOur findings suggest that the lack of effective Na+-entry into the epithelial cells of the choroid plexus leads to a profound change in the cellular phenotype, shifting from a high-rate secretory function towards a more dormant state; similar to what is observed during ageing or Alzheimer’s disease.
Highlights
Genetic disruption of slc4a10, which encodes the sodium-dependent chloride/bicarbonate exchanger sodium-dependent chloride bicarbonate exchanger (Ncbe), leads to a major decrease in Na+-dependent HCO3− import into choroid plexus epithelial cells in mice and to a marked reduction in brain intraventricular fluid volume
Ncbe ko greatly alters the general protein expression profile in the choroid plexus (CP) Mass spectrometry combined with a tandem mass tag (TMT) labeling strategy identified 1865 proteins in all 9 samples
601 were significantly changed in abundance in Ncbe ko CP (390 proteins increased, 211 proteins decreased). 340 proteins were increased in abundance by more than 10%, of which 86 were increased more than 25%
Summary
Genetic disruption of slc4a10, which encodes the sodium-dependent chloride/bicarbonate exchanger Ncbe, leads to a major decrease in Na+-dependent HCO3− import into choroid plexus epithelial cells in mice and to a marked reduction in brain intraventricular fluid volume. This suggests that Ncbe functionally is a key element in vectorial Na+ transport and thereby for cerebrospinal fluid secretion in the choroid plexus. A large fraction of the cerebrospinal fluid (CSF) is produced by the choroid plexus (CP) in the brain ventricles [1] At this site, the choroid plexus epithelial cells (CPECs) secrete solutes and water at very high rates that is not surpassed by other mammalian epithelia [2]. We have proposed Ncbe as a main candidate for the Na+ entry mechanism [12]
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