Literature DB >> 16291791

Growth and cell survival are unevenly impaired in pixie mutant wing discs.

Carmen M A Coelho1, Benjamin Kolevski, Caroline Bunn, Cherryl Walker, Anupama Dahanukar, Sally J Leevers.   

Abstract

It is largely unknown how growth slows and then stops in vivo. Similar to most organs, Drosophila imaginal discs undergo a fast, near-exponential growth phase followed by a slow growth phase before final target size is reached. We have used a genetic approach to study the role of an ABC-E protein, Pixie, in wing disc growth. pixie mutants, like mutants in ribosomal proteins genes (known as Minutes), show severe developmental delay with relatively mild alterations in final body size. Intriguingly, pixie mutant wing imaginal discs show complex regional and temporal defects in growth and cell survival that are compensated to result in near-normal final size. In S2 cells, Pixie, like its yeast homolog RLI1, is required for translation. However, a comparison of the growth of eukaryotic translation initiation factor eIF4A and pixie mutant clones in wing discs suggests that only a subset of translation regulators, including pixie, mediate regional differences in growth and cell survival in wing discs. Interestingly, some of the regional effects on pixie mutant clone growth are enhanced in a Minute background. Our results suggest that the role of Pixie is not merely to allow growth, as might be expected for a translation regulator. Instead, Pixie also behaves as a target of putative constraining signals that slow disc growth during late larval life. We propose a model in which a balance of growth inhibitors and promoters determines tissue growth rates and cell survival. An alteration in this balance slows growth before final disc size is reached.

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Year:  2005        PMID: 16291791     DOI: 10.1242/dev.02148

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


  15 in total

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2.  p53-independent apoptosis limits DNA damage-induced aneuploidy.

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4.  ABCE1 is essential for S phase progression in human cells.

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Journal:  Cell Cycle       Date:  2016-03-17       Impact factor: 4.534

5.  Structural basis of highly conserved ribosome recycling in eukaryotes and archaea.

Authors:  Thomas Becker; Sibylle Franckenberg; Stephan Wickles; Christopher J Shoemaker; Andreas M Anger; Jean-Paul Armache; Heidemarie Sieber; Charlotte Ungewickell; Otto Berninghausen; Ingo Daberkow; Annette Karcher; Michael Thomm; Karl-Peter Hopfner; Rachel Green; Roland Beckmann
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6.  Chronic activation of JNK JAK/STAT and oxidative stress signalling causes the loser cell status.

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7.  The translation factors of Drosophila melanogaster.

Authors:  Steven J Marygold; Helen Attrill; Paul Lasko
Journal:  Fly (Austin)       Date:  2016-08-05       Impact factor: 2.160

Review 8.  ABCE Proteins: From Molecules to Development.

Authors:  Carla Navarro-Quiles; Eduardo Mateo-Bonmatí; José L Micol
Journal:  Front Plant Sci       Date:  2018-08-03       Impact factor: 5.753

9.  Ribosome recycling is coordinated by processive events in two asymmetric ATP sites of ABCE1.

Authors:  Elina Nürenberg-Goloub; Holger Heinemann; Milan Gerovac; Robert Tampé
Journal:  Life Sci Alliance       Date:  2018-06-14

10.  A tumor suppressor activity of Drosophila Polycomb genes mediated by JAK-STAT signaling.

Authors:  Anne-Kathrin Classen; Brandon D Bunker; Kieran F Harvey; Thomas Vaccari; David Bilder
Journal:  Nat Genet       Date:  2009-09-13       Impact factor: 38.330

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