Ras GTPases undergo post-translational modifications that govern their subcellular trafficking and localization. In particular, palmitoylation of the Golgi tags N-Ras and H-Ras for exocytotic transport and residency at the PM (plasma membrane). Following depalmitoylation, PM-Ras redistributes to all subcellular membranes causing an accumulation of palmitate-free Ras at endomembranes, including the Golgi and endoplasmic reticulum. Palmitoylation is unanimously regarded as a critical modification at the crossroads of Ras activity and trafficking control, but its precise relevance to native wild-type Ras function in growth factor signalling is unknown. We show in the present study by use of palmitoylation-deficient N-Ras mutants and via the analysis of palmitate content of agonist-activated GTP-loaded N-Ras that only palmitoylated N-Ras becomes activated by agonists. In line with an essential role of palmitoylation in Ras activation, dominant-negative RasS17N loses its blocking potency if rendered devoid of palmitoylation. Live-cell Ras–GTP imaging shows that N-Ras activation proceeds only at the PM, consistent with activated N-Ras–GTP being palmitoylated. Finally, palmitoylation-deficient N-Ras does not sustain EGF (epidermal growth factor) or serum-elicited mitogenic signalling, confirming that palmitoylation is essential for signal transduction by N-Ras. These findings document that N-Ras activation proceeds at the PM and suggest that depalmitoylation, by removing Ras from the PM, may contribute to the shutdown of Ras signalling.
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Research Article|
August 09 2013
Ras palmitoylation is necessary for N-Ras activation and signal propagation in growth factor signalling Available to Purchase
Shu-Ping Song;
Shu-Ping Song
1
*Institute of Molecular Cell Biology, Center for Molecular Biomedicine, University Hospital, Jena, 07745, Germany
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Anne Hennig;
Anne Hennig
1
*Institute of Molecular Cell Biology, Center for Molecular Biomedicine, University Hospital, Jena, 07745, Germany
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Katja Schubert;
Katja Schubert
†Center for Sepsis Control and Care, University Hospital, Jena, 07747, Germany
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Robby Markwart;
Robby Markwart
*Institute of Molecular Cell Biology, Center for Molecular Biomedicine, University Hospital, Jena, 07745, Germany
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Philipp Schmidt;
Philipp Schmidt
*Institute of Molecular Cell Biology, Center for Molecular Biomedicine, University Hospital, Jena, 07745, Germany
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Ian A. Prior;
Ian A. Prior
‡Physiological Laboratory, Department of Molecular and Cellular Physiology, Institute of Translational Research, University of Liverpool, Liverpool L69 3BX, U.K.
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Frank-Dietmar Böhmer;
Frank-Dietmar Böhmer
*Institute of Molecular Cell Biology, Center for Molecular Biomedicine, University Hospital, Jena, 07745, Germany
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Ignacio Rubio
Ignacio Rubio
2
*Institute of Molecular Cell Biology, Center for Molecular Biomedicine, University Hospital, Jena, 07745, Germany
†Center for Sepsis Control and Care, University Hospital, Jena, 07747, Germany
2To whom correspondence should be addressed (email [email protected]).
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Publisher: Portland Press Ltd
Received:
November 30 2012
Revision Received:
May 24 2013
Accepted:
June 12 2013
Accepted Manuscript online:
June 12 2013
Online ISSN: 1470-8728
Print ISSN: 0264-6021
© The Authors Journal compilation © 2013 Biochemical Society
2013
Biochem J (2013) 454 (2): 323–332.
Article history
Received:
November 30 2012
Revision Received:
May 24 2013
Accepted:
June 12 2013
Accepted Manuscript online:
June 12 2013
Connected Content
A correction has been published:
Ras palmitoylation is necessary for N-Ras activation and signal propagation in growth factor signalling
Citation
Shu-Ping Song, Anne Hennig, Katja Schubert, Robby Markwart, Philipp Schmidt, Ian A. Prior, Frank-Dietmar Böhmer, Ignacio Rubio; Ras palmitoylation is necessary for N-Ras activation and signal propagation in growth factor signalling. Biochem J 1 September 2013; 454 (2): 323–332. doi: https://doi.org/10.1042/BJ20121799
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