Cytoplasmic and nuclear distribution of the protein complexes mTORC1 and mTORC2: rapamycin triggers dephosphorylation and delocalization of the mTORC2 components rictor and sin1

doi:10.1093/hmg/ddn192

Human Molecular Genetics Advance Access originally published online on July 8, 2008
Human Molecular Genetics 2008 17(19):2934-2948; doi:10.1093/hmg/ddn192

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Cytoplasmic and nuclear distribution of the protein complexes mTORC1 and mTORC2: rapamycin triggers dephosphorylation and delocalization of the mTORC2 components rictor and sin1

Margit Rosner and Markus Hengstschläger^*

Medical Genetics, Medical University of Vienna, Währinger Gürtel 18–20, 1090 Vienna, Austria

^* To whom correspondence should be addressed. Tel: +43 1404007847; Fax: +43 1404007848; Email: markus.hengstschlaeger{at}meduniwien.ac.at

Received June 6, 2008; Accepted July 3, 2008

The mammalian target of rapamycin (mTOR) is part of two distinctcomplexes, mTORC1, containing raptor and mLST8, and mTORC2,containing rictor, mLST8 and sin1. Although great endeavorshave already been made to elucidate the function and regulationof mTOR, the cytoplasmic nuclear distribution of the mTOR complexesis unknown. Upon establishment of the proper experimental conditions,we found mTOR, mLST8, rictor and sin1 to be less abundant inthe nucleus than in the cytoplasm of non-transformed, non-immortalized,diploid human primary fibroblasts. Although raptor is also highabundant in the nucleus, the mTOR/raptor complex is predominantlycytoplasmic, whereas the mTOR/rictor complex is abundant inboth compartments. Rapamycin negatively regulates the formationof both mTOR complexes, but the molecular mechanism of its effectson mTORC2 remained elusive. We describe that in primary cellsshort-term treatment with rapamycin triggers dephosphorylationof rictor and sin1 exclusively in the cytoplasm, but does notaffect mTORC2 assembly. Prolonged drug treatment leads to completedephosphorylation and cytoplasmic translocation of nuclear rictorand sin1 accompanied by inhibition of mTORC2 assembly. The distinctcytoplasmic and nuclear upstream and downstream effectors ofmTOR are involved in many cancers and human genetic diseases,such as tuberous sclerosis, Peutz–Jeghers syndrome, vonHippel–Lindau disease, neurofibromatosis type 1, polycystickidney disease, Alzheimer's disease, cardiac hypertrophy, obesityand diabetes. Accordingly, analogs of rapamycin are currentlytested in many different clinical trials. Our data allow newinsights into the molecular consequences of mTOR dysregulationunder pathophysiological conditions and should help to optimizerapamycin treatment of human diseases.

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