AI Article Synopsis

  • FGFRs play a significant role in brain development, with disruptions linked to schizophrenia and related disorders, as shown in a specific mouse model.
  • Changes in dopamine (DA) systems lead to increased serotonergic innervation, highlighting the interactions between DA and serotonin systems in neurodevelopment.
  • Behavioral impairments in the mouse model can be improved with atypical antipsychotics, suggesting potential therapeutic avenues for understanding and treating neurodevelopmental diseases like schizophrenia and autism.

Article Abstract

The role of fibroblast growth factor receptors (FGFR) in normal brain development has been well-documented in transgenic and knock-out mouse models. Changes in FGF and its receptors have also been observed in schizophrenia and related developmental disorders. The current study examines a transgenic th(tk-)/th(tk-) mouse model with FGF receptor signaling disruption targeted to dopamine (DA) neurons, resulting in neurodevelopmental, anatomical, and biochemical alterations similar to those observed in human schizophrenia. We show in th(tk-)/th(tk-) mice that hypoplastic development of DA systems induces serotonergic hyperinnervation of midbrain DA nuclei, demonstrating the co-developmental relationship between DA and 5-HT systems. Behaviorally, th(tk-)/th(tk-) mice displayed impaired sensory gaiting and reduced social interactions correctable by atypical antipsychotics (AAPD) and a specific 5-HT2A antagonist, M100907. The adult onset of neurochemical and behavioral deficits was consistent with the postpubertal time course of psychotic symptoms in schizophrenia and related disorders. The spectrum of abnormalities observed in th(tk-)/th(tk-) mice and the ability of AAPD to correct the behavioral deficits consistent with human psychosis suggests that midbrain 5-HT2A-controlling systems are important loci of therapeutic action. These results may provide further insight into the complex multi-neurotransmitter etiology of neurodevelopmental diseases such autism, bipolar disorder, Asperger's Syndrome and schizophrenia.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4681496PMC
http://dx.doi.org/10.1016/j.schres.2009.06.006DOI Listing

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