Cell Reports (Aug 2014)

CC2D1A Regulates Human Intellectual and Social Function as well as NF-κB Signaling Homeostasis

  • M. Chiara Manzini,
  • Lan Xiong,
  • Ranad Shaheen,
  • Dimira E. Tambunan,
  • Stefania Di Costanzo,
  • Vanessa Mitisalis,
  • David J. Tischfield,
  • Antonella Cinquino,
  • Mohammed Ghaziuddin,
  • Mehtab Christian,
  • Qin Jiang,
  • Sandra Laurent,
  • Zohair A. Nanjiani,
  • Saima Rasheed,
  • R. Sean Hill,
  • Sofia B. Lizarraga,
  • Danielle Gleason,
  • Diya Sabbagh,
  • Mustafa A. Salih,
  • Fowzan S. Alkuraya,
  • Christopher A. Walsh

DOI
https://doi.org/10.1016/j.celrep.2014.06.039
Journal volume & issue
Vol. 8, no. 3
pp. 647 – 655

Abstract

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Autism spectrum disorder (ASD) and intellectual disability (ID) are often comorbid, but the extent to which they share common genetic causes remains controversial. Here, we present two autosomal-recessive “founder” mutations in the CC2D1A gene causing fully penetrant cognitive phenotypes, including mild-to-severe ID, ASD, as well as seizures, suggesting shared developmental mechanisms. CC2D1A regulates multiple intracellular signaling pathways, and we found its strongest effect to be on the transcription factor nuclear factor κB (NF-κB). Cc2d1a gain and loss of function both increase activation of NF-κB, revealing a critical role of Cc2d1a in homeostatic control of intracellular signaling. Cc2d1a knockdown in neurons reduces dendritic complexity and increases NF-κB activity, and the effects of Cc2d1a depletion can be rescued by inhibiting NF-κB activity. Homeostatic regulation of neuronal signaling pathways provides a mechanism whereby common founder mutations could manifest diverse symptoms in different patients.