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. 2023 Aug 15;94(4):341-351.
doi: 10.1016/j.biopsych.2023.03.010. Epub 2023 Mar 22.

Pathogenic Mis-splicing of CPEB4 in Schizophrenia

Ivana Ollà  1 Antonio F Pardiñas  2 Alberto Parras  1 Ivó H Hernández  1 María Santos-Galindo  1 Sara Picó  1 Luis F Callado  3 Ainara Elorza  1 Claudia Rodríguez-López  1 Gonzalo Fernández-Miranda  4 Eulàlia Belloc  4 James T R Walters  2 Michael C O'Donovan  2 Raúl Méndez  5 Claudio Toma  6 J Javier Meana  3 Michael J Owen  2 José J Lucas  7
Affiliations
Free article

Pathogenic Mis-splicing of CPEB4 in Schizophrenia

Ivana Ollà et al. Biol Psychiatry. .
Free article

Abstract

Background: Schizophrenia (SCZ) is caused by an interplay of polygenic risk and environmental factors, which may alter regulators of gene expression leading to pathogenic misexpression of SCZ risk genes. The CPEB family of RNA-binding proteins (CPEB1-4) regulates translation of target RNAs (approximately 40% of overall genes). We previously identified CPEB4 as a key dysregulated translational regulator in autism spectrum disorder (ASD) because its neuronal-specific microexon (exon 4) is mis-spliced in ASD brains, causing underexpression of numerous ASD risk genes. The genetic factors and pathogenic mechanisms shared between SCZ and ASD led us to hypothesize CPEB4 mis-splicing in SCZ leading to underexpression of multiple SCZ-related genes.

Methods: We performed MAGMA-enrichment analysis on Psychiatric Genomics Consortium genome-wide association study data and analyzed RNA sequencing data from the PsychENCODE Consortium. Reverse transcriptase polymerase chain reaction and Western blot were performed on postmortem brain tissue, and the presence/absence of antipsychotics was assessed through toxicological analysis. Finally, mice with mild overexpression of exon 4-lacking CPEB4 (CPEB4Δ4) were generated and analyzed biochemically and behaviorally.

Results: First, we found enrichment of SCZ-associated genes for CPEB4-binder transcripts. We also found decreased usage of CPEB4 microexon in SCZ probands, which was correlated with decreased protein levels of CPEB4-target SCZ-associated genes only in antipsychotic-free individuals. Interestingly, differentially expressed genes fit those reported for SCZ, specifically in the SCZ probands with decreased CPEB4-microexon inclusion. Finally, we demonstrated that mice with mild overexpression of CPEB4Δ4 showed decreased protein levels of CPEB4-target SCZ genes and SCZ-linked behaviors.

Conclusions: We identified aberrant CPEB4 splicing and downstream misexpression of SCZ risk genes as a novel etiological mechanism in SCZ.

Keywords: CPEB; GWAS; Microexon; Mouse model; RNA-binding protein; Splicing.

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