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Recruitment of cells into theDrosophilawing primordium by a feed-forward circuit ofvestigialautoregulation
Author(s) -
Myriam Zecca,
Gary Struhl
Publication year - 2007
Publication title -
development
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.754
H-Index - 325
eISSN - 1477-9129
pISSN - 0950-1991
DOI - 10.1242/dev.006411
Subject(s) - primordium , biology , wing , microbiology and biotechnology , imaginal disc , morphogen , decapentaplegic , autoregulation , blastoderm , schneider 2 cells , anatomy , drosophila melanogaster , gene , genetics , rna interference , endocrinology , physics , embryogenesis , embryo , rna , blood pressure , thermodynamics
The Drosophila wing primordium is defined by expression of the selector gene vestigial (vg) in a discrete subpopulation of cells within the wing imaginal disc. Following the early segregation of the disc into dorsal (D) and ventral (V) compartments, vg expression is governed by signals generated along the boundary between the two compartments. Short-range DSL (Delta/Serrate/LAG-2)-Notch signaling between D and V cells drives vg expression in `border' cells that flank the boundary. It also induces these same cells to secrete the long-range morphogen Wingless(Wg), which drives vg expression in surrounding cells up to 25-30 cell diameters away. Here, we show that Wg signaling is not sufficient to activate vg expression away from the D-V boundary. Instead, Wg must act in combination with a short-range signal produced by cells that already express vg. We present evidence that this vg-dependent, vg-inducing signal feeds forward from one cell to the next to entrain surrounding cells to join the growing wing primordium in response to Wg. We propose that Wg promotes the expansion of the wing primordium following the D-V segregation by fueling this non-autonomous autoregulatory mechanism.

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