The RasGAP Proteins Ira2 and Neurofibromin Are Negatively Regulated by Gpb1 in Yeast and ETEA in Humans

Phan, Vernon T.; Ding, Vivianne W.; Li, Fenglei; Chalkley, Robert J.; Burlingame, Alma L.; McCormick, Frank

doi:10.1128/mcb.01450-08

Cited by 56 publications

(58 citation statements)

References 46 publications

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“…76 Recently, Phan et al identified the ETEA/UBXD8 protein to interact and promote NF1 ubiquitination and degradation, which would ultimately regulate the amount of NF1 at the cell surface. 77 It is unknown if these findings are linked to earlier studies reporting that NF1 phosphorylation inhibits its lysosomal degradation. 78 Interestingly, ETEA/UBXD8 does not interact with p120GAP, 77 the other ubiquitously expressed RasGAP, indicative of this interaction contributing to differential and spatiotemporal Ras signaling.…”

Section: Nf1mentioning

confidence: 70%

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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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Section: Nf1mentioning

confidence: 70%

“…77 It is unknown if these findings are linked to earlier studies reporting that NF1 phosphorylation inhibits its lysosomal degradation. 78 Interestingly, ETEA/UBXD8 does not interact with p120GAP, 77 the other ubiquitously expressed RasGAP, indicative of this interaction contributing to differential and spatiotemporal Ras signaling.…”

Section: Nf1mentioning

confidence: 70%

Differential Regulation of RasGAPs in Cancer

et al. 2011

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“…While numerous binding partners of neurofibromin have been reported (Patrakitkomjorn, et al, 2008;Phan, et al, 2010;Welti, et al, 2008), the physiological significance of the underlying protein-protein Welti, et al, 2007). A number of missense mutations of the Sec14-PH module have been identified in NF1-patients as well as single and double amino acid deletions (Table 1).…”

Section: Introductionmentioning

confidence: 99%

Structural and biochemical consequences of NF1 associated nontruncating mutations in the Sec14-PH module of neurofibromin

et al. 2011

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“…Moreover, Wang and colleagues found that neither IBMPFD-associated mutant VCP nor dominant negative VCP affected NF1 stability or ubiquitination state. This is surprising, because others have found that NF1 protein levels can be stabilized by genetic knockdown of another known VCP cofactor and NF1 interactor, UBXD8 (18). Whether UBXD8 is the missing link between VCP and NF1 in mediating synaptogenesis remains to be studied.…”

Section: Vcp Interacts With Nf1 In the Brain And Mediates Synaptogenesismentioning

confidence: 79%

“…Sudhof and Sugita have previously immunoprecipitated the synaptic vesicle protein synaptotagmin 1 (Syt1) from rat brain and identified VCP as an interactor (19). VCP associates with Syt1 in a Ca 2+ -dependent manner; however, unlike most specialized synaptic proteins, VCP is expressed at high levels in all tissues examined and did not increase during postnatal brain development, when synaptogenesis occurs (18). VCP has also been found to associate with another presynaptic protein, strumpellin, which is mutated in a dominant form of familial spastic paraplegia (SPG8) (20,21).…”

Section: Vcp Interacts With Nf1 In the Brain And Mediates Synaptogenesismentioning

confidence: 99%

Another VCP interactor: NF is enough

Weihl

2011

J. Clin. Invest.

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The RasGAP Proteins Ira2 and Neurofibromin Are Negatively Regulated by Gpb1 in Yeast and ETEA in Humans

Cited by 56 publications

References 46 publications

Differential Regulation of RasGAPs in Cancer

Differential Regulation of RasGAPs in Cancer

Structural and biochemical consequences of NF1 associated nontruncating mutations in the Sec14-PH module of neurofibromin

Another VCP interactor: NF is enough

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