KSR is a scaffold required for activation of the ERK/MAPK module

Roy, François; Laberge, Gino; Douziech, Mélanie; Ferland-McCollough, David; Therrien, Marc

doi:10.1101/gad.962902

Cited by 196 publications

(186 citation statements)

References 40 publications

(86 reference statements)

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“…KSR1 may be most important as a scaffold due to its ability to bind simultaneously to components at each level of the MAPK cascade (MAP3K, MAP2K, and MAPK). Because signaling is diminished if it is expressed in excess of its binding partners, KSR1 fits the characteristics of a scaffold [27,30,32]. A functional catalytic lysine appears to be absent from KSR, unlike what we found in WNK protein kinases; in WNKs the catalytic lysine is not in the canonical position, but it is nearby in a distinct structural element [33].…”

Section: Kinase Suppressor Of Rascontrasting

confidence: 49%

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Signal control through Raf: in sickness and in health

2011

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The extracellular signal-regulated kinase 1/2 (ERK1/2) cascade is the prototype mammalian mitogenactivated protein kinase (MAPK) signaling cascade that regulates a number of processes, including proliferation, differentiation, survival, migration, stress responses and apoptosis. How this seemingly linear cascade is modulated to achieve a specific cellular function has been a main focus of the field. In this review, we describe new as well as old findings in the regulation of the ERK1/2 pathway in normal and disease states via MAP3Ks.

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Section: Kinase Suppressor Of Rascontrasting

confidence: 49%

“…The relevance of the catalytic activity of KSR proteins is in debate [27][28][29][30][31]. KSRs contain arginine instead of the invariant catalytic lysine in the N-terminal region of the kinase domain present in other protein kinases.…”

Section: Kinase Suppressor Of Rasmentioning

confidence: 99%

Signal control through Raf: in sickness and in health

2011

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“…This raises the question of how specificity of a certain MAPK-mediated response can be achieved. Scaffolding proteins that support the formation of a particular MAPKKK-MAPKK-MAPK complex are known from yeast (Saccharomyces cerevisiae; O'Rourke and Herskowitz, 1998) and animals (Roy et al, 2002). MAPK modules with scaffolding function have also recently been identified in plants.…”

Section: Are Ros the Missing Link Between Mapks And Stress Signaling?mentioning

confidence: 99%

Mitogen-Activated Protein Kinases and Reactive Oxygen Species Signaling in Plants

2006

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“…Fus3 is predominantly nuclear, whereas Ste7 and Ste11 are cytoplasmic van Drogen et al, 2001), raising the possibility that nuclear shuttling helps Ste5 to assemble a signaling complex. Interestingly, the kinase suppressor of Ras scaffold also links MAPK cascade kinases (Raf, extracellular signal-regulated kinase kinase, extracellular signal-regulated kinase) to a membranelinked anchor (Ras) (Nguyen et al, 2002;Roy et al, 2002) and shuttles through the nucleus (Brennan et al, 2002), suggesting that multiple aspects of Ste5 localization are conserved.…”

Section: Introductionmentioning

confidence: 99%

“…The Ste5 scaffold of budding yeast is the prototype of a family of proteins that tether kinases of mitogen-activated protein kinase (MAPK) cascades in eukaryotes (Elion, 1995(Elion, , 2001Burack and Shaw, 2000;Nguyen et al, 2002;Roy et al, 2002). Ste5 assembles the mating pathway kinases Ste11 (MAPKKK), Ste7 (MAPKK), and Fus3 (MAPK) into an active signaling complex of high specific activity (Kranz et al, 1994;Choi et al, 1994; by binding the kinases through separate binding sites ( Figure 1A; Choi et al, 1994;Inouye et al, 1997b).…”

Section: Introductionmentioning

confidence: 99%

Nuclear Export and Plasma Membrane Recruitment of the Ste5 Scaffold Are Coordinated with Oligomerization and Association with Signal Transduction Components

Wang

Elion

2003

MBoC

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The Ste5 scaffold activates an associated mitogen-activated protein kinase cascade by binding through its RING-H2 domain to a G␤␥ dimer (Ste4/Ste18) at the plasma membrane in a recruitment event that requires prior nuclear shuttling of Ste5. Genetic evidence suggests that Ste5 must oligomerize to function, but its impact on Ste5 function and localization is unknown. Herein, we show that oligomerization affects Ste5 activity and localization. The majority of Ste5 is monomeric, suggesting that oligomerization is tightly regulated. Increasing the pool of Ste5 oligomers increases association with Ste11. Remarkably, Ste5 oligomers are also more efficiently exported from the nucleus, retained in the cytoplasm by Ste11 and better recruited to the plasma membrane, resulting in constitutive activation of the mating mitogen-activated protein kinase cascade. Coprecipitation tests show that the RING-H2 domain is the key determinant of oligomerization. Mutational analysis suggests that the leucine-rich domain limits the accessibility of the RING-H2 domain and inhibits export and recruitment in addition to promoting Ste11 association and activation. Our results suggest that the major form of Ste5 is an inactive monomer with an inaccessible RING-H2 domain and Ste11 binding site, whereas the active form is an oligomer that is more efficiently exported and recruited and has a more accessible RING-H2 domain and Ste11 binding site.

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KSR is a scaffold required for activation of the ERK/MAPK module

Cited by 196 publications

References 40 publications

Signal control through Raf: in sickness and in health

Signal control through Raf: in sickness and in health

Mitogen-Activated Protein Kinases and Reactive Oxygen Species Signaling in Plants

Nuclear Export and Plasma Membrane Recruitment of the Ste5 Scaffold Are Coordinated with Oligomerization and Association with Signal Transduction Components

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