Genome wide analysis of transcript levels after perturbation of the EGFR pathway in the <i>Drosophila</i> ovary

Jordan, Katherine C.; Hatfield, Steven; Tworoger, Michael; Ward, Ellen J.; Fischer, Karin A.; Bowers, Stuart; Ruohola‐Baker, Hannele

doi:10.1002/dvdy.20318

Cited by 30 publications

(29 citation statements)

References 78 publications

(81 reference statements)

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“…Table 1 shows the top 25 transcripts upregulated by Egfr ACT , and Table 2 shows the top 25 transcripts upregulated by Egfr DN [the full set is shown in Table S1 and the primary data have been submitted to GEO (GSE34872)]. Eight of these genes were also identified in other studies that conducted whole-genome transcriptional analysis of the Egfr pathway or the Ras gene, which functions downstream of Egfr (Tables 1 and 2) (Asha et al 2003;Jordan et al 2005;Firth and Baker 2007). Five known target genes were also represented within the top group of 25 genes upregulated by Egfr: ventral veinless (vvl) (de Celis et al 1995;Llimargas and Casanova 1997), sty (Hacohen et al 1998;Casci et al 1999), pnt (O'Neill et al 1994Gabay et al 1996), MASK (Smith et al 2002), and Mkp3 (Kim et al 2003;Rintelen et al 2003;Gomez et al 2005).…”

Section: Resultsmentioning

confidence: 99%

New Negative Feedback Regulators of Egfr Signaling inDrosophila

et al. 2012

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The highly conserved epidermal growth factor receptor (Egfr) pathway is required in all animals for normal development and homeostasis; consequently, aberrant Egfr signaling is implicated in a number of diseases. Genetic analysis of Drosophila melanogaster Egfr has contributed significantly to understanding this conserved pathway and led to the discovery of new components and targets. Here we used microarray analysis of third instar wing discs, in which Egfr signaling was perturbed, to identify new Egfrresponsive genes. Upregulated transcripts included five known targets, suggesting the approach was valid. We investigated the function of 29 previously uncharacterized genes, which had pronounced responses. The Egfr pathway is important for wing-vein patterning and using reverse genetic analysis we identified five genes that showed venation defects. Three of these genes are expressed in vein primordia and all showed transcriptional changes in response to altered Egfr activity consistent with being targets of the pathway. Genetic interactions with Egfr further linked two of the genes, Sulfated (Sulf1), an endosulfatase gene, and CG4096, an A Disintegrin And Metalloproteinase with ThromboSpondin motifs (ADAMTS) gene, to the pathway. Sulf1 showed a strong genetic interaction with the neuregulin-like ligand vein (vn) and may influence binding of Vn to heparan-sulfated proteoglycans (HSPGs). How Drosophila Egfr activity is modulated by CG4096 is unknown, but interestingly vertebrate EGF ligands are regulated by a related ADAMTS protein. We suggest Sulf1 and CG4096 are negative feedback regulators of Egfr signaling that function in the extracellular space to influence ligand activity.

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Section: Resultsmentioning

confidence: 99%

New Negative Feedback Regulators of Egfr Signaling inDrosophila

et al. 2012

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“…The lack of BR expression in these cells may be due to the lack of Wg signal. Wg signaling has been shown to be required for BR expression in the follicle cells of the dorsal appendage primordia of egg chambers (Jordan et al, 2005;Ward et al, 2006). However, the loss of br expression in the cells in the p2 region is not likely to be caused by lack of Wg signal, because Wg is present at higher levels in the p2 region than in the p1 region where BR is expressed (Lawrence et al, 2002).…”

Section: Jh Delayed the Adult Development Of The Abdominal Epidermismentioning

confidence: 96%

Krüppel homolog 1 (Kr-h1) mediates juvenile hormone action during metamorphosis of Drosophila melanogaster

Minakuchi

Zhou

Riddiford

2008

Mechanisms of Development

241

232

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Juvenile hormone (JH) given at pupariation inhibits bristle formation and causes pupal cuticle formation in the abdomen of Drosophila melanogaster due to its prolongation of expression of the transcription factor Broad (BR). In a microarray analysis of JH-induced gene expression in abdominal integument, we found that Krüppel homolog 1 (Kr-h1) was up-regulated during most of adult development. Quantitative real-time PCR analyses showed that Kr-h1 up-regulation began at 10h after puparium formation (APF), and Kr-h1 up-regulation occurred in imaginal epidermal cells, persisting larval muscles, and larval oenocytes. Ectopic expression of Kr-h1 in abdominal epidermis using T155-Gal4 to drive UAS-Kr-h1 resulted in missing or short bristles in the dorsal midline. This phenotype was similar to that seen after a low dose of JH or after misexpression of br between 21 and 30 h APF. Ectopic expression of Kr-h1 prolonged the expression of BR protein in the pleura and the dorsal tergite. No Kr-h1 was seen after misexpression of br. Thus, Kr-h1 mediates some of the JH signaling in the adult abdominal epidermis and is upstream of br in this pathway. We also show for the first time that the JH-mediated maintenance of br expression in this epidermis is patterned and that JH delays the fusion of the imaginal cells and the disappearance of Dpp in the dorsal midline.

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“…Recent microarray analysis has identified a number of genes that are regulated by mirr overexpression or alterations in Egfr signaling and that therefore represent potential Mirr targets (Jordan et al, 2005). Mirr also appears to regulate cell affinity, as mirr mutant clones in the eye exhibit a round shape (Yang et al, 1999).…”

Section: Research Articlementioning

confidence: 99%

Capicua regulates follicle cell fate in theDrosophilaovary through repression ofmirror

et al. 2006

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The dorsoventral axis of the Drosophila egg is established by dorsally localized activation of the epidermal growth factor receptor (Egfr)in the ovarian follicular epithelium. Subsequent positive- and negative-feedback regulation generates two dorsolateral follicle cell primordia that will produce the eggshell appendages. A dorsal midline domain of low Egfr activity between the appendage primordia defines their dorsal boundary, but little is known about the mechanisms that establish their ventral limit. We demonstrate that the transcriptional repressor Capicua is required cell autonomously in ventral and lateral follicle cells to repress dorsal fates, and functions in this process through the repression of mirror. Interestingly, ectopic expression of mirror in the absence of capicua is observed only in the anterior half of the epithelium. We propose that Capicua regulates the pattern of follicle cell fates along the dorsoventral axis by blocking the induction of appendage determinants, such as mirror, by anterior positional cues.

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Genome wide analysis of transcript levels after perturbation of the EGFR pathway in the Drosophila ovary

Cited by 30 publications

References 78 publications

New Negative Feedback Regulators of Egfr Signaling inDrosophila

New Negative Feedback Regulators of Egfr Signaling inDrosophila

Krüppel homolog 1 (Kr-h1) mediates juvenile hormone action during metamorphosis of Drosophila melanogaster

Capicua regulates follicle cell fate in theDrosophilaovary through repression ofmirror

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