There are two related long-term goals of the proposed research. First, we aim to determine the transcriptional regulators of a functional variant in the human MET promoter that is associated with autism spectrum disorder (ASD) vulnerability. Second, we plan to define the mechanisms through which the mouse Met receptor tyrosine kinase influences forebrain ontogeny. ASD is a significant neurodevelopmental disorder, with a prevalence of 1 in 150 in the United States, according to the Centers for Disease Control. Recently, we discovered that a single nucleotide polymorphism (SNP) in the 5'transcriptional regulatory region of the human MET gene (rs1858830 allele 'C') is strongly associated with ASD (P=5x10-6), and also reduces transcription factor (TF) binding and gene transcription. The convergence of data from human genetics studies in ASD and basic developmental neurobiology suggests that MET signaling is an important component for the assembly of forebrain circuits, with dysregulation leading to functional pathophysiology. We will first identify TFs that regulate MET expression. Our preliminary screen revealed 29 putative TFs, which we will validate by EMSA and ChIP assays. Over-expression and siRNA will be used to alter levels of MET-regulating TFs in vitro to delineate their individual and collective roles in regulating MET transcription. Next, we will use in situ hybridization in the mouse to establish the spatial and temporal expression of Met and its regulators during brain development. These maps are crucial for probing functional interactions that regulate Met transcription during cortical development. Finally, we will use a novel technical strategy, in utero electroporation in embryonic mice, to manipulate the expression of Lhx2, a putative Met-regulating TF, during brain development. The dual purpose of these manipulations is to reveal the effects of TF perturbation on Met expression in vivo and to define the ensuing impact on cortical development.

Public Health Relevance

Autism spectrum disorder (ASD) is a serious neurodevelopmental disorder that impacts a large number of individuals, and also their families. We have identified a change in the MET gene that alters the way in which it is regulated and more than doubles the risk of ASD. MET is known to influence brain development, and we are studying the ways in which it is normally regulated in the brain, and how dysregulation may lead to altered brain development and increased ASD susceptibility. Our focus on regulation of MET is highly relevant to many health issues, as over-expression of the gene is characteristic of highly invasive malignancies, and our work shows that under-expression may be a risk factor for ASD.

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Individual Predoctoral NRSA for M.D./Ph.D. Fellowships (ADAMHA) (F30)
Project #
5F30MH083474-03
Application #
7682848
Study Section
Special Emphasis Panel (ZNS1-SRB-M (51))
Program Officer
Desmond, Nancy L
Project Start
2007-09-25
Project End
2010-09-24
Budget Start
2009-09-25
Budget End
2010-09-24
Support Year
3
Fiscal Year
2009
Total Cost
$25,800
Indirect Cost
Name
Vanderbilt University Medical Center
Department
Pharmacology
Type
Schools of Medicine
DUNS #
004413456
City
Nashville
State
TN
Country
United States
Zip Code
37212
Eagleson, Kathie L; Campbell, Daniel B; Thompson, Barbara L et al. (2011) The autism risk genes MET and PLAUR differentially impact cortical development. Autism Res 4:68-83
Mukamel, Zohar; Konopka, Genevieve; Wexler, Eric et al. (2011) Regulation of MET by FOXP2, genes implicated in higher cognitive dysfunction and autism risk. J Neurosci 31:11437-42
Judson, Matthew C; Bergman, Mica Y; Campbell, Daniel B et al. (2009) Dynamic gene and protein expression patterns of the autism-associated met receptor tyrosine kinase in the developing mouse forebrain. J Comp Neurol 513:511-31