Abstract
BackgroundVarious members of the family of BTB/POZ zinc-finger transcription factors influence patterns of dendritic branching. One such member, Broad, is notable because its BrZ3 isoform is widely expressed in Drosophila in immature neurons around the time of arbor outgrowth. We used the metamorphic remodeling of an identified sensory neuron, the dorsal bipolar dendrite sensory neuron (dbd), to examine the effects of BrZ3 expression on the extent and pattern of dendrite growth during metamorphosis.ResultsUsing live imaging of dbd in Drosophila pupae, we followed its normal development during metamorphosis and the effect of ectopic expression of BrZ3 on this development. After migration of its cell body, dbd extends a growth-cone that grows between two muscle bands followed by branching and turning back on itself to form a compact dendritic bundle. The ectopic expression of the BrZ3 isoform, using the GAL4/UAS system, caused dbd's dendritic tree to transform from its normal, compact, fasciculated form into a comb-like arbor that spread over on the body wall. Time-lapse analysis revealed that the expression of BrZ3 caused the premature extension of the primary dendrite onto immature myoblasts, ectopic growth past the muscle target region, and subsequent elaboration onto the epidermis. To control the timing of expression of BrZ3, we used a temperature-sensitive GAL80 mutant. When BrZ3 expression was delayed until after the extension of the primary dendrite, then a normal arbor was formed. By contrast, when BrZ3 expression was confined to only the early outgrowth phase, then ectopic arbors were subsequently formed and maintained on the epidermis despite the subsequent absence of BrZ3.ConclusionsThe adult arbor of dbd is a highly branched arbor whose branches self-fasciculate to form a compact dendritic bundle. The ectopic expression of BrZ3 in this cell causes a premature extension of its growth-cone, resulting in dendrites that extend beyond their normal muscle substrate and onto the epidermis, where they form a comb-shaped, ectopic arbor. Our quantitative data suggest that new ectopic arbor represents an 'unpacking' of the normally fasciculated arbor onto the epidermis. These data suggest that the nature of their local environment can change dendrite behavior from self-adhesion to self-avoidance.
Highlights
Various members of the family of BTB/POZ zinc-finger transcription factors influence patterns of dendritic branching
We found that with Broad isoform Z3 (BrZ3) misexpression, dbd extended beyond its appropriate muscle substrate onto the epidermis, and in this new environment, its dendrites changed from having a robust fasciculated architecture to a tree-like, self-avoidance pattern of arborization
The ectopic expression of BrZ3 in this cell causes a premature extension of its growth cone, resulting in dendrites that extend beyond their normal muscle substrate and onto the epidermis where they form a comb-shaped, ectopic arbor
Summary
Various members of the family of BTB/POZ zinc-finger transcription factors influence patterns of dendritic branching. One such member, Broad, is notable because its BrZ3 isoform is widely expressed in Drosophila in immature neurons around the time of arbor outgrowth. Neuronal development requires the coordination of fate specification, cell migration, neurite pathfinding, arbor elaboration, terminal field refinement and synaptogenesis. Understanding how these dynamic developmental processes give rise to the diverse cellular forms and specific. We used dbd to investigate the effects of the Z3 isoform of the BTB/POZ zinc-finger transcription factor Broad (BrZ3) on dendritic development in intact animals. BrZ3 expression occurs after the completion of pathfinding as young neurons are initiating arbor outgrowth, but it disappears when arbor elaboration is well underway [22]
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