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Publication : Centrosomal protein FOR20 knockout mice display embryonic lethality and left-right patterning defects.

First Author  Xu Z Year  2021
Journal  FEBS Lett Volume  595
Issue  10 Pages  1462-1472
PubMed ID  33686659 Mgi Jnum  J:308526
Mgi Id  MGI:6729778 Doi  10.1002/1873-3468.14071
Citation  Xu Z, et al. (2021) Centrosomal protein FOR20 knockout mice display embryonic lethality and left-right patterning defects. FEBS Lett 595(10):1462-1472
abstractText  Centrosomal protein FOR20 has been reported to be crucial for essential cellular processes, including ciliogenesis, cell migration, and cell cycle in vertebrates. However, the function of FOR20 during mammalian embryonic development remains unknown. To investigate the in vivo function of the For20 gene in mammals, we generated For20 homozygous knockout mice by gene targeting. Our data reveal that homozygous knockout of For20 results in significant embryonic growth arrest and lethality during gestation, while the heterozygotes show no obvious defects. The absence of For20 leads to impaired left-right patterning of embryos and reduced cilia in the embryonic node. Deletion of For20 also disrupts angiogenesis in yolk sacs and embryos. These results highlight a critical role of For20 in early mammalian embryogenesis.
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