Regulation of Akt signaling activation by ubiquitination

Wei Lei Yang; Ching Yuan Wu; Juan Wu; Hui Kuan Lin

doi:10.4161/cc.9.3.10508

Regulation of Akt signaling activation by ubiquitination

Wei Lei Yang, Ching Yuan Wu, Juan Wu, Hui Kuan Lin

Research output: Contribution to journal › Review article › peer-review

117 Scopus citations

Abstract

Akt (also known as PKB) signaling orchestrates many aspects of biological functions and, importantly, its deregulation is linked to cancer development. Akt activity is well-known regulated through its phosphorylation at T308 and S473 by PDK1 and mTOrC2, respectively. Although in the last decade the research has been primarily focused on Akt phosphorylation and its role in Akt activation and functions, other posttranslational modifications on Akt have never been reported. Until very recently, a novel posttranslational modification on Akt termed ubiquitination was identified and shown to play an important role in Akt activation. The cancer-associated Akt mutant recently identified in a subset of human cancers displays enhanced Akt ubiquitination, in turn contributing to Akt hyperactivation, suggesting a potential role of Akt ubiquitination in cancers. Thus, this novel posttranslational modification on Akt reveals an exciting avenue that has advanced our current understandings of how Akt signaling activation is regulated.

Original language	English (US)
Pages (from-to)	486-497
Number of pages	12
Journal	Cell Cycle
Volume	9
Issue number	3
DOIs	https://doi.org/10.4161/cc.9.3.10508
State	Published - Feb 1 2010

Keywords

Akt
E3 ligase
Kinase
NFκB
PDK1
Phosphorylation
TRAF6
Tumorigenesis
Ubiquitination
mTORC2

ASJC Scopus subject areas

Molecular Biology
Developmental Biology
Cell Biology

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title = "Regulation of Akt signaling activation by ubiquitination",

abstract = "Akt (also known as PKB) signaling orchestrates many aspects of biological functions and, importantly, its deregulation is linked to cancer development. Akt activity is well-known regulated through its phosphorylation at T308 and S473 by PDK1 and mTOrC2, respectively. Although in the last decade the research has been primarily focused on Akt phosphorylation and its role in Akt activation and functions, other posttranslational modifications on Akt have never been reported. Until very recently, a novel posttranslational modification on Akt termed ubiquitination was identified and shown to play an important role in Akt activation. The cancer-associated Akt mutant recently identified in a subset of human cancers displays enhanced Akt ubiquitination, in turn contributing to Akt hyperactivation, suggesting a potential role of Akt ubiquitination in cancers. Thus, this novel posttranslational modification on Akt reveals an exciting avenue that has advanced our current understandings of how Akt signaling activation is regulated.",

keywords = "Akt, E3 ligase, Kinase, NFκB, PDK1, Phosphorylation, TRAF6, Tumorigenesis, Ubiquitination, mTORC2",

author = "Yang, {Wei Lei} and Wu, {Ching Yuan} and Juan Wu and Lin, {Hui Kuan}",

note = "Funding Information: We thank the members of the Lin{\textquoteright}s lab for their critical reading and comments on our manuscript. We apologize to many investigators whose important works were not cited here due to space limitations. This work is supported by M.D. Anderson Research Trust Scholar Fund to H.K. Lin, a National Science Council fund (NSC-97-2911-I-182-004-2) from Taiwan to C.Y. Wu, and a China Scholarship Council fund to J. Wu.",

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AU - Wu, Juan

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PY - 2010/2/1

Y1 - 2010/2/1

N2 - Akt (also known as PKB) signaling orchestrates many aspects of biological functions and, importantly, its deregulation is linked to cancer development. Akt activity is well-known regulated through its phosphorylation at T308 and S473 by PDK1 and mTOrC2, respectively. Although in the last decade the research has been primarily focused on Akt phosphorylation and its role in Akt activation and functions, other posttranslational modifications on Akt have never been reported. Until very recently, a novel posttranslational modification on Akt termed ubiquitination was identified and shown to play an important role in Akt activation. The cancer-associated Akt mutant recently identified in a subset of human cancers displays enhanced Akt ubiquitination, in turn contributing to Akt hyperactivation, suggesting a potential role of Akt ubiquitination in cancers. Thus, this novel posttranslational modification on Akt reveals an exciting avenue that has advanced our current understandings of how Akt signaling activation is regulated.

AB - Akt (also known as PKB) signaling orchestrates many aspects of biological functions and, importantly, its deregulation is linked to cancer development. Akt activity is well-known regulated through its phosphorylation at T308 and S473 by PDK1 and mTOrC2, respectively. Although in the last decade the research has been primarily focused on Akt phosphorylation and its role in Akt activation and functions, other posttranslational modifications on Akt have never been reported. Until very recently, a novel posttranslational modification on Akt termed ubiquitination was identified and shown to play an important role in Akt activation. The cancer-associated Akt mutant recently identified in a subset of human cancers displays enhanced Akt ubiquitination, in turn contributing to Akt hyperactivation, suggesting a potential role of Akt ubiquitination in cancers. Thus, this novel posttranslational modification on Akt reveals an exciting avenue that has advanced our current understandings of how Akt signaling activation is regulated.

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Regulation of Akt signaling activation by ubiquitination

Abstract

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