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Mitochondrial dysfunction generates a growth-restraining signal linked to pyruvate in Drosophila larvae.


ABSTRACT: The Drosophila bang-sensitive mutant tko25t, manifesting a global deficiency in oxidative phosphorylation due to a mitochondrial protein synthesis defect, exhibits a pronounced delay in larval development. We previously identified a number of metabolic abnormalities in tko25t larvae, including elevated pyruvate and lactate, and found the larval gut to be a crucial tissue for the regulation of larval growth in the mutant. Here we established that expression of wild-type tko in any of several other tissues of tko25t also partially alleviates developmental delay. The effects appeared to be additive, whilst knockdown of tko in a variety of specific tissues phenocopied tko25t, producing developmental delay and bang-sensitivity. These findings imply the existence of a systemic signal regulating growth in response to mitochondrial dysfunction. Drugs and RNAi-targeted on pyruvate metabolism interacted with tko25t in ways that implicated pyruvate or one of its metabolic derivatives in playing a central role in generating such a signal. RNA-seq revealed that dietary pyruvate-induced changes in transcript representation were mostly non-coherent with those produced by tko25t or high-sugar, consistent with the idea that growth regulation operates primarily at the translational and/or metabolic level.

SUBMITTER: George J 

PROVIDER: S-EPMC6988875 | biostudies-literature | 2019 Mar - Dec

REPOSITORIES: biostudies-literature

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Mitochondrial dysfunction generates a growth-restraining signal linked to pyruvate in <i>Drosophila</i> larvae.

George Jack J   Tuomela Tea T   Kemppainen Esko E   Nurminen Antti A   Braun Samuel S   Yalgin Cagri C   Jacobs Howard T HT  

Fly 20190301 1-4


The <i>Drosophila</i> bang-sensitive mutant <i>tko<sup>25t</sup></i>, manifesting a global deficiency in oxidative phosphorylation due to a mitochondrial protein synthesis defect, exhibits a pronounced delay in larval development. We previously identified a number of metabolic abnormalities in <i>tko<sup>25t</sup></i> larvae, including elevated pyruvate and lactate, and found the larval gut to be a crucial tissue for the regulation of larval growth in the mutant. Here we established that express  ...[more]

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