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   Cell Cycle Constraints and Environmental Control of Local DNA Hypomethylation in α-Proteobacteria  
   
نویسنده ardissone s. ,redder p. ,russo g. ,frandi a. ,fumeaux c. ,patrignani a. ,schlapbach r. ,falquet l. ,viollier p.h.
منبع plos genetics - 2016 - دوره : 12 - شماره : 12
چکیده    Heritable dna methylation imprints are ubiquitous and underlie genetic variability from bacteria to humans. in microbial genomes,dna methylation has been implicated in gene transcription,dna replication and repair,nucleoid segregation,transposition and virulence of pathogenic strains. despite the importance of local (hypo)methylation at specific loci,how and when these patterns are established during the cell cycle remains poorly characterized. taking advantage of the small genomes and the synchronizability of α-proteobacteria,we discovered that conserved determinants of the cell cycle transcriptional circuitry establish specific hypomethylation patterns in the cell cycle model system caulobacter crescentus. we used genome-wide methyl-n6-adenine (m6a-) analyses by restriction-enzyme-cleavage sequencing (rec-seq) and single-molecule real-time (smrt) sequencing to show that mucr,a transcriptional regulator that represses virulence and cell cycle genes in s-phase but no longer in g1-phase,occludes 5’-gantc-3’ sequence motifs that are methylated by the dna adenine methyltransferase ccrm. constitutive expression of ccrm or heterologous methylases in at least two different α-proteobacteria homogenizes m6a patterns even when mucr is present and affects promoter activity. environmental stress (phosphate limitation) can override and reconfigure local hypomethylation patterns imposed by the cell cycle circuitry that dictate when and where local hypomethylation is instated. © 2016 ardissone et al.
آدرس department of microbiology and molecular medicine,institute of genetics & genomics in geneva (ige3),faculty of medicine,university of geneva,geneva, Switzerland, department of microbiology and molecular medicine,institute of genetics & genomics in geneva (ige3),faculty of medicine,university of geneva,geneva,switzerland,lmgm,centre de biologie intégrative,université paul sabatier,toulouse, France, functional genomics center zurich,eth/university of zürich,zürich, Switzerland, department of microbiology and molecular medicine,institute of genetics & genomics in geneva (ige3),faculty of medicine,university of geneva,geneva,switzerland,department of fundamental microbiology,university of lausanne,lausanne, Switzerland, department of microbiology and molecular medicine,institute of genetics & genomics in geneva (ige3),faculty of medicine,university of geneva,geneva,switzerland,department of microbiology and immunobiology,harvard medical school,boston,ma, United States, functional genomics center zurich,eth/university of zürich,zürich, Switzerland, functional genomics center zurich,eth/university of zürich,zürich, Switzerland, biochemistry unit,dept. of biology,university of fribourg and swiss institute of bioinformatics,fribourg, Switzerland, department of microbiology and molecular medicine,institute of genetics & genomics in geneva (ige3),faculty of medicine,university of geneva,geneva, Switzerland
 
     
   
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