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First published online 14 December 2005
doi: 10.1242/dev.02191
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1 Department of Biology, University of Washington, Seattle WA 98195, USA.
2 Department of Biology and Center for Genomics and Bioinformatics, Indiana
University, Bloomington, IN 47405, USA.
* Author for correspondence (e-mail: hdbrown{at}u.washington.edu)
Accepted 31 October 2005
During metamorphosis, the reorganization of the nervous system of Drosophila melanogaster proceeds in part through remodeling of larval neurons. In this study, we used in-vitro imaging techniques and immunocytochemistry to track the remodeling of the thoracic ventral neurosecretory cells. Axons of these neurons prune their larval arbors early in metamorphosis and a larger, more extensive adult arbor is established via branch outgrowth. Expression of EcR dominant negative constructs and an EcR inverted repeat construct resulted in pruning defects of larval axon arbors and a lack of filopodia during pruning, but showed variable effects on outgrowth depending on the construct expressed. Cells expressing either UAS-EcR-B1W650A or UAS-EcR-AW650A lacked filopodia during the outgrowth period and formed a poorly branched, larval-like arbor in the adult. Cells expressing UAS-EcR-B1F645A, UAS-EcR-B2W650A or UAS-IR-EcR (core) showed moderate filopodial activity and normal, albeit reduced, adult-like branching during outgrowth. These results are consistent with the role of activation versus derepression via EcR for successive phases of neuronal remodeling and suggest that functional ecdysone receptor is necessary for some, but not all, remodeling events.
Key words: Drosophila, Axon remodeling, Ecdysone receptor, Metamorphosis
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