Abstract

The vertebrate central nervous system is formed with great precision into discrete yet interconnected structural and functional units that control anima behavior. Compartmentalization of the neuroepithelium into these functional units is facilitated by its exposure to signaling molecules secreted from localized organizing centers (Jessell, 2000; Hbert and Fishell, 2008; Scholpp and Lumsden, 2010). The zona limitans intrathalamica (zli) is one such signaling hub in the caudal forebrain that is the source of secreted morphogens, including Sonic hedgehog (Shh), that are essential for developing the thalamus into a vital processing and relay station for sensory and motor signals to the cerebral cortex (Epstein, 2012; Martinez-Ferre and Martinez, 2012). Mouse mutants that lack Shh in the zli and/or basal plate of the caudal diencephalon show significant alterations in thalamic progenitor identity and nucleogenesis (Szab et al., 2009; Vue et al., 2009; Jeong et al., 2011; Bluske et al., 2012). Despite the importance of the zli for thalamic morphogenesis, our knowledge of how this narrow boundary between the thalamus and prethalamus is established as a major brain-organizing center remains unresolved. Central to the understanding of zli formation is the mechanism by which Shh transcription is activated within its prescribed domain. Studies from my lab have provided substantial insight to the regulatory landscape underlying Shh transcription in the CNS (Jeong et al., 2006; Jeong et al., 2008; Geng et al., 2008; Jeong et al., 2011; Zhao et al., 2012). Experiments in this proposal will address the hypothesis that enhancers with overlapping activity in key brain signaling centers share a common cis-regulatory signature. Our preliminary studies have identified six sequence motifs that are highly enriched in a set of enhancers that coordinate the expression of Shh and other co-regulated genes in the ventral midbrain, caudal diencephalon and zli. In the following three aims, we propose to systematically evaluate the requirement of candidate components of the cis and trans regulatory network underlying Shh/zli gene expression (Aims 1 and 2), clarify the evolutionary origin of the vertebrate zli (Aim1), and determine whether specific alterations in the regulation of Shh/zli expression contribute to neurodevelopment disorders of thalamic function (Aim3).

Public Health Relevance

Alterations in the development of thalamic circuits are associated with a variety of neurological disorders, such as attention deficit, obsessive-compulsive, seizures, autism and schizophrenia. Elucidating the molecular mechanisms governing Shh expression in the zli will greatly improve our fundamental understanding of how this essential morphogen coordinates thalamic interneuron identity. If successful, our findings will add to the growing number of brain disorders associated with mutations in regulatory sequences.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
2R01NS039421-15
Application #
8815767
Study Section
Neurogenesis and Cell Fate Study Section (NCF)
Program Officer
Riddle, Robert D
Project Start
2000-03-01
Project End
2019-04-30
Budget Start
2015-05-15
Budget End
2016-04-30
Support Year
15
Fiscal Year
2015
Total Cost
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Genetics
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Corman, Tanya S; Bergendahl, Solsire E; Epstein, Douglas J (2018) Distinct temporal requirements for Sonic hedgehog signaling in development of the tuberal hypothalamus. Development 145:
Kahn, Benjamin M; Corman, Tanya S; Lovelace, Korah et al. (2017) Prenatal ethanol exposure in mice phenocopies Cdon mutation by impeding Shh function in the etiology of optic nerve hypoplasia. Dis Model Mech 10:29-37
Yao, Yao; Minor, Paul J; Zhao, Ying-Tao et al. (2016) Cis-regulatory architecture of a brain signaling center predates the origin of chordates. Nat Genet 48:575-80
Trowe, Mark-Oliver; Zhao, Li; Weiss, Anna-Carina et al. (2013) Inhibition of Sox2-dependent activation of Shh in the ventral diencephalon by Tbx3 is required for formation of the neurohypophysis. Development 140:2299-309
Lee, Bumwhee; Rizzoti, Karine; Kwon, David S et al. (2012) Direct transcriptional regulation of Six6 is controlled by SoxB1 binding to a remote forebrain enhancer. Dev Biol 366:393-403
Zhao, Li; Zevallos, Solsire E; Rizzoti, Karine et al. (2012) Disruption of SoxB1-dependent Sonic hedgehog expression in the hypothalamus causes septo-optic dysplasia. Dev Cell 22:585-96
Epstein, Douglas J (2012) Regulation of thalamic development by sonic hedgehog. Front Neurosci 6:57
Jeong, Yongsu; Dolson, Diane K; Waclaw, Ronald R et al. (2011) Spatial and temporal requirements for sonic hedgehog in the regulation of thalamic interneuron identity. Development 138:531-41
Epstein, Douglas J (2009) Cis-regulatory mutations in human disease. Brief Funct Genomic Proteomic 8:310-6
Geng, Xin; Speirs, Christina; Lagutin, Oleg et al. (2008) Haploinsufficiency of Six3 fails to activate Sonic hedgehog expression in the ventral forebrain and causes holoprosencephaly. Dev Cell 15:236-47

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