Article

Broad complex isoforms have unique distributions during central nervous system metamorphosis in Drosophila melanogaster

  1. Rebecca F. Spokony1,2,†,
  2. Linda L. Restifo1,2,3,4,*

Article first published online: 11 JUN 2009

DOI: 10.1002/cne.22119

Issue

The Journal of Comparative Neurology

The Journal of Comparative Neurology

Volume 517, Issue 1, pages 15–36, 1 November 2009

Additional Information

How to Cite

Spokony, R. F. and Restifo, L. L. (2009), Broad complex isoforms have unique distributions during central nervous system metamorphosis in Drosophila melanogaster. The Journal of Comparative Neurology, 517: 15–36. doi: 10.1002/cne.22119

Author Information

  1. 1

    Graduate Interdisciplinary Program in Insect Science, University of Arizona, Tucson, Arizona 85721-0108

  2. 2

    ARL Division of Neurobiology, University of Arizona, Tucson, Arizona 85721-0077

  3. 3

    Department of Neurology, Arizona Health Sciences Center, Tucson, Arizona 85724

  4. 4

    BIO5 Institute for Collaborative Bioresearch, University of Arizona, 85721

  1. Dept. of Human Genetics, The University of Chicago, 920 E. 58th St., Chicago, IL 60637

*ARL Division of Neurobiology, University of Arizona, 611 Gould-Simpson Bldg., 1040 E. 4th St., Tucson, AZ 85721-0077

Publication History

  1. Issue published online: 26 AUG 2009
  2. Article first published online: 11 JUN 2009
  3. Accepted manuscript online: 11 JUN 2009 12:00AM EST
  4. Manuscript Accepted: 17 MAY 2009
  5. Manuscript Revised: 3 APR 2009
  6. Manuscript Received: 20 NOV 2008

Funded by

  • National Institutes of Health (NIH). Grant Number: HD 038363
  • National Science Foundation (NSF). Grant Number: IGERT training grant DGE 0114420

SEARCH

SEARCH BY CITATION

ARTICLE TOOLS

View Full Article with Supporting Information (HTML) Get PDF (7211K)

Keywords:

  • ecdysone cascade;
  • insect;
  • neuron;
  • glia;
  • neuroblast;
  • duplicated exons;
  • subfunctionalization;
  • morphogenesis

Abstract

Broad Complex (BRC) is a highly conserved, ecdysone-pathway gene essential for metamorphosis in Drosophila melanogaster, and possibly all holometabolous insects. Alternative splicing among duplicated exons produces several BRC isoforms, each with one zinc-finger DNA-binding domain (Z1, Z2, Z3, or Z4), highly expressed at the onset of metamorphosis. BRC-Z1, BRC-Z2, and BRC-Z3 represent distinct genetic functions (BRC complementation groups rbp, br, and 2Bc, respectively) and are required at discrete stages spanning final-instar larva through very young pupa. We showed previously that morphogenetic movements necessary for adult CNS maturation require BRC-Z1, -Z2, and -Z3, but not at the same time: BRC-Z1 is required in the mid-prepupa, BRC-Z2 and -Z3 are required earlier, at the larval-prepupal transition. To explore how BRC isoforms controlling the same morphogenesis events do so at different times, we examined their central nervous system (CNS) expression patterns during the ≈16 hours bracketing the hormone-regulated start of metamorphosis. Each isoform had a unique pattern, with BRC-Z3 being the most distinctive. There was some colocalization of isoform pairs, but no three-way overlap of BRC-Z1, -Z2, and -Z3. Instead, their most prominent expression was in glia (BRC-Z1), neuroblasts (BRC-Z2), or neurons (BRC-Z3). Despite sequence similarity to BRC-Z1, BRC-Z4 was expressed in a unique subset of neurons. These data suggest a switch in BRC isoform choice, from BRC-Z2 in proliferating cells to BRC-Z1, BRC-Z3, or BRC-Z4 in differentiating cells. Together with isoform-selective temporal requirements and phenotype considerations, this cell-type-selective expression suggests a model of BRC-dependent CNS morphogenesis resulting from intercellular interactions, culminating in BRC-Z1-controlled, glia-mediated CNS movements in late prepupa. J. Comp. Neurol. 517:15–36, 2009. © 2009 Wiley-Liss, Inc.

View Full Article with Supporting Information (HTML) Get PDF (7211K)