MeCP2 gates spatial learning-induced alternative splicing events in the mouse hippocampus

MeCP2 gates spatial learning-induced alternative splicing events in the mouse hippocampus

Abstract Long-term memory formation is supported by functional and structural changes of neuronal networks, which rely on de novo gene transcription and protein synthesis. The modulation of the neuronal transcriptome in response to learning depends on transcriptional and post-transcriptional mechani...

Full description

Bibliographic Details
Main Authors: David V. C. Brito, Kubra Gulmez Karaca, Janina Kupke, Lukas Frank, Ana M. M. Oliveira
Format: Article
Language:English
Published: BMC 2020-11-01
Series:Molecular Brain
Subjects:
Alternative splicing
Adult brain
DNA methylation
Gene transcription
Rett syndrome
RNA sequencing
Online Access:http://link.springer.com/article/10.1186/s13041-020-00695-1
id doaj-1b27d872b3f64110b962b2b2b61b159c
record_format Article
spelling doaj-1b27d872b3f64110b962b2b2b61b159c2020-11-25T04:03:18ZengBMCMolecular Brain1756-66062020-11-0113111610.1186/s13041-020-00695-1MeCP2 gates spatial learning-induced alternative splicing events in the mouse hippocampusDavid V. C. Brito0Kubra Gulmez Karaca1Janina Kupke2Lukas Frank3Ana M. M. Oliveira4Department of Neurobiology, Interdisciplinary Centre for Neurosciences (IZN), Heidelberg UniversityDepartment of Neurobiology, Interdisciplinary Centre for Neurosciences (IZN), Heidelberg UniversityDepartment of Neurobiology, Interdisciplinary Centre for Neurosciences (IZN), Heidelberg UniversityDivision of Chromatin Networks, German Cancer Research Center (DKFZ) and Bioquant (Heidelberg University)Department of Neurobiology, Interdisciplinary Centre for Neurosciences (IZN), Heidelberg UniversityAbstract Long-term memory formation is supported by functional and structural changes of neuronal networks, which rely on de novo gene transcription and protein synthesis. The modulation of the neuronal transcriptome in response to learning depends on transcriptional and post-transcriptional mechanisms. DNA methylation writers and readers regulate the activity-dependent genomic program required for memory consolidation. The most abundant DNA methylation reader, the Methyl CpG binding domain protein 2 (MeCP2), has been shown to regulate alternative splicing, but whether it establishes splicing events important for memory consolidation has not been investigated. In this study, we identified the alternative splicing profile of the mouse hippocampus in basal conditions and after a spatial learning experience, and investigated the requirement of MeCP2 for these processes. We observed that spatial learning triggers a wide-range of alternative splicing events in transcripts associated with structural and functional remodeling and that virus-mediated knockdown of MeCP2 impairs learning-dependent post-transcriptional responses of mature hippocampal neurons. Furthermore, we found that MeCP2 preferentially affected the splicing modalities intron retention and exon skipping and guided the alternative splicing of distinct set of genes in baseline conditions and after learning. Lastly, comparative analysis of the MeCP2-regulated transcriptome with the alternatively spliced mRNA pool, revealed that MeCP2 disruption alters the relative abundance of alternatively spliced isoforms without affecting the overall mRNA levels. Taken together, our findings reveal that adult hippocampal MeCP2 is required to finetune alternative splicing events in basal conditions, as well as in response to spatial learning. This study provides new insight into how MeCP2 regulates brain function, particularly cognitive abilities, and sheds light onto the pathophysiological mechanisms of Rett syndrome, that is characterized by intellectual disability and caused by mutations in the Mecp2 gene.http://link.springer.com/article/10.1186/s13041-020-00695-1Alternative splicingAdult brainDNA methylationGene transcriptionRett syndromeRNA sequencing
collection DOAJ
language English
format Article
sources DOAJ
author David V. C. Brito
Kubra Gulmez Karaca
Janina Kupke
Lukas Frank
Ana M. M. Oliveira
spellingShingle David V. C. Brito
Kubra Gulmez Karaca
Janina Kupke
Lukas Frank
Ana M. M. Oliveira
MeCP2 gates spatial learning-induced alternative splicing events in the mouse hippocampus
Molecular Brain
Alternative splicing
Adult brain
DNA methylation
Gene transcription
Rett syndrome
RNA sequencing
author_facet David V. C. Brito
Kubra Gulmez Karaca
Janina Kupke
Lukas Frank
Ana M. M. Oliveira
author_sort David V. C. Brito
title MeCP2 gates spatial learning-induced alternative splicing events in the mouse hippocampus
title_short MeCP2 gates spatial learning-induced alternative splicing events in the mouse hippocampus
title_full MeCP2 gates spatial learning-induced alternative splicing events in the mouse hippocampus
title_fullStr MeCP2 gates spatial learning-induced alternative splicing events in the mouse hippocampus
title_full_unstemmed MeCP2 gates spatial learning-induced alternative splicing events in the mouse hippocampus
title_sort mecp2 gates spatial learning-induced alternative splicing events in the mouse hippocampus
publisher BMC
series Molecular Brain
issn 1756-6606
publishDate 2020-11-01
description Abstract Long-term memory formation is supported by functional and structural changes of neuronal networks, which rely on de novo gene transcription and protein synthesis. The modulation of the neuronal transcriptome in response to learning depends on transcriptional and post-transcriptional mechanisms. DNA methylation writers and readers regulate the activity-dependent genomic program required for memory consolidation. The most abundant DNA methylation reader, the Methyl CpG binding domain protein 2 (MeCP2), has been shown to regulate alternative splicing, but whether it establishes splicing events important for memory consolidation has not been investigated. In this study, we identified the alternative splicing profile of the mouse hippocampus in basal conditions and after a spatial learning experience, and investigated the requirement of MeCP2 for these processes. We observed that spatial learning triggers a wide-range of alternative splicing events in transcripts associated with structural and functional remodeling and that virus-mediated knockdown of MeCP2 impairs learning-dependent post-transcriptional responses of mature hippocampal neurons. Furthermore, we found that MeCP2 preferentially affected the splicing modalities intron retention and exon skipping and guided the alternative splicing of distinct set of genes in baseline conditions and after learning. Lastly, comparative analysis of the MeCP2-regulated transcriptome with the alternatively spliced mRNA pool, revealed that MeCP2 disruption alters the relative abundance of alternatively spliced isoforms without affecting the overall mRNA levels. Taken together, our findings reveal that adult hippocampal MeCP2 is required to finetune alternative splicing events in basal conditions, as well as in response to spatial learning. This study provides new insight into how MeCP2 regulates brain function, particularly cognitive abilities, and sheds light onto the pathophysiological mechanisms of Rett syndrome, that is characterized by intellectual disability and caused by mutations in the Mecp2 gene.
topic Alternative splicing
Adult brain
DNA methylation
Gene transcription
Rett syndrome
RNA sequencing
url http://link.springer.com/article/10.1186/s13041-020-00695-1
work_keys_str_mv AT davidvcbrito mecp2gatesspatiallearninginducedalternativesplicingeventsinthemousehippocampus
AT kubragulmezkaraca mecp2gatesspatiallearninginducedalternativesplicingeventsinthemousehippocampus
AT janinakupke mecp2gatesspatiallearninginducedalternativesplicingeventsinthemousehippocampus
AT lukasfrank mecp2gatesspatiallearninginducedalternativesplicingeventsinthemousehippocampus
AT anammoliveira mecp2gatesspatiallearninginducedalternativesplicingeventsinthemousehippocampus
_version_ 1724440747338366976

Similar Items