Literature DB >> 9012523

The Drosophila decapentaplegic and short gastrulation genes function antagonistically during adult wing vein development.

K Yu1, M A Sturtevant, B Biehs, V François, R W Padgett, R K Blackman, E Bier.   

Abstract

TGF-beta-related signaling pathways play diverse roles during vertebrate and invertebrate development. A common mechanism for regulating the activity of TGF-beta family members is inhibition by extracellular antagonists. Recently, the Drosophila short gastrulation (sog) gene was shown to encode a predicted diffusible factor which antagonizes signaling mediated by the TGF-beta-like Decapentaplegic (Dpp) pathway in the early blastoderm embryo. sog and dpp, which are among the earliest zygotic genes to be activated, are expressed in complementary dorsal-ventral domains. The opposing actions of sog and dpp in the early embryo have been highly conserved during evolution as their vertebrate counterparts, chordin and BMP-4, function homologously to define neural versus non-neural ectoderm in Xenopus. Here we exploit the genetically sensitive adult wing vein pattern to investigate the generality of the antagonistic relationship between sog and dpp. We show that dpp is expressed in vein primordia during pupal wing development and functions to promote vein formation. In contrast, sog is expressed in complementary intervein cells and suppresses vein formation. sog and dpp function during the same phenocritical periods (i.e. 16-28 hours after pupariation) to influence the vein versus intervein cell fate choice. The conflicting activities of dpp and sog are also revealed by antagonistic dosage-sensitive interactions between these two genes during vein development. Analysis of vein and intervein marker expression in dpp and sog mutant wings suggests that dpp promotes vein fates indirectly by activating the vein gene rhomboid (rho), and that sog functions by blocking an autoactivating Dpp feedback loop. These data support the view that Sog is a dedicated Dpp antagonist.

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Year:  1996        PMID: 9012523     DOI: 10.1242/dev.122.12.4033

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  24 in total

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Journal:  Dev Cell       Date:  2011-08-16       Impact factor: 12.270

3.  Computational analysis of BMP gradients in dorsal-ventral patterning of the zebrafish embryo.

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Journal:  J Theor Biol       Date:  2007-06-06       Impact factor: 2.691

Review 4.  Regulation of bone morphogenetic proteins in early embryonic development.

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5.  crossveinless defines a new family of Twisted-gastrulation-like modulators of bone morphogenetic protein signalling.

Authors:  Peter Vilmos; Rui Sousa-Neves; Tamas Lukacsovich; J Lawrence Marsh
Journal:  EMBO Rep       Date:  2005-03       Impact factor: 8.807

6.  Identification of chromosomal regions involved in decapentaplegic function in Drosophila.

Authors:  R E Nicholls; W M Gelbart
Journal:  Genetics       Date:  1998-05       Impact factor: 4.562

7.  Mouse Crossveinless-2 is the vertebrate homolog of a Drosophila extracellular regulator of BMP signaling.

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8.  Cysteine repeat domains and adjacent sequences determine distinct bone morphogenetic protein modulatory activities of the Drosophila Sog protein.

Authors:  Kweon Yu; Kyung-Hwa Kang; Petra Heine; Ujwal Pyati; Shaila Srinivasan; Brian Biehs; David Kimelman; Ethan Bier
Journal:  Genetics       Date:  2004-03       Impact factor: 4.562

9.  N-linked glycosylation restricts the function of Short gastrulation to bind and shuttle BMPs.

Authors:  Erika Negreiros; Sophie Herszterg; Kyung-Hwa Kang; Amanda Câmara; Wagner B Dias; Katia Carneiro; Ethan Bier; Adriane Regina Todeschini; Helena Araujo
Journal:  Development       Date:  2018-11-19       Impact factor: 6.868

10.  Bistability coordinates activation of the EGFR and DPP pathways in Drosophila vein differentiation.

Authors:  Shian-Jang Yan; Jeremiah J Zartman; Minjie Zhang; Anthony Scott; Stanislav Y Shvartsman; Willis X Li
Journal:  Mol Syst Biol       Date:  2009-06-16       Impact factor: 11.429

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