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Mutations in the gene encoding the methyl-CG binding protein MeCP2 cause several neurological disorders including Rett syndrome. The di-nucleotide methyl-CG (mCG) is the classical MeCP2 DNA recognition sequence, but additional methylated sequence targets have been reported. Here we show by in vitro and in vivo analyses that MeCP2 binding to non-CG methylated sites in brain is largely confined to the tri-nucleotide sequence mCAC. MeCP2 binding to chromosomal DNA in mouse brain is proportional to mCAC + mCG density and unexpectedly defines large genomic domains within which transcription is sensitive to MeCP2 occupancy. Our results suggest that MeCP2 integrates patterns of mCAC and mCG in the brain to restrain transcription of genes critical for neuronal function.

MeCP2 recognizes cytosine methylated tri-nucleotide and di-nucleotide sequences to tune transcription in the mammalian brain / Lagger, S.; Connelly, J. C.; Schweikert, G.; Webb, S.; Selfridge, J.; Ramsahoye, B. H.; Yu, M.; He, C.; Sanguinetti, G.; Sowers, L. C.; Walkinshaw, M. D.; Bird, A.. - In: PLOS GENETICS. - ISSN 1553-7404. - 13:5(2017), pp. 1-26. [10.1371/journal.pgen.1006793]

MeCP2 recognizes cytosine methylated tri-nucleotide and di-nucleotide sequences to tune transcription in the mammalian brain

Lagger, S.;Connelly, J. C.;Schweikert, G.;Webb, S.;Selfridge, J.;Ramsahoye, B. H.;Yu, M.;He, C.;Sanguinetti, G.;Sowers, L. C.;Walkinshaw, M. D.;Bird, A.

2017-01-01

Abstract

Mutations in the gene encoding the methyl-CG binding protein MeCP2 cause several neurological disorders including Rett syndrome. The di-nucleotide methyl-CG (mCG) is the classical MeCP2 DNA recognition sequence, but additional methylated sequence targets have been reported. Here we show by in vitro and in vivo analyses that MeCP2 binding to non-CG methylated sites in brain is largely confined to the tri-nucleotide sequence mCAC. MeCP2 binding to chromosomal DNA in mouse brain is proportional to mCAC + mCG density and unexpectedly defines large genomic domains within which transcription is sensitive to MeCP2 occupancy. Our results suggest that MeCP2 integrates patterns of mCAC and mCG in the brain to restrain transcription of genes critical for neuronal function.

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	Anno
	
			2017
		
	Rivista
	
			PLOS GENETICS
		
	Numero del volume
	
			13
		
	Fascicolo
	
			5
		
	Da pagina
	
			1
		
	A pagina
	
			26
		
	Numero di articolo
	
			e1006793
		
	Codice DOI
	
			https://dx.doi.org/10.1371/journal.pgen.1006793
		
	Tutti gli autori
	
			Lagger, S.; Connelly, J. C.; Schweikert, G.; Webb, S.; Selfridge, J.; Ramsahoye, B. H.; Yu, M.; He, C.; Sanguinetti, G.; Sowers, L. C.; Walkinshaw, M. D.; Bird, A.
		
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			1.1 Journal article

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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/20.500.11767/117327

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