Shp2, an SH2-containing Protein-tyrosine Phosphatase, Positively Regulates Receptor Tyrosine Kinase Signaling by Dephosphorylating and Inactivating the Inhibitor Sprouty

Hanafusa, Hiroshi; Torii, Satoru; Yasunaga, Takayuki; Matsumoto, Kunihiro; Nishida, Eisuke

doi:10.1074/jbc.m312498200

Cited by 149 publications

(133 citation statements)

References 32 publications

(31 reference statements)

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“…First, by dephosphorylating binding sites on some receptors and docking proteins that mediate binding of the Ras GTPase activating protein (RasGAP), Shp-2 prevents the localization of RasGAP to the plasma membrane and thereby, prolongs Ras activation (Klinghoffer and Kazlauskas, 1995;Agazie and Hayman, 2003;Montagner et al, 2005). Second, by dephosphorylating the negative signaling modulator Sprouty, Shp-2 prevents Sprouty from binding and blocking the membrane recruitment of Grb2/Sos (Hanafusa et al, 2004). Thus, the general underlying mechanism for the positive effects exerted by Shp-2 on Ras signaling is that Shp-2 antagonizes the ability of negative regulators to access and downregulate critical enzymes involved in Ras activation.…”

Section: Integrating Signals From Rtks To Erk/mapk MM Mckay and Dk Momentioning

confidence: 99%

Integrating signals from RTKs to ERK/MAPK

2007

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Signals received at the cell surface must be properly transmitted to critical targets within the cell to achieve the appropriate biological response. This process of signal transduction is often initiated by receptor tyrosine kinases (RTKs), which function as entry points for many extracellular cues and play a critical role in recruiting the intracellular signaling cascades that orchestrate a particular response. Essential for most RTK-mediated signaling is the engagement and activation of the mitogenactivated protein kinase (MAPK) cascade comprised of the Raf, MEK and extracellular signal-regulated kinase (ERK) kinases. For many years, it was thought that signaling from RTKs to ERK occurred only at the plasma membrane and was mediated by a simple, linear Rasdependent pathway. However, the limitation of this model became apparent with the discovery that Ras and ERK can be activated at various intracellular compartments, and that RTKs can modulate Ras/ERK signaling from these sites. Moreover, ERK scaffolding proteins and signaling modulators have been identified that play critical roles in determining the strength, duration and location of RTK-mediated ERK signaling. Together, these factors contribute to the diversity of biological responses generated by RTK signaling.

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Section: Integrating Signals From Rtks To Erk/mapk MM Mckay and Dk Momentioning

confidence: 99%

Integrating signals from RTKs to ERK/MAPK

2007

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“…Also commonly noted is the binding of SOS to FRS2 via GRB2 and the subsequent activation of the RAS-MAP kinase pathway (ibid) together with CBL induced degradation (Dailey et al, 2005). It is also known that SHP2 can induce a dephosphorylation of SPRY (Jarvis et al, 2006;Hanafusa et al, 2004) and that SPRY associates with GRB2 (Thisse and Thisse, 2005) plus CBL (Wong et al, 2001). Signal attenuation due to SRC binding FRS2 has also been reported, along with the observation that SPRY is a direct physiological substrate for SRC (Li et al, 2004).…”

Section: Model Motivationmentioning

confidence: 97%

A Mass Action Model of a Fibroblast Growth Factor Signaling Pathway and Its Simplification

2008

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We consider a kinetic law of mass action model for Fibroblast Growth Factor (FGF) signaling, focusing on the induction of the RAS-MAP kinase pathway via GRB2 binding. Our biologically simple model suffers a combinatorial explosion in the number of differential equations required to simulate the system. In addition to numerically solving the full model, we show that it can be accurately simplified. This requires combining matched asymptotics, the quasi-steady state hypothesis, and the fact subsets of the equations decouple asymptotically. Both the full and simplified models reproduce the qualitative dynamics observed experimentally and in previous stochastic models. The simplified model also elucidates both the qualitative features of GRB2 binding and the complex relationship between SHP2 levels, the rate SHP2 induces dephosphorylation and levels of bound GRB2. In addition to providing insight into the important and redundant features of FGF signaling, such work further highlights the usefulness of numerous simplification techniques in the study of mass action models of signal transduction, as also illustrated recently by Borisov and co-workers (Borisov et al. in Biophys. J. 89, 951-966, 2005, Biosystems 83, 152-166, 2006 Kiyatkin et al. in J. Biol. Chem. 281, 19925-19938, 2006). These developments will facilitate the construction of tractable models of FGF signaling, incorporating further biological realism, such as spatial effects or realistic binding stoichiometries, despite a more severe combinatorial explosion associated with the latter.

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“…Because Sprouty, which is a conserved inhibitor of the Ras-MAP kinase signaling pathway, is a known target of SHP2 [21], it will be important to elucidate whether SHP2 functions as a positive regulator of ERK1/2 pathway by inactivating Sprouty protein in mESCs. Fig.…”

Section: Discussionmentioning

confidence: 99%

SHP2 is a downstream target of ZAP70 to regulate JAK1/STAT3 and ERK signaling pathways in mouse embryonic stem cells

Cha¹,

Park²

2010

FEBS Letters

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Edited by Ned ManteiKeywords: ZAP70 SHP2 ERK1/2 LIF receptor Self-renewal a b s t r a c t Previous research indicated that ZAP70, a Syk family tyrosine kinase, is expressed in mouse embryonic stem cells (mESCs) and regulates the Janus kinase 1 (JAK1)/signal transducer and activator of transcription 3 (STAT3) signaling through consolidating SHP1 enzymatic activity. In this study, we report that SHP2 is another downstream target of ZAP70 in mESCs. We found that SHP2 phosphorylation and enzymatic activity are affected by Zap70 expression. In addition, we present evidence that ERK pathways activated by ZAP70 and SHP2 reduce the protein level of leukemia inhibitory factor (LIF) receptor. Based on these results, we propose that SHP2 is an essential mediator of the ZAP70 signal to regulate JAK1/STAT3 and ERK pathways in undifferentiated mESCs.

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Shp2, an SH2-containing Protein-tyrosine Phosphatase, Positively Regulates Receptor Tyrosine Kinase Signaling by Dephosphorylating and Inactivating the Inhibitor Sprouty

Cited by 149 publications

References 32 publications

Integrating signals from RTKs to ERK/MAPK

Integrating signals from RTKs to ERK/MAPK

A Mass Action Model of a Fibroblast Growth Factor Signaling Pathway and Its Simplification

SHP2 is a downstream target of ZAP70 to regulate JAK1/STAT3 and ERK signaling pathways in mouse embryonic stem cells

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