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Making Drosophila lineage-restricted drivers via patterned recombination in neuroblasts.

Authors :
Awasaki, Takeshi
Kao, Chih-Fei
Lee, Ying-Jou
Yang, Ching-Po
Huang, Yaling
Pfeiffer, Barret D
Luan, Haojiang
Jing, Xiaotang
Huang, Yu-Fen
He, Yisheng
Schroeder, Mark David
Kuzin, Alexander
Brody, Thomas
Zugates, Christopher T
Odenwald, Ward F
Lee, Tzumin
Source :
Nature Neuroscience; Apr2014, Vol. 17 Issue 4, p631-637, 7p
Publication Year :
2014

Abstract

The Drosophila cerebrum originates from about 100 neuroblasts per hemisphere, with each neuroblast producing a characteristic set of neurons. Neurons from a neuroblast are often so diverse that many neuron types remain unexplored. We developed new genetic tools that target neuroblasts and their diverse descendants, increasing our ability to study fly brain structure and development. Common enhancer-based drivers label neurons on the basis of terminal identities rather than origins, which provides limited labeling in the heterogeneous neuronal lineages. We successfully converted conventional drivers that are temporarily expressed in neuroblasts, into drivers expressed in all subsequent neuroblast progeny. One technique involves immortalizing GAL4 expression in neuroblasts and their descendants. Another depends on loss of the GAL4 repressor, GAL80, from neuroblasts during early neurogenesis. Furthermore, we expanded the diversity of MARCM-based reagents and established another site-specific mitotic recombination system. Our transgenic tools can be combined to map individual neurons in specific lineages of various genotypes. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
10976256
Volume :
17
Issue :
4
Database :
Complementary Index
Journal :
Nature Neuroscience
Publication Type :
Academic Journal
Accession number :
95108886
Full Text :
https://doi.org/10.1038/nn.3654