Autism Research Database - Principal Investigator Project Details | IACC

Project Element	Element Description
Project Title Project Title	Translational dysregulation of the RhoA pathway in autism
Principal Investigator Principal Investigator	Iakoucheva, Lilia
Description Description	Copy number variants (CNVs) are the regions of the human genome that represent significant genetic risk factors for autism and other neurodevelopmental disorders. One such CNV located on chromosome 16, called 16p11.2, confers a high risk for developing autism and intellectual disability when deleted, and autism, schizophrenia, bipolar disorder and intellectual disability when duplicated. Even more intriguingly, 16p11.2 deletions are associated with increased head and brain size in the carriers (macrocephaly), whereas 16p11.2 duplications are associated with the decreased head and brain size (microcephaly). However, the exact mechanism by which this CNV influences brain size is unknown. Recent work in Lilia Iakoucheva’s laboratory at the University of California, San Diego gave some clues to what this mechanism might be. The researchers have demonstrated that interaction between two proteins, KCTD13, located within the 16p11.2 CNV, and CUL3, located on chromosome 2, influences the level of a third protein, RhoA1. This three-protein complex may be important for regulating brain size during fetal development. RhoA is already known to be involved in cell migration and cell-to-cell communication, and 16p11.2 CNV may be a major regulator of RhoA levels. In a collaborative study, Lilia Iakoucheva and Alysson Muotri propose to test this hypothesis using skin fibroblasts from individuals with autism who have the 16p11.2 CNV. Fibroblasts will be differentiated into neurons and, using sequencing and other modern genomics approaches, will be used to investigate molecular changes related to alterations in RhoA levels. The team will also test RhoA inhibitors as potential candidate autism therapeutics. Gaining precise knowledge of the pathway(s) disrupted by the 16p11.2 CNV is of key importance for developing better drug targets for the treatment of autism and other disorders linked to this CNV. References: 1. Lin G.N. et al. Neuron 85, 742-754 (2015) PubMed
Funder Funder	Simons Foundation
Funding Country Funding Country	United States
Fiscal Year Funding Fiscal Year Funding	250605
Current Award Period Current Award Period	2015-2018
Strategic Plan Question Strategic Plan Question	Question 2: What is the Biology Underlying ASD?
Funder’s Project Link Funder’s Project Link	External Project Page
Institution Institution	University of California, San Diego
Institute Location Institute Location	United States
Project Number Project Number	345469
Government or Private Government or Private	Private
History/Related Projects History/Related Projects	Translational dysregulation of the RhoA pathway in autism \| 125605 \| 2015 \| 345469 Translational dysregulation of the RhoA pathway in autism \| 250000 \| 2017 \| 345469 Translational dysregulation of the RhoA pathway in autism \| 125000 \| 2018 \| 345469

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