TORC1 Inhibition by Rapamycin Promotes Antioxidant Defences in a Drosophila Model of Friedreich’s Ataxia

6533b7defe1ef96bd1275e5a

RESEARCH PRODUCT

TORC1 Inhibition by Rapamycin Promotes Antioxidant Defences in a Drosophila Model of Friedreich’s Ataxia

Pablo Calap-quintana María Dolores Moltó Sirena Soriano Sirena Soriano Juan Botas Ismael Al-ramahi José Vicente Llorens M. J. Martínez-sebastián

subject

Male lcsh:Medicine Gene Expression medicine.disease_cause Antioxidants Animals Genetically Modified Adenosine Triphosphate 0302 clinical medicine RNA interference Iron-Binding Proteins Malondialdehyde Drosophila Proteins lcsh:Science Aconitate Hydratase Genetics 0303 health sciences Multidisciplinary Reverse Transcriptase Polymerase Chain Reaction Glutathione 3. Good health Cell biology Drosophila melanogaster RNA Interference medicine.symptom Immunosuppressive Agents Drosophila Protein Research Article Ataxia Longevity Motor Activity Biology Aconitase 03 medical and health sciences medicine Animals Humans 030304 developmental biology Sirolimus Aldehydes Superoxide Dismutase lcsh:R Autophagy Repressor Proteins Disease Models Animal Oxidative Stress Friedreich Ataxia Frataxin biology.protein lcsh:Q 030217 neurology & neurosurgery Oxidative stress Transcription Factors Genetic screen

description

Friedreich's ataxia (FRDA), the most common inherited ataxia in the Caucasian population, is a multisystemic disease caused by a significant decrease in the frataxin level. To identify genes capable of modifying the severity of the symptoms of frataxin depletion, we performed a candidate genetic screen in a Drosophila RNAi-based model of FRDA. We found that genetic reduction in TOR Complex 1 (TORC1) signalling improves the impaired motor performance phenotype of FRDA model flies. Pharmacologic inhibition of TORC1 signalling by rapamycin also restored this phenotype and increased the lifespan and ATP levels. Furthermore, rapamycin reduced the altered levels of malondialdehyde + 4-hydroxyalkenals and total glutathione of the model flies. The rapamycin-mediated protection against oxidative stress is due in part to an increase in the transcription of antioxidant genes mediated by cap-n-collar (Drosophila ortholog of Nrf2). Our results suggest that autophagy is indeed necessary for the protective effect of rapamycin in hyperoxia. Rapamycin increased the survival and aconitase activity of model flies subjected to high oxidative insult, and this improvement was abolished by the autophagy inhibitor 3-methyladenine. These results point to the TORC1 pathway as a new potential therapeutic target for FRDA and as a guide to finding new promising molecules for disease treatment.

year	journal	country	edition	language
2015-07-01	PLOS ONE

https://doi.org/10.1371/journal.pone.0132376