X-chromosome upregulation is driven by increased burst frequency

Ohno's hypothesis postulates that upregulation of X-linked genes rectifies their dosage imbalance relative to autosomal genes, which are present in two active copies per cell. Here we have dissected X-chromosome upregulation into the kinetics of transcription, inferred from allele-specific sing...

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Veröffentlicht in:Nature structural & molecular biology 2019-10, Vol.26 (10), p.963-969
Hauptverfasser: Larsson, Anton J. M., Coucoravas, Christos, Sandberg, Rickard, Reinius, Björn
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Sprache:eng
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Zusammenfassung:Ohno's hypothesis postulates that upregulation of X-linked genes rectifies their dosage imbalance relative to autosomal genes, which are present in two active copies per cell. Here we have dissected X-chromosome upregulation into the kinetics of transcription, inferred from allele-specific single-cell RNA sequencing data from somatic and embryonic mouse cells. We confirmed increased X-chromosome expression levels in female and male cells and found that the X chromosome achieved upregulation by elevated burst frequencies. By monitoring transcriptional kinetics in differentiating female mouse embryonic stem cells, we found that increased burst frequency was established on the active X chromosome when X inactivation took place on the other allele. Thus, our study provides mechanistic insights into X-chromosome upregulation. Analysis of X-chromosome upregulation using single-cell transcriptional kinetics data reveals increased burst frequency of X-linked genes that appear on the active X chromosome when X inactivation takes place.
ISSN:1545-9993
1545-9985
1545-9985
DOI:10.1038/s41594-019-0306-y