The protein kinase TOR (target of rapamycin) is a key regulator of cell growth and metabolism with significant clinical relevance. In mammals, TOR signals through two distinct multi-protein complexes, mTORC1 and mTORC2 (mammalian TOR complex 1 and 2 respectively), the subunits of which appear to define the operational pathways. Rapamycin selectively targets mTORC1 function, and the emergence of specific ATP-competitive kinase inhibitors has enabled assessment of dual mTORC1 and mTORC2 blockade. Little is known, however, of the molecular action of mTORC2 components or the relative importance of targeting this pathway. In the present study, we have identified the mTORC2 subunit Sin1 as a direct binding partner of the PKC (protein kinase C) ϵ kinase domain and map the interaction to the central highly conserved region of Sin1. Exploiting the conformational dependence for PKC phosphorylation, we demonstrate that mTORC2 is essential for acute priming of PKC. Inducible expression of Sin1 mutants, lacking the PKC-interaction domain, displaces endogenous Sin1 from mTORC2 and disrupts PKC phosphorylation. PKB (protein kinase B)/Akt phosphorylation is also suppressed by these Sin1 mutants, but not the mTORC1 substrate p70S6K (S6 kinase), providing evidence that Sin1 serves as a selectivity adaptor for the recruitment of mTORC2 targets. This inducible selective mTORC2 intervention is used to demonstrate a key role for mTORC2 in cell proliferation in three-dimensional culture.
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October 2011
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Research Article|
September 28 2011
mTORC2 targets AGC kinases through Sin1-dependent recruitment
Angus J. M. Cameron;
Angus J. M. Cameron
*Protein Phosphorylation Laboratory, Cancer Research UK, London Research Institute, Lincoln's Inn Fields Laboratories, 44 Lincoln's Inn Fields, London WC2A 3LY, U.K.
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Mark D. Linch;
Mark D. Linch
*Protein Phosphorylation Laboratory, Cancer Research UK, London Research Institute, Lincoln's Inn Fields Laboratories, 44 Lincoln's Inn Fields, London WC2A 3LY, U.K.
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Adrian T. Saurin;
Adrian T. Saurin
1
*Protein Phosphorylation Laboratory, Cancer Research UK, London Research Institute, Lincoln's Inn Fields Laboratories, 44 Lincoln's Inn Fields, London WC2A 3LY, U.K.
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Cristina Escribano;
Cristina Escribano
2
*Protein Phosphorylation Laboratory, Cancer Research UK, London Research Institute, Lincoln's Inn Fields Laboratories, 44 Lincoln's Inn Fields, London WC2A 3LY, U.K.
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Peter J. Parker
Peter J. Parker
3
*Protein Phosphorylation Laboratory, Cancer Research UK, London Research Institute, Lincoln's Inn Fields Laboratories, 44 Lincoln's Inn Fields, London WC2A 3LY, U.K.
†Division of Cancer Studies, King's College London, New Hunt's House, St Thomas Street, London SE1 1UL, U.K.
3To whom correspondence should be addressed (email [email protected]).
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Publisher: Portland Press Ltd
Received:
April 14 2011
Revision Received:
July 27 2011
Accepted:
August 01 2011
Accepted Manuscript online:
August 01 2011
Online ISSN: 1470-8728
Print ISSN: 0264-6021
© The Authors Journal compilation © 2011 Biochemical Society
2011
Biochem J (2011) 439 (2): 287–297.
Article history
Received:
April 14 2011
Revision Received:
July 27 2011
Accepted:
August 01 2011
Accepted Manuscript online:
August 01 2011
Citation
Angus J. M. Cameron, Mark D. Linch, Adrian T. Saurin, Cristina Escribano, Peter J. Parker; mTORC2 targets AGC kinases through Sin1-dependent recruitment. Biochem J 15 October 2011; 439 (2): 287–297. doi: https://doi.org/10.1042/BJ20110678
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