A Wingless and Notch double-repression mechanism regulates G1–S transition in the Drosophila wing

Herranz, Héctor; Pérez, Lídia; Martín, Francisco A.; Milán, Marco

doi:10.1038/emboj.2008.84

Cited by 99 publications

(156 citation statements)

References 48 publications

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“…This assumption is based on a variety of experimental models in which reorganization of pattern is always accompanied by growth (French et al 1976). Consistent with this idea, Myc expression is regulated by several conserved factors that control pattern formation (He et al 1998;Herranz et al 2008;Johnston et al 1999;Prober and Edgar 2002), whereas Myc itself controls the growth and proliferation of cells by regulating numerous genes required for ribosome biogenesis and protein synthesis (Grewal et al 2005;Hulf et al 2005). However, our experiments suggest that the hierarchy between pattern and growth is not absolute.…”

Section: Discussionsupporting

confidence: 74%

“…By the end of larval development dmyc expression is very low in hinge cells but high in cells of the notum and WP. With the onset of proneural specification at the wing margin, dmyc expression is repressed by the activities of Wg and Notch in cells flanking the D/V boundary as these cells arrest growth and division ( Figure 1G) ( Johnston et al 1999;Johnston and Sanders 2003;Duman-Scheel et al 2004;Herranz et al 2008). dMyc protein expression is similar to dmyc mRNA at all stages examined ( Figure 1H, Figure S1, and data not shown).…”

Section: Resultsmentioning

confidence: 88%

“…Despite being smaller, dm mutant flies appear morphologically normal with no obvious patterning defects ( Johnston et al 1999), suggesting tight linkage between the patterning machinery and dMyc. In the wing, Wg and Notch activity repress dMyc expression in the zone of nonproliferating cells that surrounds the D/V boundary to enforce a cell cycle arrest of these cells ( Johnston et al 1999;Duman-Scheel et al 2004;Herranz et al 2008). However, how dMyc contributes to wing development and the nature of the relationship between pattern formation and dMyc expression and activity in the growing wing disc is not understood.…”

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confidence: 99%

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Control of Wing Size and Proportions by Drosophila Myc

Wu¹,

Johnston

2010

Genetics

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Generation of an organ of appropriate size and shape requires mechanisms that coordinate growth and patterning, but how this is achieved is not understood. Here we examine the role of the growth regulator dMyc in this process during Drosophila wing imaginal disc development. We find that dMyc is expressed in a dynamic pattern that correlates with fate specification of different regions of the wing disc, leading us to hypothesize that dMyc expression in each region directs its growth. Consistent with this view, clonal analysis of growth in each region demonstrated distinct temporal requirements for dMyc that match its expression. Surprisingly, however, experiments in which dMyc expression is manipulated reveal that the endogenous pattern has only a minor influence on wing shape. Indeed, when dMyc function is completely lacking in the wing disc over most of its development, the discs grow slowly and are small in size but appear morphologically normal. Our experiments indicate, therefore, that rather than directly influence differential growth in the wing disc, the pattern of dMyc expression augments growth directed by other regulators. Overall, however, an appropriate level of dMyc expression in the wing disc is necessary for each region to achieve a proportionately correct size.H OW pattern and growth are coordinated during development to produce an organ of correct size and shape is a central question in biology. The Drosophila wing is an elegant, self-organizing system that is ideal for the study of this coordination. Wing growth is coupled to the specification of cell fates, and these processes are regulated by a small number of conserved signaling pathways and selector proteins. The wing develops from the wing imaginal disc, a proliferating epithelium housed in the larva that also gives rise to the dorsal thorax of the adult fly. The adult wing includes the blade, made from wing pouch (WP) cells of the wing disc, and hinge structures, which are formed by cells immediately proximal to the WP.Wing development proceeds through a series of steps in which regions of fates are specified. Discs begin development composed of cells with either anterior (A) or posterior (P) identity and subsequently undergo several subdivisions. Early in the second larval instar (L2), the action of Wingless (Wg) and the EGF receptor divide the wing disc into large domains that define the body wall and wing (Wang et al. 2000;Zecca and Struhl 2002).

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Section: Discussionsupporting

confidence: 74%

Section: Resultsmentioning

confidence: 88%

mentioning

confidence: 99%

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Control of Wing Size and Proportions by Drosophila Myc

Wu¹,

Johnston

2010

Genetics

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“…Among the first connections between Wnt signaling and miRNAs, was the observation that impairment of Wnt signaling in Drosophila melanogaster fly larvae led to increased activity of the bantam miRNA (Brennecke et al, 2003). The regulatory mechanism was not further defined, but a subsequent study suggested that it depended on modulation of Notch activity (Herranz et al, 2008). In another developmental setting, ectopic stimulation of Wnt signaling in Xenopus laevis frog embryos led to decreased miR-15/-16 levels (Martello et al, 2007).…”

Section: Introductionmentioning

confidence: 99%

Attenuation of the beta-catenin/TCF4 complex in colorectal cancer cells induces several growth-suppressive microRNAs that target cancer promoting genes

et al. 2011

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“…Likewise, ban is regulated by a growing number of genes. For example, Notch signaling inhibits ban expression in the wing disc [78]. ban is also a target of the Hippo pathway [27–29], making it an ideal candidate for mediating crosstalk between different signaling pathways.…”

Section: Discussionmentioning

confidence: 99%

bantam microRNA is a negative regulator of the Drosophila decapentaplegic pathway

Kane

Vora

Padgett

et al. 2018

Fly

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Decapentaplegic (Dpp), the Drosophila homolog of the vertebrate bone morphogenetic protein (BMP2/4), is crucial for patterning and growth in many developmental contexts. The Dpp pathway is regulated at many different levels to exquisitely control its activity. We show that bantam (ban), a microRNA, modulates Dpp signaling activity. Over expression of ban decreases phosphorylated Mothers against decapentaplegic (Mad) levels and negatively affects Dpp pathway transcriptional target genes, while null mutant clones of ban upregulate the pathway. We provide evidence that dpp upregulates ban in the wing imaginal disc, and attenuation of Dpp signaling results in a reduction of ban expression, showing that they function in a feedback loop. Furthermore, we show that this feedback loop is important for maintaining anterior-posterior compartment boundary stability in the wing disc through regulation of optomotor blind (omb), a known target of the pathway. Our results support a model that ban functions with dpp in a negative feedback loop.

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A Wingless and Notch double-repression mechanism regulates G1–S transition in the Drosophila wing

Cited by 99 publications

References 48 publications

Control of Wing Size and Proportions by Drosophila Myc

Control of Wing Size and Proportions by Drosophila Myc

Attenuation of the beta-catenin/TCF4 complex in colorectal cancer cells induces several growth-suppressive microRNAs that target cancer promoting genes

bantam microRNA is a negative regulator of the Drosophila decapentaplegic pathway

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