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Publication : Gsx1 expression defines neurons required for prepulse inhibition.

First Author  Bergeron SA Year  2015
Journal  Mol Psychiatry Volume  20
Issue  8 Pages  974-85
PubMed ID  25224259 Mgi Jnum  J:315112
Mgi Id  MGI:6829219 Doi  10.1038/mp.2014.106
Citation  Bergeron SA, et al. (2015) Gsx1 expression defines neurons required for prepulse inhibition. Mol Psychiatry 20(8):974-85
abstractText  In schizophrenia, cognitive overload is thought to reflect an inability to suppress non-salient information, a process which is studied using prepulse inhibition (PPI) of the startle response. PPI is reduced in schizophrenia and routinely tested in animal models and preclinical trials of antipsychotic drugs. However, the underlying neuronal circuitry is not well understood. We used a novel genetic screen in larval zebrafish to reveal the molecular identity of neurons that are required for PPI in fish and mice. Ablation or optogenetic silencing of neurons with developmental expression of the transcription factor genomic screen homeobox 1 (gsx1) produced profound defects in PPI in zebrafish, and PPI was similarly impaired in Gsx1 knockout mice. Gsx1-expressing neurons reside in the dorsal brainstem and form synapses closely apposed to neurons that initiate the startle response. Surprisingly, brainstem Gsx1 neurons are primarily glutamatergic despite their role in a functionally inhibitory pathway. As Gsx1 has an important role in regulating interneuron development in the forebrain, these findings reveal a molecular link between control of interneuron specification and circuits that gate sensory information across brain regions.
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