Caenorhabditis elegans eyes absent ortholog EYA-1 Is required for stress resistance

被引:0
作者
Bing-ying Wang
Xue-song Xu
Yu-xiao Cui
Hua Wang
Ge Liu
Zhizhuang Joe Zhao
Jun-feng Ma
Xue-qi Fu
机构
[1] Jilin University,The State Engineering Laboratory of AIDS Vaccine
[2] Jilin University,Key Laboratory for Molecular Enzymology and Engineering, Ministry of Education
[3] Jilin University,China
[4] University of Oklahoma Health Sciences Center,Japan Union Hospital
来源
Biochemistry (Moscow) | 2014年 / 79卷
关键词
EYA-1; RNA interference; stress resistance;
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摘要
Eyes absent (Eya) is a highly conserved transcription cofactor and protein phosphatase that regulates multiple developmental processes throughout the metazoans. It is a dual function protein, working as a transcription factor in the nucleus and as a tyrosine phosphatase in the cytoplasm. In this study, we isolated EYA-1 of Caenorhabditis elegans, the only homolog of Eyes absent, and set up an effective feeding-based RNAi (RNA interference) against the gene. We found that knockdown of EYA-1 decreased heat and oxidative stress tolerance and accelerated the onset of paralysis mediated by Aβ1-42 proteotoxicity and polyQ. Under heat stress (35°C), EYA-1 knockdown shortened the mean lifespan by 16.8%, which could be attributed to decrease in heat shock protein-16.2 (hsp-16.2) expression. Under oxidative stress, EYA-1 knockdown could shorten the mean lifespan by 18.7%, which could be attributed to intracellular ROS accumulation and the decrease of superoxide dismutase-3 (sod-3) protein expression. Moreover, EYA-1 knockdown animals also showed increased lipofuscin accumulation under oxidative stress. Further studies demonstrated that EYA-1 knockdown could not inhibit daf-16 nuclear accumulation in wild-type worms in response to stress. On the other hand, EYA-1 deficiency did not further reduce stress resistance of daf-16 mutants, which are stress sensitive. Quantitative real-time PCR results also showed that the expression of two daf-16 target genes, hsp-12.3 and sod-3, was downregulated in EYA-1 RNAi-treated worms under stress. All this evidence indicates EYA-1 is required for stress resistance of worms, and it might act downstream of daf-16 to regulate expression of stress resistance-associated genes.
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页码:653 / 662
页数:9
相关论文
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