Radically truncated MeCP2 rescues Rett syndrome-like neurological defects

Tillotson, Rebekah; Selfridge, Jim; Koerner, Martha V.; Gadalla, Kamal K.E.; Guy, Jacky; Sousa, Diana De; Hector, Ralph D.; Cobb, Stuart; Bird, Adrian

doi:10.1038/nature24058

Cited by 129 publications

(125 citation statements)

References 37 publications

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“…The key function of MeCP2 is to form a bridge between methylated DNA and the NCOR1/2 corepressor complexes, dependent on the MBD and NID (NCOR1/2 Interaction Domain), respectively (Guy et al, 2018;Kruusvee et al, 2017;Lyst et al, 2013;Tillotson et al, 2017).…”

Section: A Chimeric Mecp2 That Selectively Binds Mcgmentioning

confidence: 99%

Neuronal non-CG methylation is an essential target for MeCP2 function

Tillotson

Cholewa-Waclaw

Chhatbar

et al. 2020

Preprint

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SUMMARYDNA methylation is implicated in neuronal biology via the protein MeCP2, mutation of which causes Rett syndrome. MeCP2 recruits the NCOR1/2 corepressor complexes to methylated cytosine in the CG dinucleotide, but also to non-CG methylation, which is abundant specifically in neuronal genomes. To test the biological significance of its dual binding specificity, we replaced the MeCP2 DNA binding domain with an orthologous domain whose specificity is restricted to mCG motifs. Knock-in mice expressing the domain-swap protein displayed severe Rett syndrome-like phenotypes, demonstrating that interaction with sites of non-CG methylation, specifically the mCAC trinucleotide, is critical for normal brain function. The results support the notion that the delayed onset of Rett syndrome is due to the late accumulation of both mCAC and its reader MeCP2. Intriguingly, genes dysregulated in both Mecp2-null and domain-swap mice are implicated in other neurological disorders, potentially highlighting targets of particular relevance to the Rett syndrome phenotype.

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Section: A Chimeric Mecp2 That Selectively Binds Mcgmentioning

confidence: 99%

Neuronal non-CG methylation is an essential target for MeCP2 function

Tillotson

Cholewa-Waclaw

Chhatbar

et al. 2020

Preprint

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“…Several functional domains have been identified previously in MeCP2 and shown to play important roles in vivo and in vitro (Baker et al, 2013;Ghosh et al, 2010b;Heckman et al, 2014;Tillotson et al, 2017). Here we have examined the contributions of these domains to the dynamic behavior of single MeCP2 molecules in live granule cell nuclei, revealing several interesting features of MeCP2 that have not been reported previously.…”

Section: Different Aspects Of Mecp2 Dynamic Behavior Are Governed By mentioning

confidence: 77%

MeCP2 nuclear dynamics in live neurons results from low and high affinity chromatin interactions

Piccolo

Liu

Dong

et al. 2019

Preprint

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Loss of function mutations in Methyl-CpGbinding Protein 2 (MeCP2) cause the severe neurological disorder Rett Syndrome. MeCP2 is a highly abundant nuclear protein particularly enriched in neurons. Although biochemical and genomic analyses of MeCP2-DNA interaction and genomic distribution demonstrate that MeCP2 binding on chromatin is dependent on DNA modification state, the dynamic behavior of individual MeCP2 proteins in live neurons has not been explored. Here we use live-cell singlemolecule imaging to assess the detailed kinetic features of MeCP2 in distinct sub-nuclear regions at high spatial and temporal resolution. Surprisingly, we found that, in granule cell nuclei, MeCP2 has unique diffusion and chromatin binding kinetics that are distinct from highly mobile sequence-specific transcription factors (TF) and immobile histone proteins. Approximately, half of MeCP2 is bound to DNA in a transiently stable mode that is similar to TF binding to their cognate sites. The binding of meCP2 to DNA requires its methyl-binding domain (MBD) and is sensitive to the levels of both DNA methylation and hydroxymethylation. However, when not stably bound, MeCP2 moves slowly in the nucleus most closely resembling histone H1.0. The rate of MeCP2 diffusion in compact, granule cell nuclei is determined by weak, transient DNA interactions mediated primarily by the MBD and three AT-hook domains located in the C-terminal portion of the protein. Both the fraction of stably bound MeCP2 and its rate of diffusion depend on the level of chromatin compaction and neuronal cell type.Our data reveal new features of MeCP2 that dictate its dynamic behavior in neuronal nuclei and suggest that the limited nuclear diffusion of MeCP2 in live neurons may contribute to its local impact on chromatin structure and gene expression.

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“…Our data raise the possibility that aspects of the CdLS phenotype may be reversible by postnatal intervention. Precedent for such rescue comes from pioneering studies in mouse models of Rett syndrome, where postnatal correction of Mecp2 deficiency ameliorates deregulated gene expression and behavioural defects 22,23 . As the Rett protein MECP2, cohesin exerts its effects on transcription by interfacing with chromatin marking systems 44 , and the dynamics of cohesin on chromatin is controlled in part by acetylation and deacetylation of its SMC subunits 45 .…”

Section: Discussionmentioning

confidence: 99%

“…Postnatal intervention can alleviate transcriptional changes and abnormal behaviours in mouse models of Rett Syndrome 22,23 . In light of these results, we asked whether gene expression changes induced by acute cohesin depletion in Rad21 Tev/Tev neurons can be reversed when cohesin levels are restored.…”

Section: Rescue Of Cohesin-dependent Gene Expressionmentioning

confidence: 99%

“…However, these studies have been unable to discern whether these changes are the result of cohesin deficiency during development, or reflect an ongoing requirement for cohesin in mature neurons. This is of interest, as mouse models of neurodevelopmental syndromes such as Rett Syndrome can benefit from postnatal interventions that correct aberrant gene expression and animal behaviour 22,23 . Although aberrant gene expression is a likely cause of neuronal dysfunction in CdLS, studies of gene expression in CdLS patient cells have to date been limited to induced pluripotent stem cells (iPSCs) 24 , cardiac 24 and lymphoblastoid cells 25 .…”

Section: Introductionmentioning

confidence: 99%

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Partial rescue of neuronal genes deregulated in Cornelia de Lange Syndrome by cohesin

Weiss

Calderón

Wang

et al. 2020

Preprint

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Cornelia de Lange Syndrome (CdLS) is a human developmental disorder caused by mutations that compromise the function of cohesin, a major regulator of 3D genome organization. Cognitive impairment is a universal and as yet unexplained feature of CdLS. We characterized the transcriptional profile of cortical neurons from CdLS patients and found deregulation of hundreds of genes enriched for neuronal functions related to synaptic transmission, signalling processes, learning and behaviour. Inducible proteolytic cleavage of cohesin disrupted 3-D genome organization and transcriptional control in post-mitotic cortical mouse neurons. The genes affected belonged to similar gene ontology classes and showed significant numerical overlap with those deregulated in CdLS. Interestingly, gene expression was largely rescued by subsequent reconstitution of cohesin function. These experiments show that cohesin is continuously required for neuronal gene expression and provide a tractable approach for addressing mechanisms of neuronal dysfunction in CdLS.

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Radically truncated MeCP2 rescues Rett syndrome-like neurological defects

Cited by 129 publications

References 37 publications

Neuronal non-CG methylation is an essential target for MeCP2 function

Neuronal non-CG methylation is an essential target for MeCP2 function

MeCP2 nuclear dynamics in live neurons results from low and high affinity chromatin interactions

Partial rescue of neuronal genes deregulated in Cornelia de Lange Syndrome by cohesin

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