An Acylation Cycle Regulates Localization and Activity of Palmitoylated Ras Isoforms

Rocks, Oliver; Peyker, Anna; Kahms, Martin; Verveer, Peter J.; Koerner, Carolin; Lumbierres, María; Kuhlmann, Jürgen; Waldmann, Herbert; Wittinghofer, Alfred; Bastiaens, Philippe I. H.

doi:10.1126/science.1105654

Cited by 767 publications

(806 citation statements)

References 38 publications

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“…Inhibition of the palmitoylation/de-palmitoylation cycle prevented accumulation and activation of H-Ras on the Golgi [64]. In this model Ras activation stimulates depalmitoylation and traffic to the Golgi where a new and distinct pool of effectors may be subsequently activated.…”

Section: Compartmentalised Ras Signallingmentioning

confidence: 91%

“…Several advanced fluorescence based approaches [89]. Some studies have revealed endomembrane Ras activation in addition to the cell surface pool [64,[90][91][92][93], whilst others only detect plasma membranelocalised Ras activation [94][95][96]. One criticism of the evidence for endomembranous Ras activation is that it is normally seen only with over-expression of Ras.…”

Section: Compartmentalised Ras Signallingmentioning

confidence: 99%

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Ras proteins: paradigms for compartmentalised and isoform-specific signalling

Omerovic

Laude

Prior

2007

Cell. Mol. Life Sci.

113

122

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Ras GTPases mediate a wide variety of cellular processes by converting a multitude of extracellular stimuli into specific biological responses including proliferation, differentiation and survival. In mammalian cells, three ras genes encode four Ras isoforms (H-Ras, K-Ras4A, KRas4B and N-Ras) that are highly homologous but functionally distinct. Differences between the isoforms, including their post-translational modifications and intracellular sorting, mean that Ras has emerged as an important model system of compartmentalised signalling and membrane biology. Ras isoforms in different subcellular locations are proposed to recruit distinct upstream and downstream accessory proteins and activate multiple signalling pathways. Here, we summarise data relating to isoform specific signalling, its role in disease and the mechanisms promoting compartmentalised signalling. Further understanding of this field will reveal the role of Ras signalling in development, cellular homeostasis and cancers and may suggest new therapeutic approaches.

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Section: Compartmentalised Ras Signallingmentioning

confidence: 91%

Section: Compartmentalised Ras Signallingmentioning

confidence: 99%

Ras proteins: paradigms for compartmentalised and isoform-specific signalling

Omerovic

Laude

Prior

2007

Cell. Mol. Life Sci.

113

122

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“…2). [25,26] Non-palmitoylated K-Ras4B also traffics back and forth from the PM, although by other mechanisms: phosphorylation of K-Ras4B by PKC promotes its release from the PM and its transfer to mitochondria. [27] Calmodulin binding to K-Ras4B also dislodges it from the PM, facilitating its translocation to the GC and to early endosomes.…”

Section: Ras: An Actor On Many Stagesmentioning

confidence: 99%

The Ras‐ERK pathway: Understanding site‐specific signaling provides hope of new anti‐tumor therapies

2010

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Recent discoveries have suggested the concept that intracellular signals are the sum of multiple, site-specified subsignals, rather than single, homogeneous entities. In the context of cancer, searching for compounds that selectively block subsignals essential for tumor progression, but not those regulating ''house-keeping'' functions, could help in producing drugs with reduced side effects compared to compounds that block signaling completely. The Ras-ERK pathway has become a paradigm of how space can differentially shape signaling. Today, we know that Ras proteins are found in different plasma membrane microdomains and endomembranes. At these localizations, Ras is subject to site-specific regulatory mechanisms, distinctively engaging effector pathways and switching-on diverse genetic programs to generate different biological responses. The Ras effector pathway leading to ERKs activation is also under strict, space-related regulatory processes. These findings may open a gate for aiming at the Ras-ERK pathway in a spatially restricted fashion, in our quest for new anti-tumor therapies.

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“…These isoforms of Ras diVer mainly in their C-terminal membrane anchors that determine cellular localization and micro-localization within membranes (Rocks et al 2006). For instance, within the whole cell an acylation cycle dynamically partitions H-Ras between the plasma membrane and the Golgi (Rocks et al 2005). On the other hand K-Ras is not subject to such an acylation cycle but its association with the plasma membrane is regulated via phosphorylation (Bivona et al 2006).…”

Section: Signaling Via Protein Clusters In the Plasma Membranementioning

confidence: 99%

Quantitative microscopy and systems biology: seeing the whole picture

Verveer

Bastiaens

2008

Histochem Cell Biol

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Understanding cellular function requires studying the spatially resolved dynamics of protein networks. From the isolated proteins we can only learn about their individual properties, but by investigating their behavior in their natural environment, the cell, we obtain information about the overall response properties of the network module in which they operate. Fluorescence microscopy methods provide currently the only tools to study the dynamics of molecular processes in living cells with high temporal and spatial resolution. Combined with computational approaches they allow us to obtain insights in the reactiondiVusion processes that determine biological function on the scale of cells.

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An Acylation Cycle Regulates Localization and Activity of Palmitoylated Ras Isoforms

Cited by 767 publications

References 38 publications

Ras proteins: paradigms for compartmentalised and isoform-specific signalling

Ras proteins: paradigms for compartmentalised and isoform-specific signalling

The Ras‐ERK pathway: Understanding site‐specific signaling provides hope of new anti‐tumor therapies

Quantitative microscopy and systems biology: seeing the whole picture

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