Translational Psychiatry (Feb 2021)

A unique missense variant in the E1A-binding protein P400 gene is implicated in schizophrenia by whole-exome sequencing and mutant mouse models

  • Yoshiro Morimoto,
  • Shinji Ono,
  • Shintaro Yoshida,
  • Hiroyuki Mishima,
  • Akira Kinoshita,
  • Takeshi Tanaka,
  • Yoshihiro Komohara,
  • Naohiro Kurotaki,
  • Tatsuya Kishino,
  • Yuji Okazaki,
  • Hiroki Ozawa,
  • Koh-ichiro Yoshiura,
  • Akira Imamura

DOI
https://doi.org/10.1038/s41398-021-01258-1
Journal volume & issue
Vol. 11, no. 1
pp. 1 – 12

Abstract

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Abstract Genetic and epidemiological evidence has suggested that genetic factors are important in schizophrenia, although its pathophysiology is poorly understood. This study used whole-exome sequencing to investigate potential novel schizophrenia-causing genes in a Japanese family containing several members affected by severe or treatment-resistant schizophrenia. A missense variant, chr12:132064747C>T (rs200626129, P2805L), in the E1A-binding protein P400 (EP400) gene completely segregated with schizophrenia in this family. Furthermore, numerous other EP400 mutations were identified in the targeted sequencing of a schizophrenia patient cohort. We also created two lines of Ep400 gene-edited mice, which had anxiety-like behaviours and reduced axon diameters. Our findings suggest that rs200626129 in EP400 is likely to cause schizophrenia in this Japanese family, and may lead to a better understanding and treatment of schizophrenia.