Abstract
BackgroundRett syndrome is best known due to its severe and devastating symptoms in the central nervous system. It is produced by mutations affecting the Mecp2 gene that codes for a transcription factor. Nevertheless, evidence for MECP2 activity has been reported for tissues other than those of the central nervous system. Patients affected by Rett presented with intestinal affections whose origin is still not known. We have observed that the Mecp2-null mice presented with episodes of diarrhea, and decided to study the intestinal phenotype in these mice.Methods Mecp2-null mice or bearing the conditional intestinal deletion of MECP2 were used. Morphometirc and histologic analysis of intestine, and RT-PCR, western blot and immunodetection were perfomed on intestinal samples of the animals. Electrical parameters of the intestine were determined by Ussing chamber experiments in freshly isolated colon samples.ResultsFirst we determined that MECP2 protein is mainly expressed in cells of the lower part of the colonic crypts and not in the small intestine. The colon of the Mecp2-null mice was shorter than that of the wild-type. Histological analysis showed that epithelial cells of the surface have abnormal localization of key membrane proteins like ClC-2 and NHE-3 that participate in the electroneutral NaCl absorption; nevertheless, electrogenic secretion and absorption remain unaltered. We also detected an increase in a proliferation marker in the crypts of the colon samples of the Mecp2-null mice, but the specific silencing of Mecp2 from intestinal epithelium was not able to recapitulate the intestinal phenotype of the Mecp2-null mice.ConclusionsIn summary, we showed that the colon is severely affected by Mecp2 silencing in mice. Changes in colon length and epithelial histology are similar to those observed in colitis. Changes in the localization of proteins that participate in fluid absorption can explain watery stools, but the exclusive deletion of Mecp2 from the intestine did not reproduce colon changes observed in the Mecp2-null mice, indicating the participation of other cells in this phenotype and the complex interaction between different cell types in this disease.Electronic supplementary materialThe online version of this article (doi:10.1186/s40348-016-0065-3) contains supplementary material, which is available to authorized users.
Highlights
Rett syndrome is best known due to its severe and devastating symptoms in the central nervous system
After we described the effects of methyl-CpG binding protein 2 (MECP2) absence in the colon, we questioned if using the Cre-loxP system the sole deletion of Mecp2 from intestinal epithelium was sufficient to reproduce the intestinal phenotype of the Mecp2-null mouse
In summary, we have described for the first time the effects of Mecp2 silencing on mouse intestine
Summary
Rett syndrome is best known due to its severe and devastating symptoms in the central nervous system. It is produced by mutations affecting the Mecp gene that codes for a transcription factor. Evidence for MECP2 activity has been reported for tissues other than those of the central nervous system. Patients affected by Rett presented with intestinal affections whose origin is still not known. Rett syndrome (RTT) is a devastating neurodevelopmental disorder affecting mainly girls since their early childhood. The major cause of RTT are mutations affecting the methyl-CpG binding protein 2 (MECP2) coding gene [1]. RTT patients have a high incidence of symptoms affecting the lower section of the gastrointestinal tract like
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