Abstract

Four neural structures in the Drosophila optic lobes (lamina, medulla, lobula and lobula complex) sequentially process visual information through neural networks of specialized cell types organized in a retinotopic manner. We will continue our investigations to understand how neuronal diversity is generated in the developing optic lobes, which are comprised of more than 100 cell types. Our observations suggest that neuronal specification in the medulla results from the integration of three mechanisms: (i) 800 neuroblasts express a sequence of temporal transcription factors to generate distinct types of neurons as they age, each contacting one of the 800 columns innervated by photoreceptors. (ii) The temporal series is modified locally by regional transcription factors and produces neurons that innervate multiple columns. (iii) Binary fate choice via Notch further diversifies daughters of the terminal cell division. In the posterior-most region of the developing medulla and in the progenitor region of the lobula complex, neurogenesis differs significantly with a different set of transcription factors that act not only to specify neuronal fate but also to control the precursor mode of division and the death or survival of neurons. This illustrates how complex brain structures use different strategies to adapt and produce the correct number of specific cell types with the appropriate characteristics. We will investigate the mechanisms controlling this neurogenesis.
Aim 1 : Temporal progression of neuroblasts: Timing and transition mechanisms Temporal patterning is a general mechanism to generate neural diversity in flies and vertebrates. We will explore the molecular processes controlling the temporal progression of neuroblasts in the medulla.
Aim 2. Regionalization of the medulla neuroepithelium and specialization of neuroblasts We will investigate the rules that modify the output of the temporal series in different regions of the medulla progenitor domain. This allows the local production of neurons that migrate to occupy the entire medulla.
Aim 3. Correlation between transcription factor expression and neuronal characteristics To understand how transcription networks control the characteristics of neurons, we will use large-scale single cell transcriptomics to identify regulatory interactions and determine how these define the identity of each neuron.
Aim 4. Regulation of the mode of neuroblast division and neuronal survival or death by temporal patterning We will investigate how temporal transcription factors act on the cell cycle and on pro-apoptotic genes to characterize the different strategies used by distinct parts of the optic lobes to produce specialized neurons.
Aim 5. Temporal patterning-independent neurogenesis in lobula complex progenitors We will explore the molecular mechanisms that control a different mode of neurogenesis that produces 3 types of lobula neurons without a temporal series by controlling the rapid exit of neuroblasts from proliferation. This ambitious work will allow us to identify basic principles of neural patterning and diversity generation, which have broad implications for other neuronal systems in flies and vertebrates.

Public Health Relevance

Drosophila, with its genetic amenability and small brain size, yet sophisticated behavior, has been very successfully developed as a model system to study how neural circuits form. We investigate how neuronal diversity is generated in the optic lobes that contain more than one hundred cell types and will define the molecular mechanisms that specify the different neurons that process various aspects of visual information. The principles deduced from this project will be applicable to other neural systems in more complex organisms.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Research Project (R01)
Project #
5R01EY017916-11
Application #
9204835
Study Section
Neurogenesis and Cell Fate Study Section (NCF)
Program Officer
Greenwell, Thomas
Project Start
2007-02-01
Project End
2020-01-31
Budget Start
2017-02-01
Budget End
2018-01-31
Support Year
11
Fiscal Year
2017
Total Cost
$356,625
Indirect Cost
$131,625

  Institution

Name
New York University
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
041968306
City
New York
State
NY
Country
United States
Zip Code
10012

  Publications

Konstantinides, Nikolaos; Kapuralin, Katarina; Fadil, Chaimaa et al. (2018) Phenotypic Convergence: Distinct Transcription Factors Regulate Common Terminal Features. Cell 174:622-635.e13
Pinto-Teixeira, Filipe; Koo, Clara; Rossi, Anthony Michael et al. (2018) Development of Concurrent Retinotopic Maps in the Fly Motion Detection Circuit. Cell 173:485-498.e11
Barnhart, Erin L; Wang, Irving E; Wei, Huayi et al. (2018) Sequential Nonlinear Filtering of Local Motion Cues by Global Motion Circuits. Neuron 100:229-243.e3
Erclik, Ted; Li, Xin; Courgeon, Maximilien et al. (2017) Integration of temporal and spatial patterning generates neural diversity. Nature 541:365-370
Rossi, Anthony M; Fernandes, Vilaiwan M; Desplan, Claude (2017) Timing temporal transitions during brain development. Curr Opin Neurobiol 42:84-92
Nériec, Nathalie; Desplan, Claude (2016) From the Eye to the Brain: Development of the Drosophila Visual System. Curr Top Dev Biol 116:247-71
Pinto-Teixeira, Filipe; Desplan, Claude (2016) Re-utilization of a transcription factor. Elife 5:
Payre, François; Desplan, Claude (2016) RNA. Small peptides control heart activity. Science 351:226-7
Cavey, Matthieu; Collins, Ben; Bertet, Claire et al. (2016) Circadian rhythms in neuronal activity propagate through output circuits. Nat Neurosci 19:587-95
Pinto-Teixeira, Filipe; Konstantinides, Nikolaos; Desplan, Claude (2016) Programmed cell death acts at different stages of Drosophila neurodevelopment to shape the central nervous system. FEBS Lett 590:2435-2453

Showing the most recent 10 out of 29 publications