Drosophila ribosomal protein mutants control tissue growth non-autonomously via effects on the prothoracic gland and ecdysone

Jane I. Lin, Naomi C. Mitchell, Marina Kalcina, Elly Tchoubrieva, Mary J. Stewart, Steven J. Marygold, Cherryl D. Walker, George Thomas, Sally J. Leevers, Richard B. Pearson, Leonie M. Quinn, Ross D. Hannan

Research output: Contribution to journalArticlepeer-review

30 Citations (Scopus)

Abstract

The ribosome is critical for all aspects of cell growth due to its essential role in protein synthesis. Paradoxically, many Ribosomal proteins (Rps) act as tumour suppressors in Drosophila and vertebrates. To examine how reductions in Rps could lead to tissue overgrowth, we took advantage of the observation that an RpS6 mutant dominantly suppresses the small rough eye phenotype in a cyclin E hypomorphic mutant (cycE JP). We demonstrated that the suppression of cycE JP by the RpS6 mutant is not a consequence of restoring CycE protein levels or activity in the eye imaginal tissue. Rather, the use of UAS-RpS6 RNAi transgenics revealed that the suppression of cycE JP is exerted via a mechanism extrinsic to the eye, whereby reduced Rp levels in the prothoracic gland decreases the activity of ecdysone, the steroid hormone, delaying developmental timing and hence allowing time for tissue and organ overgrowth. These data provide for the first time a rationale to explain the counter-intuitive organ overgrowth phenotypes observed for certain members of the Minute class of Drosophila Rp mutants. They also demonstrate how Rp mutants can affect growth and development cell non-autonomously.

Original languageEnglish
Article numbere1002408
JournalPLoS Genetics
Volume7
Issue number12
DOIs
Publication statusPublished - Dec 2011
Externally publishedYes

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