ebi regulates epidermal growth factor receptor signaling pathways in Drosophila

Dong, Xinzhong; Tsuda, Leo; Zavitz, Kenton H.; Lin, Michael; Li, Songhui; Carthew, Richard W.; Zipursky, S. Lawrence

doi:10.1101/gad.13.8.954

Cited by 76 publications

(121 citation statements)

References 57 publications

(56 reference statements)

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“…In addition, overexpression of all enhancers except ebi suppressed dlg and Fas2 tumorigenesis ( Figures 3C and 4D), further confirming that the identified genes function in a BLJ network. BLJ pathway components in the nucleus and their putative relationship to Notch: ebi encodes an F-box protein with WD repeats that promotes protein degradation of specific targets (Dong et al 1999;Boulton et al 2000). The failure of ebi overexpression to suppress Fas2 or dlg, and the relatively mild ebi phenotypes (midoogenesis small-nucleus and epithelial-organization defects, but no defects in germinal vesicle localization), suggest that ebi may function in only one of the three branches of BLJ signaling ( Figure 1A) or in a parallel pathway to the BLJ.…”

Section: Discussionmentioning

confidence: 99%

“…Thus ebi could enhance Fas2 and dlg tumorigenesis by functioning within the proliferationrepressing branch of the BLJ, or the importance of ebi for differentiation suggests that it could function in the EMT branch of the BLJ ( Figure 1A) or both. On the other hand, ebi promotes protein degradation in response to Notch (N) and Drosophila EGF receptor (EgfR) signals (Dong et al 1999;Boulton et al 2000;Tsuda et al 2002), suggesting that it may act in a parallel pathway. Both Ebi and its mammalian homolog, TBL1, function in a corepressor complex through association with nuclear hormone transcriptional corepressor SMRTER/SMRT (Guenther et al 2000;Tsuda et al 2002).…”

Section: Discussionmentioning

confidence: 99%

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Basolateral Junctions Utilize Warts Signaling to Control Epithelial-Mesenchymal Transition and Proliferation Crucial For Migration and Invasion of Drosophila Ovarian Epithelial Cells

Zhao¹,

Szafrański²,

Hall³

et al. 2008

Genetics

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Fasciclin2 (Fas2) and Discslarge (Dlg) localize to the basolateral junction (BLJ) of Drosophila follicle epithelial cells and inhibit their proliferation and invasion. To identify a BLJ signaling pathway we completed a genomewide screen for mutants that enhance dlg tumorigenesis. We identified two genes that encode known BLJ scaffolding proteins, lethal giant larvae (lgl) and scribble (scrib), and several not previously associated with BLJ function, including warts (wts) and roughened eye (roe), which encode a serine-threonine kinase and a transcription factor, respectively. Like scrib, wts and roe also enhance Fas2 and lgl tumorigenesis. Further, scrib, wts, and roe block border cell migration, and cause noninvasive tumors that resemble dlg partial loss of function, suggesting that the BLJ utilizes Wts signaling to repress EMT and proliferation, but not motility. Apicolateral junction proteins Fat (Ft), Expanded (Ex), and Merlin (Mer) either are not involved in these processes, or have highly spatio-temporally restricted roles, diminishing their significance as upstream inputs to Wts in follicle cells. This is further indicated in that Wts targets, CyclinE and DIAP1, are elevated in Fas2, dlg, lgl, wts, and roe cells, but not Fat, ex, or mer cells. Thus, the BLJ appears to regulate epithelial polarity and dynamics not only as a localized scaffold, but also by communicating signals to the nucleus. Wts may be regulated by distinct junction inputs depending on developmental context.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Basolateral Junctions Utilize Warts Signaling to Control Epithelial-Mesenchymal Transition and Proliferation Crucial For Migration and Invasion of Drosophila Ovarian Epithelial Cells

