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PiggyBac-based mosaic screen identifies a postmitotic function for cohesin in regulating developmental axon pruning.


ABSTRACT: Developmental axon pruning is widely used to refine neural circuits. We performed a mosaic screen to identify mutations affecting axon pruning of Drosophila mushroom body gamma neurons. We constructed a modified piggyBac vector with improved mutagenicity and generated insertions in >2000 genes. We identified two cohesin subunits (SMC1 and SA) as being essential for axon pruning. The cohesin complex maintains sister-chromatid cohesion during cell division in eukaryotes. However, we show that the pruning phenotype in SMC1(-/-) clones is rescued by expressing SMC1 in neurons, revealing a postmitotic function. SMC1(-/-) clones exhibit reduced levels of the ecdysone receptor EcR-B1, a key regulator of axon pruning. The pruning phenotype is significantly suppressed by overexpressing EcR-B1 and is enhanced by a reduced dose of EcR, supporting a causal relationship. We also demonstrate a postmitotic role for SMC1 in dendrite targeting of olfactory projection neurons. We suggest that cohesin regulates diverse aspects of neuronal morphogenesis.

SUBMITTER: Schuldiner O 

PROVIDER: S-EPMC2268086 | biostudies-literature | 2008 Feb

REPOSITORIES: biostudies-literature

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piggyBac-based mosaic screen identifies a postmitotic function for cohesin in regulating developmental axon pruning.

Schuldiner Oren O   Berdnik Daniela D   Levy Jonathan Ma JM   Wu Joy S JS   Luginbuhl David D   Gontang Allison Camille AC   Luo Liqun L  

Developmental cell 20080201 2


Developmental axon pruning is widely used to refine neural circuits. We performed a mosaic screen to identify mutations affecting axon pruning of Drosophila mushroom body gamma neurons. We constructed a modified piggyBac vector with improved mutagenicity and generated insertions in >2000 genes. We identified two cohesin subunits (SMC1 and SA) as being essential for axon pruning. The cohesin complex maintains sister-chromatid cohesion during cell division in eukaryotes. However, we show that the  ...[more]

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