Isolation and characterization of a Drosophila homologue of mitogen-activated protein kinase phosphatase-3 which has a high substrate specificity towards extracellular-signal-regulated kinase

Kim, Sun Hong; Kwon, Hyung Bae; Kim, Yong Sik; Ryu, Ji Hwan; Kim, Kyung Sub; Ahn, Yong-Ho; Lee, Won Jae; Choi, Kang Yell

doi:10.1042/bj3610143

Cited by 30 publications

(41 citation statements)

References 41 publications

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“…This hypothesis is supported by data from Chu et al (Chu et al, 1996) who showed that the mammalian Sevenmaker homologue ERK2 D319N is inactivated by DSPs in COS-7 cells at high, but not in NIH3T3 cells at lower expression. The genetic interactions are consistent with a function of DMKP3 between Raf and Rl SEM and strongly support the interpretation that ERK is the main target of DMKP3 (Kim et al, 2002).…”

Section: Dmkp3 Interacts Genetically With Components Of the Ras Pathwaysupporting

confidence: 67%

“…In a recent study Kim et al (Kim et al, 2002) have shown that the Drosophila dual specificity phosphatase DMKP3 dephosphorylates ERK, but not JNK or p38 MAP kinases in vitro. Here we provide in vivo evidence in Drosophila that DMKP3 is a phosphatase specific for ERK.…”

Section: Dmkp3 Has a High Specificity Towards Erk In Vivomentioning

confidence: 99%

“…(1) DMKP3 dephosphorylates ERK but not JNK in vitro (Kim et al, 2002). (2) showing both Dmkp3 -(pink in the bar diagram) and Dmkp3 + photoreceptors (red) at any position.…”

Section: Dmkp3 Is a Negative Regulator Of The Ras/mapk Pathwaymentioning

confidence: 99%

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TheDrosophiladual-specificity ERK phosphatase DMKP3 cooperates with the ERK tyrosine phosphatase PTP-ER

2003

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ERK MAP kinase plays a key role in relaying extracellular signals to transcriptional regulation. As different activity levels or the different duration of ERK activity can elicit distinct responses in one and the same cell, ERK has to be under strict positive and negative control. Although numerous genes acting positively in the ERK signaling pathway have been recovered in genetic screens, mutations in genes encoding negative ERK regulators appear underrepresented. We therefore sought to genetically characterize the dual-specificity phosphatase DMKP3. First, we established a novel assay to elucidate the substrate preferences of eukaryotic phosphatases in vivo and thereby confirmed the specificity of DMKP3 as an ERK phosphatase. The Dmkp3 overexpression phenotype characterized in this assay permitted us to isolate Dmkp3 null mutations. By genetic analysis we show that DMKP3 and the tyrosine phosphatase PTP-ER perform partially redundant functions on the same substrate, ERK. DMKP3 functions autonomously in a subset of photoreceptor progenitor cells in eye imaginal discs. In addition, DMKP3 function appears to be required in surrounding nonneuronal cells for ommatidial patterning and photoreceptor differentiation.

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Section: Dmkp3 Interacts Genetically With Components Of the Ras Pathwaysupporting

confidence: 67%

Section: Dmkp3 Has a High Specificity Towards Erk In Vivomentioning

confidence: 99%

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TheDrosophiladual-specificity ERK phosphatase DMKP3 cooperates with the ERK tyrosine phosphatase PTP-ER

2003

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“…The MAPK pathway plays a role in the maintenance of tracheal branch integrity, but not through the nuclear effector Pnt Mkp3 has been shown to act as a specific negative regulator of the ERK-type MAPK (Kim et al, 2002;Rintelen et al, 2003). ERK is a central element of the Ras/MAPK pathway whose activity is regulated by phosphorylation (Roux and Blenis, 2004).…”

Section: Overexpression Of Mkp3 Is Responsible For the Branch Integrimentioning

confidence: 99%

Egfr is essential for maintaining epithelial integrity during tracheal remodelling inDrosophila

Cela

Llimargas

2006

Development

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A fundamental requirement during organogenesis is to preserve tissue integrity to render a mature and functional structure. Many epithelial organs, such as the branched tubular structures, undergo a tremendous process of tissue remodelling to attain their final pattern. The cohesive properties of these tissues need to be finely regulated to promote adhesion yet allow flexibility during extensive tissue remodelling. Here, we report a new role for the Egfr pathway in maintaining epithelial integrity during tracheal development in Drosophila. We show that the integrity-promoting Egfr function is transduced by the ERK-type MAPK pathway, but does not require the downstream transcription factor Pointed. Compromising Egfr signalling, by downregulating different elements of the pathway or by overexpressing the Mkp3 negative regulator, leads to loss of tube integrity, whereas upregulation of the pathway results in increased tissue stiffness. We find that regulation of MAPK pathway activity by Breathless signalling does not impinge on tissue integrity. Egfr effects on tissue integrity correlate with differences in the accumulation of markers for cadherinbased cell-cell adhesion. Accordingly, downregulation of cadherin-based cell-cell adhesion gives rise to tracheal integrity defects. Our results suggest that the Egfr pathway regulates maintenance of tissue integrity, at least in part, through the modulation of cell adhesion. This finding establishes a link between a developmental pathway governing tracheal formation and cell adhesiveness.

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“…PTP-ER est ellemême phosphorylée et inactivée par ERK, décrivant ainsi une boucle de rétroaction. Par ailleurs, MKP3, une phosphatase à double spécificité (sérine/thréo-nine et tyrosine) agissant aussi sur ERK, a été mise en évidence par homologie de séquence chez la mouche et le nématode [45,46]. Une étude chez la drosophile a montré que PTP-ER et MKP3 peuvent agir indépen-damment l'une de l'autre, ou de manière concertée selon le contexte cellulaire [47].…”

Section: Apport Des Modèles Génétiquesunclassified

La signalisation RTK/RAS/ERK élargie

Ashton‐Beaucage

Therrien

2010

Med Sci (Paris)

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Isolation and characterization of a Drosophila homologue of mitogen-activated protein kinase phosphatase-3 which has a high substrate specificity towards extracellular-signal-regulated kinase

Cited by 30 publications

References 41 publications

TheDrosophiladual-specificity ERK phosphatase DMKP3 cooperates with the ERK tyrosine phosphatase PTP-ER

TheDrosophiladual-specificity ERK phosphatase DMKP3 cooperates with the ERK tyrosine phosphatase PTP-ER

Egfr is essential for maintaining epithelial integrity during tracheal remodelling inDrosophila

La signalisation RTK/RAS/ERK élargie

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