| Literature DB >> 33318149 |
Mark Perfetto1,2, Xiaolu Xu1, Congyu Lu1, Yu Shi1, Natasha Yousaf2, Jiejing Li2,3, Yvette Y Yien1, Shuo Wei4.
Abstract
Mutations in the RNA helicase DDX3 have emerged as a frequent cause of intellectual disability in humans. Because many individuals carrying DDX3 mutations have additional defects in craniofacial structures and other tissues containing neural crest (NC)-derived cells, we hypothesized that DDX3 is also important for NC development. Using Xenopus tropicalis as a model, we show that DDX3 is required for normal NC induction and craniofacial morphogenesis by regulating AKT kinase activity. Depletion of DDX3 decreases AKT activity and AKT-dependent inhibitory phosphorylation of GSK3β, leading to reduced levels of β-catenin and Snai1: two GSK3β substrates that are crucial for NC induction. DDX3 function in regulating these downstream signaling events during NC induction is likely mediated by RAC1, a small GTPase whose translation depends on the RNA helicase activity of DDX3. These results suggest an evolutionarily conserved role of DDX3 in NC development by promoting AKT activity, and provide a potential mechanism for the NC-related birth defects displayed by individuals harboring mutations in DDX3 and its downstream effectors in this signaling cascade.Entities:
Keywords: AKT; DDX3; GSK3β; Neural crest (NC); Wnt signaling; Xenopus
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Year: 2021 PMID: 33318149 PMCID: PMC7847268 DOI: 10.1242/dev.184341
Source DB: PubMed Journal: Development ISSN: 0950-1991 Impact factor: 6.862