Cell
Volume 147, Issue 1, 30 September 2011, Pages 223-234
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Article
Beclin1 Controls the Levels of p53 by Regulating the Deubiquitination Activity of USP10 and USP13

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Summary

Autophagy is an important intracellular catabolic mechanism that mediates the degradation of cytoplasmic proteins and organelles. We report a potent small molecule inhibitor of autophagy named “spautin-1” for specific and potent autophagy inhibitor-1. Spautin-1 promotes the degradation of Vps34 PI3 kinase complexes by inhibiting two ubiquitin-specific peptidases, USP10 and USP13, that target the Beclin1 subunit of Vps34 complexes. Beclin1 is a tumor suppressor and frequently monoallelically lost in human cancers. Interestingly, Beclin1 also controls the protein stabilities of USP10 and USP13 by regulating their deubiquitinating activities. Since USP10 mediates the deubiquitination of p53, regulating deubiquitination activity of USP10 and USP13 by Beclin1 provides a mechanism for Beclin1 to control the levels of p53. Our study provides a molecular mechanism involving protein deubiquitination that connects two important tumor suppressors, p53 and Beclin1, and a potent small molecule inhibitor of autophagy as a possible lead compound for developing anticancer drugs.

Highlights

► Spautin-1 inhibits autophagy, targeting ubiquitin-specific proteases USP10 and USP13 ► USP10 and USP13 deubiquitinate Beclin1 to regulate Vps34, a class III PI3 kinase ► In turn, Beclin1 and Vps34 regulates USP10 and USP13 activity ► Beclin1/Vps34 are tumor suppressors that modulate levels of p53, a USP10 target

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5

These authors contributed equally to this work

6

These authors contributed equally to this work