Zhao¹,

Szafrański²,

Hall³

et al. 2008

Genetics

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“…As described above, activation of Notch prevents R7 from assuming the R1/R6 fate. One important function of RTKs in the presumptive R7 is to activate an E3 Ligase complex composed of Seven in absentia (Sina), Phyllopod (Phyl), and Ebi (Li et al, 1997;Tang et al, 1997;Dong et al, 1999;Boulton et al, 2000;Li et al, 2002). This E3 complex ubiquitinates Tramtrack88 (Ttk88), a transcriptional repressor, targeting it for proteolysis.…”

Section: Photoreceptor R7mentioning

confidence: 99%

Signal integration during development: Insights from the Drosophila eye

Voas

Rebay

2003

Developmental Dynamics

161

159

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The Drosophila eye is a highly ordered epithelial tissue composed of ϳ750 subunits called ommatidia arranged in a reiterated hexagonal pattern. At higher resolution, observation of the constituent photoreceptors, cone cells, and pigment cells of the eye reveals a highly ordered mosaic of amazing regularity. This relatively simple organization belies the repeated requirement for spatially and temporally coordinated inputs from the Hedgehog (Hh), Wingless (Wg), Decapentaplegic (Dpp), JAK-STAT, Notch, and receptor tyrosine kinase (RTK) signaling pathways. This review will discuss how signaling inputs from the Notch and RTK pathways, superimposed on the developmental history of a cell, facilitate context-specific and appropriate cell fate specification decisions in the developing fly eye. Lessons learned from investigating the combinatorial signal integration strategies underlying Drosophila eye development will likely reveal cell-cell communication paradigms relevant to many aspects of invertebrate and mammalian development. Developmental Dynamics 229:162-175, 2004.

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“…We examined whether other E3 ligases induce the ubiquitination of Smad3. Fbw1a and hEbi1 are F-box proteins containing WD40 repeats, whereas Fbl1 (also termed Skp2) and Fbl5 have leucine-rich repeats (Cenciarelli et al, 1999;Dong et al, 1999;Winston et al, 1999a). Of these F-box proteins, only Fbw1a efficiently induced the ubiquitination of Smad3C ( Figure 4D).…”

Section: Roc1-scf Fbw1a Induces Ubiquitination Of Smad3mentioning

confidence: 99%

Ligand-dependent Degradation of Smad3 by a Ubiquitin Ligase Complex of ROC1 and Associated Proteins

Fukuchi

Imamura

Chiba

et al. 2001

MBoC

200

142

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Smads are signal mediators for the members of the transforming growth factor-β (TGF-β) superfamily. Upon phosphorylation by the TGF-β receptors, Smad3 translocates into the nucleus, recruits transcriptional coactivators and corepressors, and regulates transcription of target genes. Here, we show that Smad3 activated by TGF-β is degraded by the ubiquitin–proteasome pathway. Smad3 interacts with a RING finger protein, ROC1, through its C-terminal MH2 domain in a ligand-dependent manner. An E3 ubiquitin ligase complex ROC1-SCFFbw1a consisting of ROC1, Skp1, Cullin1, and Fbw1a (also termed βTrCP1) induces ubiquitination of Smad3. Recruitment of a transcriptional coactivator, p300, to nuclear Smad3 facilitates the interaction with the E3 ligase complex and triggers the degradation process of Smad3. Smad3 bound to ROC1-SCFFbw1a is then exported from the nucleus to the cytoplasm for proteasomal degradation. TGF-β/Smad3 signaling is thus irreversibly terminated by the ubiquitin–proteasome pathway.

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ebi regulates epidermal growth factor receptor signaling pathways in Drosophila

Cited by 76 publications

References 57 publications

Basolateral Junctions Utilize Warts Signaling to Control Epithelial-Mesenchymal Transition and Proliferation Crucial For Migration and Invasion of Drosophila Ovarian Epithelial Cells

Basolateral Junctions Utilize Warts Signaling to Control Epithelial-Mesenchymal Transition and Proliferation Crucial For Migration and Invasion of Drosophila Ovarian Epithelial Cells

Signal integration during development: Insights from the Drosophila eye

Ligand-dependent Degradation of Smad3 by a Ubiquitin Ligase Complex of ROC1 and Associated Proteins

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