SynGAP-MUPP1-CaMKII Synaptic Complexes Regulate p38 MAP Kinase Activity and NMDA Receptor- Dependent Synaptic AMPA Receptor Potentiation

Krapivinsky, Grigory; Medina, Igor; Krapivinsky, Luba; Gapon, Svetlana; Clapham, David E.

doi:10.1016/j.neuron.2004.08.003

Cited by 265 publications

(307 citation statements)

References 47 publications

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“…Alternatively, it is possible that SynGAP functions to catalyze inactivation of Ras related GTPases such as Rin and Rap, or even distinct GTPases including members of the Rab family. Indeed, there is precedent for promiscuity among classes of GAPs and small G proteins (29), and SynGAP has recently been shown to regulate Rap1 in vitro (13). Interestingly, calcium influx stimulates a Rap1͞BRAF signaling pathway that leads to ERK activation in neurons (30), and the expression of an inhibitory Rap1 isoform in the forebrain results in suppression of ERK1͞2 (31), suggesting multiple independent pathways for this type of signaling.…”

Section: Discussionmentioning

confidence: 99%

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SynGAP regulates synaptic strength and mitogen-activated protein kinases in cultured neurons

Rumbaugh

Adams

Kim

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

241

252

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Silent synapses, or excitatory synapses that lack functional ␣-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptors (AMPARs), are thought to be critical for regulation of neuronal circuits and synaptic plasticity. Here, we report that SynGAP, an excitatory synapse-specific RasGAP, regulates AMPAR trafficking, silent synapse number, and excitatory synaptic transmission in hippocampal and cortical cultured neurons. Overexpression of SynGAP in neurons results in a remarkable depression of AMPAR-mediated miniature excitatory postsynaptic currents, a significant reduction in synaptic AMPAR surface expression, and a decrease in the insertion of AMPARs into the plasma membrane. This change is specific for AMPARs because no change is observed in synaptic NMDA receptor expression or total synapse density. In contrast to these results, synaptic transmission is increased in neurons from SynGAP knockout mice as well as in neuronal cultures treated with SynGAP small interfering RNA. In addition, activation of the extracellular signalregulated kinase, ERK, is significantly decreased in SynGAP-overexpressing neurons, whereas P38 mitogen-activated protein kinase (MAPK) signaling is potentiated. Furthermore, ERK activation is up-regulated in neurons from SynGAP knockout mice, whereas P38 MAPK function is depressed. Taken together, these data suggest that SynGAP plays a critical role in the regulation of neuronal MAPK signaling, AMPAR membrane trafficking, and excitatory synaptic transmission.trafficking ͉ Ras ͉ glutamate ͉ receptor ͉ plasticity E xcitatory synaptic transmission in the mammalian forebrain is primarily mediated by activation of both ␣-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid (AMPA) and NMDA receptors (1-3). AMPA receptors (AMPARs) mediate the bulk of ion flux during excitatory postsynaptic currents (EPSCs). In contrast, the NMDA receptor is restricted in its ability to pass current because of a voltage-dependent block of its ion channel by magnesium ions, which precludes it from participating in fast synaptic transmission at normal resting membrane potentials. However, when NMDA receptors are activated under depolarized conditions, its high calcium permeability triggers a cascade of signaling events responsible for inducing long-lasting changes in synaptic transmission.Recently, studies have demonstrated that stimuli that elicit long-term potentiation (LTP), a cellular correlate to learning and memory, also result in AMPAR delivery to synapses (4, 5). These studies have led to the idea that AMPARs are highly dynamic and the number of AMPARs at synaptic sites is tightly controlled. With this concept in mind, one can envision that AMPAR concentration at synapses is a major determinant of synaptic ''weight'' or ''strength.'' Thus, molecules and signaling pathways that regulate AMPAR trafficking are likely to directly influence LTP and may be key effectors in neuronal circuit plasticity and information storage.SynGAP, a neuronal specific RasGAP that binds to the PDZ domains of PSD-95 and SAP102 (6), ...

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Section: Discussionmentioning

confidence: 99%

“…3C). We also obtained siRNAs that specifically knock down only SynGAP-␣ [si ALPHA (13)], the isoform of SynGAP that binds to synaptic PDZ proteins. These oligonucleotides were equally effective in knocking down SynGAP protein (data not shown).…”

mentioning

confidence: 99%

SynGAP regulates synaptic strength and mitogen-activated protein kinases in cultured neurons

Rumbaugh

Adams

Kim

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

241

252

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“…synapses where it associates with PSD-95 and regulates cofilin activity [297][298][299] siRNA, exhibit increased actin polymerization and phospho-cofilin levels, and an increase in the synaptic strength and the in number of "mushroom" spines 297,301,305 , which is one of the notable classes of spine shape in addition to "thin", "stubby", and "branched". SYNGAP1…”

Section: Accepted Manuscriptmentioning

confidence: 99%

Dendritic spine actin cytoskeleton in autism spectrum disorder

Joensuu¹,

Lanoue

Hotulainen

2018

Progress in Neuro-Psychopharmacology and Biological Psychiatry

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“…[12][13][14][15] Indeed, all GAP1 family members except GAP1 m and even Syn-GAP can stimulate Rap1-GTP hydrolysis. [12][13][14][15]118 At first, these unexpected findings appeared difficult to interprete, as GAPs specific for Ras and Rap1 act differently. Unlike Ras, Rap1 does not possess a glutamine at position 61, and RapGAPs do not employ a catalytic arginine residue (arginine finger) but provide an asparagine (asparagine thumb) to stimulate GTP hydrolysis.…”

Section: Gap1 M and Gap1 Ib4bpmentioning

confidence: 99%

Differential Regulation of RasGAPs in Cancer

et al. 2011

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Ever since their discovery as cellular counterparts of viral oncogenes more than 25 years ago, much progress has been made in understanding the complex networks of signal transduction pathways activated by oncogenic Ras mutations in human cancers. The activity of Ras is regulated by nucleotide exchange factors (GEFs) and GTPase activating proteins (GAPs), and much emphasis has been put into the biochemical and structural analysis of the Ras/GAP complex. The mechanisms by which GAPs catalyze Ras-GTP hydrolysis have been clarified and revealed that oncogenic Ras mutations confer resistance to GAPs and remain constitutively active. However, it is yet unclear how cells coordinate the large and divergent GAP protein family to promote Ras inactivation and ensure a certain biological response. Different domain arrangements in GAPs to create differential protein-protein and protein-lipid interactions are probably key factors determining the inactivation of the 3 Ras isoforms H-, K-, and N-Ras and their effector pathways. In recent years, in vitro as well as cell-and animal-based studies examining GAP activity, localization, interaction partners, and expression profiles have provided further insights into Ras inactivation and revealed characteristics of several GAPs to exert specific and distinct functions. This review aims to summarize knowledge on the cell biology of RasGAP proteins that potentially contributes to differential regulation of spatiotemporal Ras signaling.

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SynGAP-MUPP1-CaMKII Synaptic Complexes Regulate p38 MAP Kinase Activity and NMDA Receptor- Dependent Synaptic AMPA Receptor Potentiation

Cited by 265 publications

References 47 publications

SynGAP regulates synaptic strength and mitogen-activated protein kinases in cultured neurons

SynGAP regulates synaptic strength and mitogen-activated protein kinases in cultured neurons

Dendritic spine actin cytoskeleton in autism spectrum disorder

Differential Regulation of RasGAPs in Cancer

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