Abstract

To unravel how the astonishing diversity of neurons is derived through birth order/timing-dependent cell fate specification, we propose to use sophisticated genetic tools in a relatively simple organism, the fruit fly Drosophila, to study the mechanisms of neuronal temporal identity. From a genetic mosaic screen, we have identified the Drosophila Chinmo BTB-zinc finger protein, and in particular its gradients through neurogenesis, as a novel mechanism conferring neuronal temporal identity. We have further demonstrated that the establishment of the Chinmo gradient involves the differential translation of chinmo messages carrying a 1.7kb-long 5'UTR. In this proposal, we will (1) examine the generality of Chinmo function in specifying neuronal temporal identity, (2) investigate the chinmo 5'UTR-dependent translational control for tracing back the origin for Chinmo-governed neuronal temporal cell fate specifications, and (3) screen for additional genes that may act within the Chinmo pathway or operate independently to control neuronal temporal identity. This study, including thorough analysis of Chinmo function and systematical identification of temporal identity genes, promises to provide major insights into the mechanisms governing birth order/timing-dependent neuronal diversification, a crucial developmental process in the brain. ?

Public Health Relevance

The brain is composed of a monumental number of different types of neurons. These neurons interact with each other forming the complex brain circuits that underlie behavior and the coordination of the vital functions of the body. Congenital and developmental disorders that interfere with the formation of neuronal diversity have drastic consequences for brain function. Further, knowledge about the stem cells that in the brain give rise to this diversity may provide powerful clinical approaches for interventions during degenerative disorders or after injury. The goal of this project is to understand how brain stem cells give rise to neuronal diversity according to the order in which neurons are born (temporal identity). To address this question we are using a powerful model system, the fruit fly Drosophila, in which the genes controlling temporal identity can be isolated in an efficient manner. Our studies in this system have isolated a gene, called chinmo (chronologically inappropriate morphogenesis) with central roles in this process. In this project we will elucidate the mechanisms of Chinmo function by (a) determining if it is a universal temporal identity gene, or whether there are other genes that also can fulfill this function, (b) determining the mechanisms by which Chinmo functions, and (c) searching for other cell identity genes that may function with Chinmo, or in a Chinmo-independent fashion to confer temporal identity. We expect that the studies proposed will have a fundamental impact in our understanding of how neuronal diversity is generated, how this neuronal diversity is encoded in stem cells, and how these stem cells can be manipulated in order to generate particular neuron populations. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Project (R01)
Project #
1R01MH080739-01A2
Application #
7526520
Study Section
Neurogenesis and Cell Fate Study Section (NCF)
Program Officer
Panchision, David M
Project Start
2008-08-01
Project End
2013-06-30
Budget Start
2008-08-01
Budget End
2009-06-30
Support Year
1
Fiscal Year
2008
Total Cost
$367,969
Indirect Cost

  Institution

Name
University of Massachusetts Medical School Worcester
Department
Biology
Type
Schools of Medicine
DUNS #
603847393
City
Worcester
State
MA
Country
United States
Zip Code
01655

  Publications

Lee, Tzumin (2014) Generating mosaics for lineage analysis in flies. Wiley Interdiscip Rev Dev Biol 3:69-81
Awasaki, Takeshi; Kao, Chih-Fei; Lee, Ying-Jou et al. (2014) Making Drosophila lineage-restricted drivers via patterned recombination in neuroblasts. Nat Neurosci 17:631-7
Lin, Suewei; Marin, Elizabeth C; Yang, Ching-Po et al. (2013) Extremes of lineage plasticity in the Drosophila brain. Curr Biol 23:1908-13
Yang, Jacob S; Awasaki, Takeshi; Yu, Hung-Hsiang et al. (2013) Diverse neuronal lineages make stereotyped contributions to the Drosophila locomotor control center, the central complex. J Comp Neurol 521:2645-Spc1
Yu, Hung-Hsiang; Awasaki, Takeshi; Schroeder, Mark David et al. (2013) Clonal development and organization of the adult Drosophila central brain. Curr Biol 23:633-43
Kao, Chih-Fei; Yu, Hung-Hsiang; He, Yisheng et al. (2012) Hierarchical deployment of factors regulating temporal fate in a diverse neuronal lineage of the Drosophila central brain. Neuron 73:677-84
Pitman, Jena L; Huetteroth, Wolf; Burke, Christopher J et al. (2011) A pair of inhibitory neurons are required to sustain labile memory in the Drosophila mushroom body. Curr Biol 21:855-61
Yu, Hung-Hsiang; Kao, Chih-Fei; He, Yisheng et al. (2010) A complete developmental sequence of a Drosophila neuronal lineage as revealed by twin-spot MARCM. PLoS Biol 8:
Kao, Chih-Fei; Lee, Tzumin (2010) Birth time/order-dependent neuron type specification. Curr Opin Neurobiol 20:14-21
Lin, Suewei; Lai, Sen-Lin; Yu, Huang-Hsiang et al. (2010) Lineage-specific effects of Notch/Numb signaling in post-embryonic development of the Drosophila brain. Development 137:43-51

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