FoxP1 orchestration of ASD-relevant signaling pathways in the striatum

Author:

Araujo Daniel J.,Anderson Ashley G.,Berto Stefano,Runnels Wesley,Harper Matthew,Ammanuel Simon,Rieger Michael A.,Huang Hung-Chung,Rajkovich Kacey,Loerwald Kristofer W.,Dekker Joseph D.,Tucker Haley O.,Dougherty Joseph D.,Gibson Jay R.,Konopka Genevieve

Abstract

Mutations in the transcription factor Forkhead box p1 (FOXP1) are causative for neurodevelopmental disorders such as autism. However, the function of FOXP1 within the brain remains largely uncharacterized. Here, we identify the gene expression program regulated by FoxP1 in both human neural cells and patient-relevant heterozygous Foxp1 mouse brains. We demonstrate a role for FoxP1 in the transcriptional regulation of autism-related pathways as well as genes involved in neuronal activity. We show that Foxp1 regulates the excitability of striatal medium spiny neurons and that reduction of Foxp1 correlates with defects in ultrasonic vocalizations. Finally, we demonstrate that FoxP1 has an evolutionarily conserved role in regulating pathways involved in striatal neuron identity through gene expression studies in human neural progenitors with altered FOXP1 levels. These data support an integral role for FoxP1 in regulating signaling pathways vulnerable in autism and the specific regulation of striatal pathways important for vocal communication.

Funder

National Science Foundation

National Institutes of Health

Lymphoma Foundation

Cancer Prevention Research Institute of Texas

Marie Betzner Morrow Centennial Endowment

McDonnell Center for Systems Neuroscience

March of Dimes Foundation

Once Upon a Time Foundation

Autism Research at University of Texas Southwestern Endowment

Publisher

Cold Spring Harbor Laboratory

Subject

Developmental Biology,Genetics

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