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Synthetic reversed sequences reveal default genomic states
by
Camellato, Brendan R
, Maurano, Matthew T
, Boeke, Jef D
, Brosh, Ran
, Ashe, Hannah J
in
Ablation
/ Biological activity
/ Biological evolution
/ Chromatin
/ CpG islands
/ Embryo cells
/ Genes
/ Genomes
/ Genomics
/ Horizontal transfer
/ Regulatory sequences
/ Species diversity
/ Stem cells
/ Transcription
/ X chromosomes
/ Yeast
2024
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Synthetic reversed sequences reveal default genomic states
by
Camellato, Brendan R
, Maurano, Matthew T
, Boeke, Jef D
, Brosh, Ran
, Ashe, Hannah J
in
Ablation
/ Biological activity
/ Biological evolution
/ Chromatin
/ CpG islands
/ Embryo cells
/ Genes
/ Genomes
/ Genomics
/ Horizontal transfer
/ Regulatory sequences
/ Species diversity
/ Stem cells
/ Transcription
/ X chromosomes
/ Yeast
2024
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
Synthetic reversed sequences reveal default genomic states
by
Camellato, Brendan R
, Maurano, Matthew T
, Boeke, Jef D
, Brosh, Ran
, Ashe, Hannah J
in
Ablation
/ Biological activity
/ Biological evolution
/ Chromatin
/ CpG islands
/ Embryo cells
/ Genes
/ Genomes
/ Genomics
/ Horizontal transfer
/ Regulatory sequences
/ Species diversity
/ Stem cells
/ Transcription
/ X chromosomes
/ Yeast
2024
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Synthetic reversed sequences reveal default genomic states
Journal Article
Synthetic reversed sequences reveal default genomic states
2024
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Overview
Pervasive transcriptional activity is observed across diverse species. The genomes of extant organisms have undergone billions of years of evolution, making it unclear whether these genomic activities represent effects of selection or 'noise'14. Characterizing default genome states could help understand whether pervasive transcriptional activity has biological meaning. Here we addressed this question by introducing a synthetic 101-kb locus into the genomes of Saccharomyces cereuisiae and Mus musculus and characterizing genomic activity. The locus was designed by reversing but not complementing human HPRT1, including its flanking regions, thus retaining basic features of the natural sequence but ablating evolved coding or regulatory information. We observed widespread activity of both reversed and native HPRT1 loci in yeast, despite the lack of evolved yeast promoters. By contrast, the reversed locus displayed no activity at all in mouse embryonic stem cells, and instead exhibited repressive chromatin signatures. The repressive signature was alleviated in a locus variant lacking CpG dinucleotides; nevertheless, this variant was also transcriptionally inactive. These results show that synthetic genomic sequences that lack coding information are active in yeast, but inactive in mouse embryonic stem cells, consistent with a major difference in 'default genomic states' between these two divergent eukaryotic cell types, with implications for understanding pervasive transcription, horizontal transfer of genetic information and the birth of new genes.
Publisher
Nature Publishing Group
Subject
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