共 42 条
FoxO3 controls autophagy in skeletal muscle in vivo
被引:1637
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Romanello, Vanina
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机构: Venet Inst Mol Med, Padua 35129, Italy

Masiero, Eva
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机构: Venet Inst Mol Med, Padua 35129, Italy

Rudolf, Ruediger
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机构: Venet Inst Mol Med, Padua 35129, Italy

Del Piccolo, Paola
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机构: Venet Inst Mol Med, Padua 35129, Italy

Burden, Steven J.
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机构: Venet Inst Mol Med, Padua 35129, Italy

Di Lisi, Raffaella
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机构: Venet Inst Mol Med, Padua 35129, Italy

Sandri, Claudia
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机构: Venet Inst Mol Med, Padua 35129, Italy

Zhao, Jinghui
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机构: Venet Inst Mol Med, Padua 35129, Italy

Goldberg, Alfred L.
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机构: Venet Inst Mol Med, Padua 35129, Italy

Schiaffino, Stefano
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机构: Venet Inst Mol Med, Padua 35129, Italy

Sandri, Marco
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Venet Inst Mol Med, Padua 35129, Italy Venet Inst Mol Med, Padua 35129, Italy
机构:
[1] Venet Inst Mol Med, Padua 35129, Italy
[2] Univ Padua, Dept Biomed Sci, I-35121 Padua, Italy
[3] Dulbecco Telethon Inst, I-35129 Padua, Italy
[4] Forschungszentrum Karlsruhe, Inst Toxicol & Genet, D-76021 Karlsruhe, Germany
[5] NYU, Sch Med, Skirball Inst Biomol Med, New York, NY 10016 USA
[6] Harvard Univ, Harvard Med Sch, Dept Cell Biol, Boston, MA 02115 USA
[7] Inst Neurosci, Consiglio Nazl Ric, I-35121 Padua, Italy
关键词:
D O I:
10.1016/j.cmet.2007.11.001
中图分类号:
Q2 [细胞生物学];
学科分类号:
071009 ;
090102 ;
摘要:
Autophagy allows cell survival during starvation through the bulk degradation of proteins and organelles by lysosomal enzymes. However, the mechanisms responsible for the induction and regulation of the autophagy program are poorly understood. Here we show that the FoxO3 transcription factor, which plays a critical role in muscle atrophy, is necessary and sufficient for the induction of autophagy in skeletal muscle in vivo. Akt/PKB activation blocks FoxO3 activation and autophagy, and this effect is not prevented by rapamycin. FoxO3 controls the transcription of autophagy-related genes, including LC3 and Bnip3, and Bnip3 appears to mediate the effect of FoxO3 on autophagy. This effect is not prevented by proteasome inhibitors. Thus, FoxO3 controls the two major systems of protein breakdown in skeletal muscle, the ubiquitin-proteasomal and autophagic/lysosomal pathways, independently. These findings point to FoxO3 and Bnip3 as potential therapeutic targets in muscle wasting disorders and other degenerative and neoplastic diseases in which autophagy is involved.
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页码:458 / 471
页数:14
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