Abstract

Our long-term goal for this project is to advance our understanding of developmental disorders of the brainstem and cerebellum, brain structures derived from the embryonic midbrain and hindbrain, which we refer to collectively as mid-hindbrain malformations (MHM). These disorders affect a minimum of 1 per 6-7000 live births, and likely far more as these numbers do not account for cerebellar abnormalities associated with preterm birth or with autism. Further, cerebellar malformations are known to co-occur with several more common developmental disorders including autism, mental retardation and some types of early life epilepsy. With this renewal, we propose to continue using our large and growing cohort of human subjects with MHM to define the genes, pathways and biological mechanisms underlying these developmental disorders. We will use the most recent genomic technology - massively parallel (NextGen) sequencing of targeted gene panels, whole exome sequencing (WXS) or whole genome sequencing (WGS) - combined with older methods to find the causes of both rare and common MHM.
In Aim 1, we will continue to search for genes underlying rare single gene causes of MHM that will demonstrate the most important molecular pathways, including pathways that contribute to more common disorders such as autism. As an example, we have identified the first missense mutation of the AUTS2 gene (previously linked to autism) in a child with MHM.
In Aim 2, we will turn to the more challenging but also more important problem of Dandy-Walker malformation, the most common MHM in humans. This specific malformation demonstrates substantial causal heterogeneity and has proven difficult to solve with older technologies, making whole exome and genome sequencing approaches essential.
Aims 1 -2 need to be supported by ongoing subject recruitment, as studies of comparable disorders such as mental retardation and autism have benefited from large numbers of subjects.
In Aim 3, we propose to test the biological function of genes and networks identified in Aims 1-2 using new CRISPR/Cas technology to efficiently generate new mouse models of proven and strong candidate MHM-associated genes. For example, we are now generating the first mouse models of Auts2. We expect that these studies will contribute rapidly to more accurate diagnosis and counseling, and over time will lead to development of specific treatments for a subset of these disorders. We predict that studies of mid-hindbrain development will have broad significance for human developmental disorders generally, providing compelling evidence for a connection between cerebellar development and other classes of developmental disorders.

Public Health Relevance

Developmental disorders of the brainstem and cerebellum - which are derived from the embryonic midbrain and hindbrain - are a collectively important class of disorders that affect a minimum of 2.4 per 1000 resident births based on data from the CDC. The true frequency is likely much higher. This large class of disorders co-occurs with more common developmental disorders such as autism, mental retardation and some forms of infantile epilepsy, and shares some of the same causes. We propose to find the causes of several different types of brainstem and cerebellar malformations, which will contribute to more accurate diagnosis and counseling in the short term, and to specific treatments for some of these disorders in the long term.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS050375-12
Application #
9013505
Study Section
Developmental Brain Disorders Study Section (DBD)
Program Officer
Riddle, Robert D
Project Start
2005-09-15
Project End
2020-05-31
Budget Start
2016-06-01
Budget End
2017-05-31
Support Year
12
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
Seattle Children's Hospital
Department
Type
DUNS #
048682157
City
Seattle
State
WA
Country
United States
Zip Code
98101

  Publications

Dobyns, William B; Aldinger, Kimberly A; Ishak, Gisele E et al. (2018) MACF1 Mutations Encoding Highly Conserved Zinc-Binding Residues of the GAR Domain Cause Defects in Neuronal Migration and Axon Guidance. Am J Hum Genet 103:1009-1021
Brock, Stefanie; Stouffs, Katrien; Scalais, Emmanuel et al. (2018) Tubulinopathies continued: refining the phenotypic spectrum associated with variants in TUBG1. Eur J Hum Genet 26:1132-1142
Di Donato, Nataliya; Timms, Andrew E; Aldinger, Kimberly A et al. (2018) Analysis of 17 genes detects mutations in 81% of 811 patients with lissencephaly. Genet Med 20:1354-1364
Haldipur, Parthiv; Dang, Derek; Millen, Kathleen J (2018) Embryology. Handb Clin Neurol 154:29-44
De Mori, Roberta; Romani, Marta; D'Arrigo, Stefano et al. (2017) Hypomorphic Recessive Variants in SUFU Impair the Sonic Hedgehog Pathway and Cause Joubert Syndrome with Cranio-facial and Skeletal Defects. Am J Hum Genet 101:552-563
Brun, Brianna N; Mockler, Shelley R H; Laubscher, Katie M et al. (2017) Comparison of brain MRI findings with language and motor function in the dystroglycanopathies. Neurology 88:623-629
Haldipur, Parthiv; Dang, Derek; Aldinger, Kimberly A et al. (2017) Phenotypic outcomes in Mouse and Human Foxc1 dependent Dandy-Walker cerebellar malformation suggest shared mechanisms. Elife 6:
Syrbe, Steffen; Harms, Frederike L; Parrini, Elena et al. (2017) Delineating SPTAN1 associated phenotypes: from isolated epilepsy to encephalopathy with progressive brain atrophy. Brain 140:2322-2336
Van De Weghe, Julie C; Rusterholz, Tamara D S; Latour, Brooke et al. (2017) Mutations in ARMC9, which Encodes a Basal Body Protein, Cause Joubert Syndrome in Humans and Ciliopathy Phenotypes in Zebrafish. Am J Hum Genet 101:23-36
Byers, Heather M; Adam, Margaret P; LaCroix, Amy et al. (2017) Description of a new oncogenic mechanism for atypical teratoid rhabdoid tumors in patients with ring chromosome 22. Am J Med Genet A 173:245-249

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