Female mice lacking Ftx lncRNA exhibit impaired X-chromosome inactivation and a microphthalmia-like phenotype.
Yusuke HosoiMiki SomaHirosuke ShiuraTakashi SadoHidetoshi HasuwaKuniya AbeTakashi KohdaFumitoshi IshinoShin KobayashiPublished in: Nature communications (2018)
X-chromosome inactivation (XCI) is an essential epigenetic process in female mammalian development. Although cell-based studies suggest the potential importance of the Ftx long non-protein-coding RNA (lncRNA) in XCI, its physiological roles in vivo remain unclear. Here we show that targeted deletion of X-linked mouse Ftx lncRNA causes eye abnormalities resembling human microphthalmia in a subset of females but rarely in males. This inheritance pattern cannot be explained by X-linked dominant or recessive inheritance, where males typically show a more severe phenotype than females. In Ftx-deficient mice, some X-linked genes remain active on the inactive X, suggesting that defects in random XCI in somatic cells cause a substantially female-specific phenotype. The expression level of Xist, a master regulator of XCI, is diminished in females homozygous or heterozygous for Ftx deficiency. We propose that loss-of-Ftx lncRNA abolishes gene silencing on the inactive X chromosome, leading to a female microphthalmia-like phenotype.
Keyphrases
- copy number
- long non coding rna
- mitochondrial dna
- long noncoding rna
- poor prognosis
- early onset
- endothelial cells
- induced apoptosis
- genome wide
- transcription factor
- single cell
- type diabetes
- binding protein
- signaling pathway
- cancer therapy
- small molecule
- drug delivery
- oxidative stress
- autism spectrum disorder
- mesenchymal stem cells
- induced pluripotent stem cells
- protein protein
- climate change
- endoplasmic reticulum stress
- genome wide analysis